Oncotelic Therapeutics, Inc. (OTLC) — 10-K

Filed 2025-04-15 · Period ending 2024-12-31 · 81,673 words · SEC EDGAR

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# Oncotelic Therapeutics, Inc. (OTLC) — 10-K

**Filed:** 2025-04-15
**Period ending:** 2024-12-31
**Accession:** 0001641172-25-004846
**Source:** [SEC EDGAR](https://www.sec.gov/Archives/edgar/data/908259/000164117225004846/)
**Origin leaf:** f196a92512b04158d17597f0a663098911d933f15841a9de467d2e2085bb0963
**Words:** 81,673



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**
UNITED
STATES**
**SECURITIES
AND EXCHANGE COMMISSION**
**Washington,
D.C. 20549**
**FORM
10-K**
**(Mark
One)**
**ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934**
**For
the fiscal year ended December 31, 2024**
**OR**
**TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934**
**For
the transition period from to**
**Commission
File Number: 0-21990**
**Oncotelic
Therapeutics, Inc.**
**(Exact
name of registrant as specified in its charter)**
| 
Delaware | 
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13-3679168 | |
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(State
or other jurisdiction of
incorporation or organization) | 
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(I.R.S.
Employer
Identification No.) | |
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29397
Agoura Road, Suite 107 
Agoura Hills, CA | 
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91301 | |
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(Address
of principal executive offices) | 
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(Zip
Code) | |
**Registrants
telephone number, including area code: (650) 635-7000**
**Securities
registered pursuant to Section 12(b) of the Exchange Act:**
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Title
of Each Class | 
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Name
of Each Exchange on Which Registered | |
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None | 
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**Securities
registered pursuant to Section 12(g) of the Exchange Act:**
**Common
stock, par value $0.01 per share**
Indicate
by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act. Yes No 
Indicate
by check mark if the registrant is not required to file reports pursuant to Section 13 or Section 15(d) of the Exchange Act. Yes 
No 
Indicate
by check mark whether the registrant (1) has filed all reports required to be filed by Section 13 or 15(d) of the Securities Exchange
Act of 1934 during the preceding 12 months (or for such shorter period that the registrant was required to file such reports), and (2)
has been subject to such filing requirements for the past 90 days. Yes No 
Indicate
by check mark whether the registrant has submitted electronically every Interactive Data File required to be submitted pursuant to Rule
405 of Regulation S-T ( 232.405 of this chapter) during the preceding 12 months (or for such shorter period that the registrant
was required to submit such files). Yes No 
Indicate
by check mark if disclosure of delinquent filers pursuant to Item 405 of Regulation S-K ( 229.405 of this chapter) is not contained
herein, and will not be contained, to the best of registrants knowledge, in definitive proxy or information statements incorporated
by reference in Part III of this Form 10-K, or any amendment to this Form 10-K. 
Indicate
by check mark whether the registrant is a large accelerated filer, an accelerated filer, a non-accelerated filer, a smaller reporting
company, or an emerging growth company. See the definitions of large accelerated filer, accelerated filer,
smaller reporting company, and emerging growth company in Rule 12b-2 of the Exchange Act. (Check one):
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Large
accelerated filer | 
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Accelerated
filer | 
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Non-accelerated
filer | 
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Smaller
reporting company | 
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Emerging
growth company | 
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If
an emerging growth company, indicate by check mark if the registrant has elected not to use the extended transition period for complying
with any new or revised financial accounting standards provided pursuant to Section 13(a) of the Exchange Act. 
Indicate
by check mark whether the registrant has filed a report on and attestation to its managements assessment of the effectiveness
of its internal control over financial reporting under Section 404(b) of the Sarbanes-Oxley Act (15 U.S.C. 7262(b)) by the registered
public accounting firm that prepared or issued its audit report. 
If
securities are registered pursuant to Section 12(b) of the Act, indicate by check mark whether the financial statements of the registrant
included in the filing reflect the correction of an error to previously issued financial statements.
Indicate
by check mark whether any of those error corrections are restatements that required a recovery analysis of incentive-based compensation
received by any of the registrants executive officers during the relevant recovery period pursuant to 240.10D-1(b).
Indicate
by check mark whether the registrant is a shell company (as defined in Rule 12b-2 of the Exchange Act). Yes No 
The
aggregate market value of the registrants voting and non-voting common stock held by non-affiliates of the registrant (without
admitting that any person whose shares are not included in such calculation is an affiliate) computed by reference to the price at which
the common stock was last sold, as of June 30, 2022 was approximately $5,633,200.
As
of April 14, 2025, the aggregate number of outstanding shares of common stock of the registrant was 408,292,450.
**DOCUMENTS
INCORPORATED BY REFERENCE**
None.
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**TABLE
OF CONTENTS**
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PAGE | |
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PART I | 
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ITEM
1. | 
BUSINESS | 
1 | |
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REGULATORY MATTERS | 
14 | |
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PATENTS AND PROPRIETARY RIGHTS | 
20 | |
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COMPETITION | 
21 | |
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EMPLOYEES | 
21 | |
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ITEM
1A. | 
RISK FACTORS | 
21 | |
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ITEM
1B. | 
UNRESOLVED STAFF COMMENTS | 
36 | |
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ITEM
2. | 
PROPERTIES | 
37 | |
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ITEM
3. | 
LEGAL PROCEEDINGS | 
37 | |
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ITEM
4. | 
MINE SAFETY DISCLOSURES | 
37 | |
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PART II | 
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ITEM
5. | 
MARKET FOR REGISTRANTS COMMON EQUITY, RELATED STOCKHOLDER MATTERS AND ISSUER PURCHASES OF EQUITY SECURITIES | 
37 | |
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ITEM
6. | 
RESERVED | 
38 | |
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ITEM
7. | 
MANAGEMENTS DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS | 
38 | |
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RESULTS OF OPERATIONS | 
47 | |
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LIQUIDITY AND CAPITAL RESOURCES | 
49 | |
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ITEM
7A. | 
QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK | 
50 | |
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ITEM
8. | 
FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA | 
51 | |
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ITEM
9. | 
CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE | 
51 | |
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ITEM
9A. | 
CONTROLS AND PROCEDURES | 
51 | |
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ITEM
9B. | 
OTHER INFORMATION | 
52 | |
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PART III | 
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ITEM
10. | 
DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE | 
53 | |
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ITEM
11. | 
EXECUTIVE COMPENSATION | 
57 | |
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ITEM
12. | 
SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT AND RELATED STOCKHOLDER MATTERS | 
64 | |
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ITEM
13. | 
CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS AND DIRECTOR INDEPENDENCE | 
67 | |
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ITEM
14. | 
PRINCIPAL ACCOUNTING FEES AND SERVICES | 
68 | |
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PART IV | 
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ITEM
15. | 
EXHIBITS AND FINANCIAL STATEMENT SCHEDULES | 
69 | |
| I | |
**FORWARD-LOOKING
STATEMENTS**
This
2024 Annual Report on Form 10-K (this *Annual Report* or *Report*) contains forward-looking statements
within the meaning of Section 27A of the Securities Act and Section 21E of the Securities Exchange Act of 1934 (the *Exchange
Act*) that involve substantial risks and uncertainties. We generally identify forward-looking statements by terminology such
as may, will, should, expect, plan, anticipate, could,
would, intend, target, aim, project, believe, estimate,
predict, potential, seek, indicate, or continue or the negative
of these terms or other similar words, although not all forward-looking statements contain these words. Forward-looking statements include,
but are not limited to, statements regarding our or our managements expectations, hopes, beliefs, intentions or strategies regarding
the future, such as our estimates regarding anticipated operating income or losses, future performance, future revenues and projected
expense, including that to fund our clinical and other development programs; our liquidity and our expectations regarding our needs for
and ability to raise additional capital; our ability to continue as a going concern; our ability to select and capitalize on commercially
desirable product opportunities as a result of limited financial resources; our ability to manage our expenses effectively and raise
the funds needed to continue our business; our ability to retain the services of our current or future executive officers, directors
and principal consultants; the competitive nature of our industry and the possibility that our products or product candidates may become
obsolete or may not generate revenues as expected or at all; our ability to obtain and maintain regulatory approval of our existing products
and any future products we may develop; the development of and the process of commercializing AI/Blockchain and other technologies for
supporting the development of OT- 101 and Artemisinin for COVID-19, OT-101, including development of OT-101, Artemisinin, OXi4503, CA4P
and our 2021 in-licensing of apomorphine; the initiation, timing, progress and results of our preclinical and clinical trials, research
and development programs; regulatory and legislative developments in the United States and foreign countries; the timing, costs and other
limitations involved in obtaining regulatory approval for any product; the further preclinical or clinical development and commercialization
of our product candidates; the entering into any corporate transactions to develop our products through partnerships, joint ventures
or other corporate transactions; our ability to make a proposed initial public offering between us and our joint-venture partners for
the joint venture, statements about future plans related to the operations of the JV, taking the JV into an initial public offering or
the success thereof: building and the success of our nanoparticle platform and the related success of launching the platform; the expected
valuation of the JV, and therefore a corresponding increase in the valuation of the Company, by virtue of its ownership in the
JV; the success of the launch of Pet2DAO, a corporation with a DAO infrastructure, the success of Pet2DAO and the plans surrounding the
pet and animal health, the ability for the Company to register the tokens of Pet2DAO, the actual filing of a registration statement and
approval of the tokens as registrable securities with the Securities and Exchange Commission (*SEC*) through a registration
statement, the ability of the tokens to be tradable or any value such tokens may have if they become tradable; our ability to obtain
and maintain orphan drug exclusivity for some of our product candidates; the potential benefits of our product candidates over other
therapies; our ability to enter into and maintain any collaboration with respect to product candidates; our ability to continue to develop
or commercialize our products or product candidates in the event any license agreements in place with third parties expire or are terminated;
the performance and conduct of third parties, including our third-party manufacturers and third party service providers used in our clinical
trials; our ability to obtain and maintain intellectual property protection for our products and operate our business without infringing
upon the intellectual property rights of others; the potential liability exposure related to our products and our insurance coverage
for such exposure; our ability to form alliances with other third parties to develop the products in our pipeline through partnerships,
joint ventures, mergers or acquisitions; the successful development of our sales and marketing capabilities; the size and growth of the
potential markets for our products and our ability to serve those markets; the rate and degree of market acceptance of any future products;
the volatility of the price of our common stock; the ability to achieve secondary trading of our stock in certain states; the dilutive
effects of potential future equity issuances; our expectation that no dividends will be declared on our common stock in the foreseeable
future; our ability to maintain an effective system of internal controls; the payment and reimbursement methods used by private or governmental
third-party payers; our ability to retain adequate staffing levels; unfavorable global economic conditions; unfavorable global epidemic
and pandemic conditions; a failure of our internal computer systems or those of our contractors and consultants; potential misconduct
or other improper activities by our employees, contractors or consultants; the ability of our business continuity and disaster recovery
plans to protect us in the event of a natural disaster; and other factors discussed elsewhere in this document or any document incorporated
by reference herein or therein.
The
forward-looking statements contained in this document are based on our current expectations and beliefs concerning future developments
and their potential effects on us. There can be no assurance that future developments affecting us will be those that we have anticipated.
These forward-looking statements involve several risks, uncertainties (many of which are beyond our control) or other assumptions that
may cause actual results or performance to be materially different from those expressed or implied by these forward-looking statements.
Should one or more of these risks or uncertainties materialize, or should any of our assumptions prove incorrect, actual results may
vary from those projected in these forward-looking statements. We undertake no obligation to update or revise any forward-looking statements,
whether as a result of new information, future events or otherwise, except as may be required under applicable securities laws. The sections
captioned Risk Factors as well as other sections in this document or incorporated by reference into this document discuss
some of the factors that could contribute to these differences.
The
forward-looking statements made in this document relate only to events known as of the date on which the statements are made. We undertake
no obligation to update any forward-looking statement to reflect events or circumstances after the date on which the statement is made
or to reflect the occurrence of unanticipated events.
This
Annual Report also contains market data related to our business and industry. These market data include projections that are based on
a number of assumptions. While we believe these assumptions to be reasonable and sound as of the date of this Annual Report, if these
assumptions turn out to be incorrect, actual results may materially differ from the projections based on these assumptions. As a result,
the markets for our product candidates may not grow at the rates projected by these data, or at all. The failure of these markets to
grow at these projected rates may have a material adverse effect on our business, results of operations, financial condition and the
market price of our common stock.
| II | |
**PART
I**
**ITEM
1. BUSINESS**
**Company
Background**
Oncotelic
Therapeutics, Inc. (f/k/a Mateon Therapeutics, Inc.) (*Oncotelic*), was formed in the State of New York in 1988 as
OXiGENE, Inc., was reincorporated in the State of Delaware in 1992, and changed its name to Mateon Therapeutics, Inc. in 2016, and Oncotelic
Therapeutics, Inc. in November 2020. Oncotelic conducts business activities through Oncotelic and its wholly-owned subsidiaries, Oncotelic,
Inc., a Delaware corporation, PointR Data, Inc. (*PointR*), a Delaware corporation, Pet2DAO, Inc., a Delaware corporation;
and EdgePoint AI, Inc. (*Edgepoint*), a Delaware Corporation for which there are non-controlling interests, (Oncotelic,
Oncotelic Inc., PointR, Pet2DAO and Edgepoint are collectively called the *Company* or *We*). The
Company is currently developing OT-101, in addition to five additional compounds, for various cancers and COVID-19 through its joint
venture, GMP Biotechnology Limited (*GMP Bio*), with Dragon Overseas Capital, Limited (*Dragon*),
Artemisinin for COVID-19 and AI technologies for clinical development and manufacturing. The Company also acquired apomorphine for Parkinsons
Disease, erectile dysfunction and female sexual dysfunction. In addition, the Company is evaluating the further development of its product
candidates OXi4503, as a treatment for acute myeloid leukemia and myelodysplastic syndromes, and CA4P, in combination with a checkpoint
inhibitor for the treatment of advanced metastatic melanoma. The Company is also planning to address the animal health industry through
Pet2DAO. Our principal corporate office is in the United States at 29397 Agoura Road, Suite 107, Agoura Hills, CA 91301 (telephone: 650-635-7000).
Our internet address is www.oncotelic.com.
**Overview**
We
are a clinical-stage biopharmaceutical company developing drugs for the treatment of orphan oncology indications, developing antisense
and small molecule injectable drugs for the treatment of cancer. After the acquisition of Mateon Therapeutics, Inc through a reverse
merger in 2019, we realigned the company pipeline to focus on various cancers, including but not limited to rare pediatric cancers. The
United States Food and Drug Administration (*FDA*) has granted us Rare Pediatric Designations (*RPD*)
for pediatric Diffuse Intrinsic Pontine Glioma (*DIPG*) for OT-101, which was transferred to our joint venture as
part of the joint venture agreement (see *JV* below), pediatric melanoma for CAP4 and acute myeloid leukemia (*AML*)
for Oxi4503. In addition, the Company, through its JV, is developing 5 additional products for treatments of various cancers.
Each of the products being developed by the JV has the potential of becoming very successful drugs. The JV is contemplating developing
and obtaining regulatory approval for each of the 5 additional products via different regulatory pathways and in various countries and
regions. Further, the Company aims to capitalize on a voucher program in the United States (*US*). By focusing on
capitalizing on the RPD we anticipate: 1) reducing the cost of clinical development by way of a smaller and faster clinical trial, 2)
acceleration of the approval process and final approval, 3) obtaining regulatory/ marketing exclusivity for up to 12 years as a biologic,
and 4) obtaining vouchers worth a significantly large monetary value upon regulatory approval, which can be upwards of several million
dollars. Approval in the US could allow for approval in the rest of the world (*ROW*) using the US dossier. Phase
3 clinical trials for approval in adult indications could be conducted following the positive interim read of the pediatric trials. This
approach maximizes return on investment for the shareholders.
Concurrently
we also explore opportunities to create value for shareholders by forming strategic alliances and/or licensing our product portfolio.
In this connection, in March 2022, the Company entered into a joint venture (*JV*) with Dragon, affiliates of Golden
Mountain Partners, LLC, to form GMP Biotechnology, Limited (*GMP Bio*). GMP Bio and the Company are also looking to
take the JV into an initial public offering (*IPO*) of the JV and which is anticipated to be a liquidity event for
Company, especially if the IPO is successful. While we believe that the IPO can be completed and would be successful, we cannot provide
assurance for either of the events to occur; or if they occur, and then whether the IPO would be successful.
We
believe we are well positioned as a biotech company with our drug candidate OT-101 through our JV- targeting high value TGF-2,
and the new product portfolio being developed by the JV, for various cancers and COVID-19, PointR artificial intelligence (*AI*)
for clinical trials, research and development, Edgepoint for developing technologies for manufacturing and for developing technologies
for supporting our COVID-19 programs, our vascular disruptor proven safe in more than 500 patients capable of causing massive antigen
release which would stimulate immune response against the cancerous tumor and apomorphine, which we in-licensed in 2021, for developing
against Parkinsons Disease (*PD*), erectile disfunction (*ED*) and female sexual disfunction
(*FSD*).
| 1 | |
We may also plan to continue to develop OT-101, through our JV, an antisense
against TGF-2 for the treatment of various viruses, which would include the severe acute respiratory syndrome (*SARS*)
and the coronavirus (*COVID-19*), on its own and in conjunction with other compounds. Viral replication cannot occur
without TGF-; and TGF- surge and a cytokine storm cannot occur without TGF-. A Phase 2 trial was completed for OT-101
in South America. This was a randomized, double-blind, placebo-controlled Phase 2 study to evaluate the safety and efficacy of OT- 101
in adult patients hospitalized with positive COVID-19 and pneumonia. Based on the final results of the trial, the trial was planned to
be expanded into a Phase 3 trial; however with the impact of COVID-19 reducing in the past year, the Company will be re-evaluating this
treatment for further development upon the occurrence or recurrence of the COVID-19 or any similar virus. We were conducting an observational
study in conjunction with the Biomedical Advanced Research and Development Authority (*BARDA*. For more information
on BARDA, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024. At this time, since the impact of COVID-19
has significantly reduced, the development of OT-101 for COVID-19 is not a top priority. In addition, during 2020 and 2021, the Company
was developing Artemisinin as a potential therapy for the virus causing COVID-19. Again, with the impact of COVID-19 reducing over the
past year or so, we have put on hold any further development of Artemisinin, till we have another severe virus situation. We will focus
on any future development on Artemisinin against other respiratory viruses with unmet needs when the circumstances arise. For more information
on Artemisinin, refer to our 2022 Annual Report on Form 10-K filed with the SEC on April 14, 2023.
In
September 2021, Oncotelic entered into an exclusive License Agreement (the Agreement) with Autotelic, Inc. (*Autotelic*),
pursuant to which Autotelic granted Oncotelic the exclusive right and license to certain Autotelic Patents for AL-101 - an intranasal
apomorphine asset with clear 505(b)2 pathway to approval for PD as well unique mechanism of action for treatment of ED and FSD. For more
information on AL-101, refer to our 2022 Annual Report on Form 10-K filed with the SEC on April 14, 2023.
We
currently have three primary drugs of our own, 6 drugs through our JV, and AI technology programs we are seeking to advance, presently
or in the future:
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AL-101
- Intranasal drug and delivery system for intra-nasal Apomorphine for the treatment of PD, ED and FSD. | |
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CA4P-
a vascular disrupting agent (VDA) - in combination with Ipilimumab for the treatment of solid tumors with focus on
melanoma in adult and pediatric melanoma. A RPD has been granted to the Company by the FDA for pediatric melanoma. | |
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Oxi4503-
a second generation VDA - for the treatment of liquid tumors with focus on childhood leukemia. A RPD has been granted to the Company
by the FDA for AML. | |
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OT-101
- an antisense against TGF-2 for the treatment of various cancers and for the treatment of various viruses, including
COVID-19, on its own and in conjunction with other compounds.. This is being advanced through our JV. | |
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Five
additional nanoparticle products - for the treatment of various cancers, using various regulatory pathways and for various regions/countries.
This is being advanced through our JV. | |
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Artemisinin
a natural derivative from an Asian herb Artemisia Annua - Artemisinin has shown to be highly potent at inhibiting the ability
of various viruses to multiply. This will be advanced through our JV at an appropriate time. | |
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Developing newer AI based technologies to enhance the development and commercialization
of support technologies. The JV has acquired a non-exclusive license for the AI platform developed by PointR/EdgePoint for implementation
in a planned CDMO. | |
In
November 2022, the Company formed a Decentralized autonomous organization (*DAO*) entity, Pet2DAO, Inc.
(*Pet2DAO*), as a wholly owned subsidiary. A DAO is an emerging form of legal structure, that has no central
governing body, and whose members share a common goal to act in the best interest of the entity. Pet2DAO is a DAO technology
company, integrating the strong governance of traditional corporations with the innovative DAO architecture. The Company will look
to engage stakeholders, to build value through the DAO, while maintaining the rigor of traditional corporations, including
governance, compliance, and accountability through a team of veterans in public companies with innovators in AI, blockchain and
Web3. Pet2DAO will be looking to develop products for the animal health space. The Company will initially issue utility tokens
and non-fungible tokens (*NFT* and cumulatively *Tokens*) of Pet2DAO, called PDAO, to its
employees, shareholders and key opinion leaders (*KOLs*) and use the Tokens to propose and vote on various human
and animal health related programs. In the future, the Company will evaluate and plans to register these tokens with the SEC to make
such Tokens freely tradable.
| 2 | |
**Our
products, including our JV products, under development**
**AL-101:
PD/ ED/FSD**
Oncotelic
acquired AL-101 for the intranasal delivery of apomorphine for the treatment of PD. Over 60,000 new patients being diagnosed with PD
in the United States and currently there are over 1 million patients in the US and expected to increase to over 1.2 million by 2030.
In addition, approximately 10 million suffer from this disease globally. https://www.parkinson.org/Understanding-Parkinsons/Statistics.
AL-101 is also being developed for ED. ED is the most prevalent male sexual disorder globally. The percentages of men affected by ED
are as follows: 14.3- 70% of men aged 60 years, 6.7-48% of men aged 70 years, and 38% of men aged 80 years (Geerkens MJM et al. (2019).
Eur Urol Focus. pii: S2405-4569(19)30079-3). However, with the increasing administration of PDE5 inhibitors in clinical practice, it
was found that approximately 30-35% of ED patients are treatment failures (McMahon CN et al. (2006). BMJ, 332: 589-92). AL-101 is designed
to target treatment failure ED patients who do not respond to PDE5 inhibitors. Through similar mechanism of action, AL-101 is being developed
for FSD. FSD is a prevalent problem, afflicting approximately 40% of women and there are few treatment options. FSD is more typical as
women age and is a progressive and widespread condition. (Allahdadi, KJ et al. (2009) Cardiovascular & hematological agents in medicinal
chemistry, 7(4), 260-269). There is no available drug for the treatment of FSD. In June 2019, the FDA approved Vyleesi (bremelanotide)
to treat acquired, generalized hypoactive sexual desire disorder (*HSDD*) in premenopausal women. This is the only
available drug treatment. Vyleesi has essentially replaced the only other drug for HSDD, however, it has a long list of drug-drug interactions,
including commonly used antidepressants, such as fluoxetine and sertraline. In addition, it has a black box warning regarding its use
with alcohol, a combination that has been associated with hypotension and syncopal episodes. Therefore, there is an urgent need for effective
therapy against FSD and HSDD.
**CA4P
as an Immuno-Oncology Agent**
Radiation
therapy, recognized for its potent cytotoxic effect on cancer cells by inducing direct DNA damage, can sometimes elicit a systemic antitumoral
response. Irradiation releases a plethora of neoantigens and pro- inflammatory cytokines, acting like an in-situ vaccine, resulting in
tumor regression within the primary site, but may also occasionally result in regression of distant secondary lesions. This regression
of distant cancer metastases when the primary tumor is irradiated is defined as the abscopal effect. Yet, an abscopal effect with radiotherapy
alone occurs infrequently, signifying that the antitumor immunity caused by radiation is not sufficient to abolish the tumor and its
metastases nor able to prevent the metastatic process or the immunosuppressing effect the cancer exhibits on the hosts systemic
macroenvironment. Recently, several studies have confirmed the synergistic antitumoral immunity caused by the combination of radiation
with immunotherapy, which has demonstrated a durable abscopal effect in patients with advanced malignancies. Postow, et al, Golden, et
al, Hinicker, et al and others have all described early findings of a reproducible abscopal effect when combining irradiation with Ipilimumab
and/or Nivolumab.
Similarly,
CA4P causes rapid and widespread tumor cell necrosis. A number of laboratories have shown that the type of tumor cell death induced by
ischemic necrosis not only controls the presence or absence of specific tumor antigens, but also can result in immunological responses
ranging from immunosuppression to anti-tumor immunity. The terms immunogenicity of cell death or immunogenic cell
death (ICD) is often used by scientists to describe the ability of dead/dying cells (especially of tumor cells) to mount antigen-specific
and particularly CD8 + T-cell- mediated adaptive immune responses and not simply lead to innate inflammation. CD8 + T-cells play a significant
role in tumor protection and development of this type of immunity. A modernized concept has emerged which defines immunogenic cell death
in general because of mutual or consequent processes including endoplasmic reticulum stress release of find-me signals
(e.g., ATP), exposure of eat-me signals (e.g., calreticulin, phosphatidylserine) and damage-associated molecular patterns
(DAMPs [HMGB1, F-actin]). These molecular changes might occur in the cells undergoing necrotic death. These and other signals appear
to be relevant to the potential for CA4P to increase immunogenicity following induction of ischemic necrosis.
Preclinical
studies in which CA4P was combined with an anti-CTLA4 antibody using an EMT-6 mammary tumor model showed that 7 out of 8 mice receiving
a combination of CA4P and an anti-CTLA4 antibody experienced complete remission of their tumors, compared to only 1 of 8 in the CA4P
monotherapy arm and 2 of 8 in the anti- CTLA4 antibody monotherapy.
| 3 | |
Three
of four follow-up preclinical studies confirmed that CA4P combined with immuno-oncology agents could delay tumor growth. Follow-up studies
were conducted in a CT26-32 colon cancer model, a larger tumor EMT- 6 mammary cancer model, and a C3H mammary cancer model. Studies in
a CT-26-32 colon cancer animal model using CA4P combined with anti-CTLA4 antibodies demonstrated a 77% reduction in tumor size compared
to immuno- oncology agents alone, and an 89% reduction in tumor size compared to control. This large tumor model also showed a survival
benefit for the animals receiving combination therapy, with all animals in the combination therapy group surviving to the end of the
study, compared to no animals surviving on the control and only half of the animals surviving that received immuno-oncology agents alone.
Additional
analyses of changes induced within tumors following combination therapy have shown that CA4P increases the immunogenic effect of checkpoint
inhibitors when used alone as monotherapy. Tumor-fighting white blood cell counts, T-cells and cytotoxic T-cells compared to immuno-oncology
agents alone. Tumor necrosis with the combination of CA4P and immuno-oncology agents is nearly double the necrosis with only immuno-oncology
agents (63.9% compared to 32.8%, control = 25.8%).
The
overall data from all these studies provides evidence that CA4P may enhance the activity of immuno- oncology agents for the treatment
of cancer, including anti-CTLA4 antibodies. Furthermore, CA4P has clinical activity in melanoma in early clinical testing and repeated
demonstration of CA4P mediated necrotic tumor cell death across 17 completed clinical trials and >500 patients. During various phase
1 studies, we found that CA4P treatment resulted in significant disease control among patients with solid tumors who progressed on standard
therapies. CA4P treatment resulted in 2 Stable Disease (SD) of 5 melanoma patients treated. The combination of CA4P with carboplatin
and paclitaxel was well tolerated in the majority of patients with adequate premedication and had antitumor activity in patients who
were heavily pretreated. Patients with advanced cancer refractory to standard therapy were treated with CA4P as a 10-min infusion, 20
h before carboplatin, paclitaxel, or paclitaxel, followed by carboplatin. Responses were seen in 10 of 46 (22%) patients with ovarian,
esophageal, small-cell lung cancer, and melanoma. One Partial Response (PR) was observed of 6 melanoma patients treated follow progressing
during first-line trial therapy with dacarbazine and sorafenib. In melanoma animal model- B16-F10 murine melanoma experimental tumors-
seventy- four hours after drug administration, a decrease in the number of tumor blood vessels was apparent and necrotic areas within
tumors were visible. Building on the single agent activity of CA4P, we are expecting that combination of CA4P with Ipilimumab or other
immune-oncology drug would result in improved tumor control for these patients above the 2 PR out of 17 patients treated with Ipilimumab
alone which supported the approval of Ipilimumab in pediatric melanoma.
**CA4P:
Pediatric Melanoma**
Until
the recent approval of ipilimumab as the first immunotherapy agent approved for children, metastatic or nonresectable pediatric melanoma
did not have any FDA-approved therapies available. As for adult melanoma patients, the mainstay of care is surgical excision. Studies
also show that children treated for melanoma should be closely monitored as they are at increased risk of recurrence later in life. However,
there is only very limited data on the efficacy of systemic therapy in children and adolescents with advanced melanoma and new effective
therapies are urgently needed. Several phase I/II trials have been designed to evaluate therapies for pediatric cancer patients that
included subsets of patients with advanced melanoma.
Ipilimumab
was evaluated in a phase I clinical study in children with unresectable stage IIIC or IV melanoma and in a pediatric phase II trial (NCT01696045)
that included children aged 12 years or older with previously treated or untreated, unresectable stage III or IV malignant melanoma.
Of the 17 melanoma patients older than 12 years treated with ipilimumab across both studies, two experienced objective responses. Immune-related
adverse events included pancreatitis, pneumonitis, endocrinopathies, colitis, and transaminitis, with dose-limiting toxicities observed
at 5 mg/kg. No grade 2 or higher immune-related toxicities were identified at doses of 3 mg/kg or less. Based upon the results of these
studies and evidence from studies in adult patients, in July 2017, the FDA approved ipilimumab for the treatment of unresectable or metastatic
melanoma in children aged 12 years and older.
It
is expected that combination of CA4P with Ipilimumab or other immune-oncology drugs would result in improved tumor control for these
patients above the 2 PR out of 17 patients treated with ipilimumab.
| 4 | |
The
FDA has granted Rare Pediatric Disease Designation for CA4P/ Fosbretabulin tromethamine for the treatment of stage IIBIV melanoma
due to genetic mutations that disproportionately affect pediatric patients as a drug. Preclinical studies in which CA4P was combined
with an anti-CTLA4 antibody using an EMT-6 mammary tumor model showed that 7 out of 8 mice receiving a combination of CA4P and an anti-CTLA4
antibody experienced complete remission of their tumors, compared to only 1 of 8 in the CA4P monotherapy arm and 2 of 8 in the anti-
CTLA4 antibody monotherapy. This application is based on observed CA4P activity in melanoma in early clinical testing. During various
phase 1 studies, we found that CA4P treatment resulted in significant disease control among patients with solid tumors who progressed
on standard therapies. CA4P treatment resulted in 2 Stable Disease (SD) of 5 melanoma patients treated. One Partial Response (PR) was
observed of 6 melanoma patients treated follow progressing during first-line trial therapy with dacarbazine and sorafenib. Building on
the single agent activity of CA4P, we are expecting that combination of CA4P with Ipilimumab or other immune-oncology drug would result
in improved tumor control for the target pediatric population above the 2 PR out of 17 patients treated with Ipilimumab alone which supported
the approval of Ipilimumab in pediatric melanoma.
**OXi4503
for Acute Myeloid Leukemia**
OXi4503
(combretastatin A1-diphsphate; CA1P) is a novel investigational VDA that has been shown to have a significant in vitro cytotoxic as well
as chemo-sensitizing activity against human AML cells. OXi4503 also exhibited in vivo anti-leukemic activity in xenografted mice with
human AML.
OXi4503
employs a new, broader strategy against AML than currently exists for standard chemotherapy, as it provides a dual mechanism of action
involving both anti-vascular effects and direct cytotoxicity to AML cells. Vascular and/or Bone marrow endothelial cells (*ECs*)
appear to provide a protective effect for AML cells, keeping them dormant within the bone marrow. VDAs may target these ECs and reverse
their chemo protective effect, providing a novel approach to the treatment of AML which may otherwise be resistant to other chemotherapeutic
therapies. Preclinical data indicate that OXi4503 alone and in combination with traditional AML treatments such as cytarabine may provide
significant benefit in eliminating AML cells. Results from two completed Phase I clinical trials demonstrated the clinical impact potential
of OXi4503 against relapsed AML when it is alone or in combination with the standard chemotherapy drug cytarabine (*ARA-C*)
can induce complete remissions in relapsed AML patients. Notably, OXi4503 showed single agent activity in a clinical Phase I trial and
resulted in complete remission of a relapsed AML patient. Sustained complete remissions were also achieved in relapsed AML patients who
were treated with OXi4503 in combination with ARA-C.
OXi4503
has received orphan designation for AML in both the United States (Designation No. 12-3824) and the European Union (Designation No. EU/3/15/1587
- EMA/OD/144/15). In 2017, the FDA granted fast-track designation to OXi4503 for the treatment of relapsed/refractory AML. Oxi4503 met
the qualifying criteria for the Fast Track designation since AML is a serious and life-threatening condition, and a large unmet medical
need exists for additional treatment strategies for this disease.
The
Investigator-Sponsored trial (IST) UF OXi4503 AML MDS Ph 1 (UF4503), A Phase 1 Clinical Trial of OXi4503 for Relapsed and Refractory
AML and Myelodysplastic Syndromes (*MDS*) was designed to evaluate the safety profile and the maximum tolerated dose
(I) as well as a recommended Phase 2 dose (RP2D) of OXi4503 in patients with recurrent/refractory (R/R) AML and MDS (ClinicalTrials.gov
NCT01085656) (14, 50). The clinical single agent activity of OXi4503 was also assessed within the confines of a Phase 1 clinical trial
setting. A total of 18 patients enrolled in the study from February 2011 to January 2016. The patients were predominantly male (78%)
and the median age was 62.5 years. Of the 15 patients with AML, 4 (27%) had primary refractory AML, 2 (13%) were in first relapse, and
9 (60%) had refractory AML beyond CR1.
Eight
patients (44%) completed at least one cycle of CA1P and were evaluable for efficacy assessments. Of the eight patients evaluable, one
achieved morphologic remission with incomplete blood count recovery (*CRi*) after 1 cycle but came off study in cycle
2 due to fungal pneumonia. Three patients had stable disease after at least one cycle of CA1P. Three patients experienced progressive
disease after 1 cycle of CA1P and were withdrawn from the study.
The
Phase 1 dose-escalation combination of the Company sponsored study OX1222 (NCT02576301) was a Phase 1b dose escalation study of OXi4503
as a single agent and in combination with Cytarabine with subsequent combination Phase 2 cohorts for subjects with relapsed/refractory
(R/R) AML and MDS. 29 subjects were treated with OXi4503 in combination with Cytarabine.
| 5 | |
Of
these 29 patients, one was evaluable for safety analysis, but no EFS/OS data or response data were available for activity evaluations.
Of the 28 patients evaluable for EFS/OS outcome analyses, 26 had AML and 2 had MDS. For the 26 AML patients, there were 4 CRs. The CR
responses were associated with prolonged overall survival substantially better the median OS time: One patient who became eligible for
allogeneic PBSCT remains alive, free- of-leukemia at 720+ days. The overall survival times were 434 days, 521 days, 535 days, and 720
days, respectively. The median OS time for the 4 patients who achieved a CR/CRi was 528 (95% CI: 434 - NA) days which was significantly
better than the median OS time of 113 (95% CI: 77 - 172) days for the remaining 22 AML patients who did not achieve a CR (Log Rank =
11.8, P-value = 0.0006).
Three
of the 4 CR/CRis were achieved in 1st relapse patients while one patient with CRi had failed 5 previous regimens, including 7:3, HiDAC,
and PBSCT. Patients who achieved a CR/CRi went on to receive other treatments after receiving 4-6 cycles of OXi4503. The median OS for
all 26 AML patients who received therapy was 119 (95% CI: 87 - 232) days. Patients who had rapidly progressive disease or developed toxicity
could not get as many OXi4503 doses as patients who responded to their treatment favorably. The median OS time for 18 patients receiving
1-3 doses Of OXi4503 was 82 (95% CI: 66 - 135) days and these patients exhibited a worse survival outcome compared to 9 patients receiving
4-6 doses which was recorded at 434 (95% CI: 191 - NA) days (Log Rank = 12.3, P-value = 0.0004).
**OXi4503:
Pediatric AML**
Pediatric
AML is most common during the first 2 years of life and during the teenage years. In the United States, about 730 people under age 20
are diagnosed with AML each year. The number of deaths was 0.6 per 100,000 children per year. These rates are age-adjusted and based
on 2012-2016 cases.
Compared
with pediatric acute lymphoblastic leukemia (*ALL*), the outlook for pediatric AML patients is far worse. Even though
pediatric AML cases are far fewer than pediatric ALL, the mortality rate is about the same, illustrating that AML is a devastating disease
and the need for continuing research to identify effective treatments for these children. The prognosis for AML in children remains relatively
poor, with a 5-year survival rate of 64% compared with 90% in ALL.
Patients
with poor-risk cytogenetics include those that lack any favorable changes and harbor any of the following cytogenetic abnormalities:
monosomy 7, monosomy 5, deletion of 5q, abnormalities of 3q, t(6;9) (p23;q34), and complex karyotype which is defined as three or more
cytogenetic abnormalities. Children and adolescents harboring these unfavorable features have survival of less than 50 percent, and in
many cases less than 20 percent.
The
standard of care for management of pediatric AML involves predominantly induction therapy intended to put the patient into remission
and consolidation chemotherapy designed to eradicate leukemia cells that may have escaped front line induction therapy. Whereas >80%
of pediatric AML patients will achieve remission, only about half will remain disease-free for an appreciable period of time. Approximately
30 percent of children with AML will experience relapse and only one third of them become long-term survivors after salvage therapy.
Although cure rates for children and adolescents with AML have improved, outcomes for pediatric AML patients with adverse prognostic
biologic features (e.g., high risk genetic mutations or chromosomal abnormalities) and refractory or relapsed disease who failed or did
not respond to their initial standard induction chemotherapy remains poor and limited treatment options are available for these patients.
Novel therapies for these high-risk patients are urgently needed. OXi4503 shows clinical potential and promise for this indication based
on the proof-of-concept data obtained from nonclinical and clinical studies.
The
FDA has granted a RPD for OXi4503 for the treatment of pediatric AML.
**Developments
through our JV:**
**OT-101:
An Antisense Against TGF-2**
The
pharmaceutical development of OT-101 is being advanced through our JV. This is being reported here for informational purposes only.
| 6 | |
Trabedersen
(AP12009, OT-101) is a novel antisense oligodeoxynucleotide (*ODN*) developed by Oncotelic Inc. for the treatment
of patients with pancreatic carcinoma, malignant melanoma, colorectal carcinoma, high-grade glioma (*HGG*), and other
transforming growth factor beta 2 (*TGF-2*) overexpressing malignancies (e.g., prostate carcinoma, renal cell
carcinoma, etc.). Trabedersen is a synthetic 18-mer phosphorothioate oligodeoxynucleotide (*S- ODN*) complementary
to the messenger ribonucleic acid (*mRNA*) of the human TGF-2 gene.
TGF-
is a multifunctional cytokine with a key role in promoting tumor growth and progression including cell proliferation, cell migration,
and angiogenesis. Above all, TGF- is a highly potent immunosuppressive molecule. Inhibition of TGF- overexpression in tumor
tissue represents a novel multimodal treatment principle leading to the reduction of tumor growth, inhibition of metastasis, and restoration
of host antitumor immune responses. Despite its recognized pivotal role in cancer, therapeutics targeting TGF- have not been successful
and many have failed due to toxicity issues possibly due to inhibition of TGF-1 essential functions. The high level of homology
between the various TGF- isoforms is making it impossible to create mAb or small molecule inhibitor without TGF-1 cross-
inhibition. Therefore, Oncotelic Inc. chose to target TGF-2 only using OT-101 antisense approach. The sequence of OT-101 can only
target TGF-2 and does not have any impact on other TGF- isotypes. However, suppression of TGF-2 directly by OT-101
would also result in suppression of TGF-2 indirectly, but not TGF-3.
Trabedersen
is believed to reverse TGF-s immunosuppressive effects, rendering the tumor visible to a patients immune system and
resulting in priming and specific activation of the patients anti-tumor immune response. OT-101 has completed multiple clinical
trials with promising outcomes. OT-101, is being developed as a broad- spectrum anti-cancer drug that can also be used in combination
with other standard cancer therapies to establish an effective multi-modality treatment strategy for difficult-to-treat cancers. Oncotelic
plans to initiate phase 3 clinical trials for OT-101 in both high-grade glioma and pancreatic cancer. During phase 2 clinical trials
in pancreatic cancer, melanoma, and colorectal cancers (Study P001) and in high-grade gliomas (Study G004), meaningful single agent activity
with meaningful tumor reduction was observed, and OT-101 exhibited a favorable safety profile. Both partial and complete responses have
been observed in the G004 Phase 2 clinical trial of OT-101 as a single agent in patients with aggressive brain tumors.
Oncotelic
Inc.s, and now the JVs, self-immunization protocol (SIP) is based on the novel and proprietary sequential treatment
of cancers with OT-101 (antisense against TGF-2) and chemotherapies. Proper Sequencing of treatments is key to optimal immunotherapy.
Leveraging from its in-depth knowledge of TGF- immunotherapy, Oncotelic Inc. ordered the various treatments in the following sequence:
(1) expand immune reserve through IL-2 treatment or infusion of immune cells; (2) prime immune response with TGF- inhibitor OT-101;
(3) boost immune response with chemotherapy; and (4) revitalize the exhausted of immune response with checkpoint inhibitors. This sequential
treatment strategy is aimed at achieving effective self-immunization against a patients own cancer, resulting in robust therapeutic
immune response and consequently better control of the cancer and improved survival. Prolonged states of being cancer-free have been
observed in some patients with the most aggressive forms of cancer, raising a renewed hope for a potential cure. The use of OT-101 lifts
the suppression of the patients immune cells around the cancer tissue, providing the foundation for an effective initial priming,
which is critical for a successful immune response. The subsequent chemotherapy results in the release of neoantigens that result in
a robust boost of the immune response. This process is termed Xenogenization process and can be: (1) hypermutation by temozolomide in
the treatment of brain cancer, (2) immunogenic cell death by taxanes and 5FU in pancreatic cancer, or (3) necrotic cell death by VDA
(vascular disrupting agent) in melanoma and MDS. Additionally, the Company believes that a rational combination of the Oncotelic Inc.
SIP platform with immune-modulatory drugs like interleukin 2 (IL-2) and/or immune checkpoint inhibitors has the potential to help achieve
sustained and robust immune responses in patients with the most difficult-to-treat forms of cancer. The combinations with IL-2 and NK
are already partnered with external corporate partners. The Company entered into a JV with Dragon Overseas Capital Limited (Dragon
Overseas) and GMP Biotechnology Limited (GMP Bio), affiliates of GMP on March 31, 2022. GMP Bio and the Company
will focus to further expand the development of OT-101 for various oncology indications like pancreatic cancer, melanomas, gliomas etc.
as also for viral infections like COVID-19. This path is being evaluated as a monotherapy, as well as combination therapies in conjunction
with other drugs like checkpoint inhibitors.
| 7 | |
**Pancreatic
Cancer**
Pancreatic
cancer is associated with the poorest prognosis of gastrointestinal cancers and is expected to become the second leading cause of cancer-related
mortality in the USA by 2030. Pancreatic cancer is traditionally considered to be an immune-resistant disease. There is a lack of effector
T cells, an abundance of myeloid-derived suppressor T cells, and a dearth of key immune effector and regulatory cells. This may be part
of the reason why single-agent checkpoint inhibitors are not as effective in comparison to other diseases. Here is where breaking immune
tolerance by inhibiting TGF- with OT-101 will have a significant impact.
The
P001 trial was an open-label, multicenter dose-escalation study to evaluate the safety and tolerability of OT-101 (TGF-2-specific
Phosphorothioate Antisense Oligodeoxynucleotide) in adult patients with advanced tumors known to overproduce TGF- 2, which are
not or no longer amenable to established therapies. The primary objective of the study was to determine the maximum tolerated dose (MTD)
and the dose-limiting toxicities (DLTs) of two cycles of trabedersen administered intravenously (i.v.) on a 7-days-on/7-days-off or 4-days-on/10-days-off
schedule. Secondary objectives included were: (1) determining the safety and tolerability of OT-101 administered intravenously at weekly
intervals for four days every other week; (2) assessing the plasma pharmacokinetic profile of OT-101 administered intravenously at weekly
intervals and for four days every other week; (3) establishing a suitable determination method and to assess the urine pharmacokinetic
profile of OT-101 administered intravenously for four days every other week; (4) determining the effect of OT-101 administered intravenously
at weekly intervals and for four days every other week on TGF-2 plasma concentration levels; and (5) Assessing the potential antitumor
activity of OT-101 administered intravenously at weekly intervals and for four days every other week, as assessed by the effect on tumor
size and tumor markers.
Of
the 61 patients treated, 37 had advanced treatment failure pancreas cancer, a very difficult-to-treat cancer with an overall survival
rate that is measured in months even with the best available chemotherapy regimens. Globally, over 400,000 people die of pancreatic cancer
each year. MTD was not reached for the 4-days-on/10-days-off schedule, which became the schedule adopted for the phase 2 expansion phase
of the trial. Disease control (complete response (CR)), partial response (PR) or stable disease (SD)) was achieved in 19 of 35 evaluable
pancreas cancer patients (54%). Among liver mets only patients, there are exceptional single-agent activity and survival. Patient 1006
was pushed to complete response (CR) and survived as far out as 77 mos. This patient failed multiple lines of therapies: (1) surgery:
Whipples procedure, (2) 1st line: 5-FU/LV, Dose 425 mg/m2, (3) 2nd line: 5-FU/LV, Dose 2600 mg/m2/24hr, (4) 3rd line: Gemcitabine,
Dose 1000 mg/m2/week, and (5) went on to OT-101with liver mets and complete response. Patient 1022 was pushed to stable disease (*SD*)
with overall survival of 40 months. This patient had also failed multiple lines of therapies: (1) surgery: Whipples procedure,
(2) 1st line: radiation therapy (50 Gy), (3) 2nd line: 5FU, and (4) went on to OT-101 with liver mets and SD.
OT-101
treatment more than doubled the ratio of patients being able to go onto subsequent chemotherapy versus not being able, and consistent
with the expected immunization boost coming from Xenogenization with subsequent chemotherapies (taxanes and 5FU/Cisplatin) as discussed
for SIP, those with subsequent chemotherapy exhibited increased mOS and more than doubled their 1-year survival. Patients treated with
the non-SIP agent did not exhibit these properties.
The
JV initiated a Phase 2/3 clinical trial for pancreatic cancer and is actively seeking participants to enroll into the study. While enrollment
has been slow, due to a smaller patient population and the protocol, the JV is working hard to enroll patients and to complete the trial.
**Gliomas**
Brain
tumors in the United States are rare and only accounted for 2% of all adult cancers. However, the rate of brain tumors has been on the
rise for the last 30 years. The more common and most malignant form of brain tumors glioblastoma (*GBM*) has
more than doubled from 2.4 to 5.0 per 100,000. In the face of this increase, treatment remained essentially unchanged during the last
decade. And despite aggressive surgery followed by radiation and/or chemotherapy, GBM has the worst fiveyear survival rates among
all human cancers, with an average survival from diagnosis of only about 1 year and less than 5% of the patient survived after 5 years.
On top of it all, GBM will recur or regrow in most patients. Treatment of recurring a high-grade GBM that has recurred does not always
improve survival compared with hospice care alone and deciding when to stop treating the cancer and entering into hospice care is frequently
recommended when the patient is unlikely to live longer than six months.
| 8 | |
GBM
resilience and persistence is in stark contrast with the recent excitement in oncology where Immuno Oncology (*IO*)
agents have shown promise to be curative by driving the immune cells to attack the tumors. Though extraordinarily effective against the
growing number of tumors, IOs have been ineffective against GBM. GBM is generally considered immunologically cold with
few immune effector cells needed for successful immunotherapy. The overexpression of transforming growth factor-beta 2 (*TGF-2*)
is associated with poor prognosis of tumors and plays a key role in malignant progression of various tumors including GBM by inducing
proliferation, metastasis, angiogenesis, and immunosuppression. Oncotelic Inc. is developing a novel TGF-2 antisense agent OT-101
as immunotherapy against GBM.
G004
is a multinational, multicenter, open-label, randomized, active-controlled, parallel-group study in adult patients with either recurrent
or refractory AA (WHO grade III) or recurrent or refractory GBM (WHO grade IV). There were 3 treatment groups: (1) 10 M Trabedersen,
(2) 80 M Trabedersen, and (3) standard chemotherapy (mostly temozolomide). Tumor control rate at 6 months was the primary endpoint.
Response assessment included the tumor control rate and the overall response rate, which were assessed at 6, 12, and 14 months by central
MRI reading. The tumor control rate was defined as the percentage of patients with either CR, PR, or SD and the overall response rate
was defined as percentage of patients with either CR or PR. An independent blinded central MRI reading was performed to obtain a standardized
response assessment for the efficacy analysis. Central reading was performed by 2 independent neuroradiologists with an additional adjudicator
deciding in case of conflicting opinions.
All
patients had previous tumor surgery, almost all patients had previous radiation therapy, and more than half of the patients had received
previous chemotherapy. A total of 134 patients, 89 patients in the OT-101 test group and 45 patients in the standard chemotherapy control
group were assessed. The findings of a randomized Phase II study further confirmed the feasibility of intratumoral application of OT-101
via convection enhanced delivery (CED) for up to 6 months and showed that it results in early disease control at 6 months at a rate comparable
to that achieved with temozolomide. OT-101 was administered to 89 R/R high-grade glioma (HGG) (Anaplastic Astrocytoma/AA:27; Glioblastoma
multiforme/GBM: 62) patients with an intratumoral catheter using a convection enhanced delivery (CED) system. 77 patients (Efficacy population;
GBM: 51; AA: 26) received at least the intended minimum number of 4 OT-101 treatment cycles. Response determinations were based on central
review of MRI scans according to McDonald criteria. Standard statistical methods were applied for the analysis of data. Nineteen patients
had a complete response (CR) or partial response (PR) following a slow but robust size reduction of their target lesions. In addition,
7 patients had stable disease (SD) lasting 6 months. For the combined group of 26 AA/GBM patients with favorable responses, the median
PFS was >3 years and OS was >3.5 years (16, 17). Hence, OT-101 administered intratumorally exhibits clinically meaningful single-agent
activity and induces durable CR/PR/SD in R/R HGG patients. These results provided the proof of concept that targeting TGF2 with
intratumoral OT-101 therapy can result in a favorable survival outcome for R/R HGG patients (AA, WHO grade 3 and GBM, WHO Grade 4).
| 9 | |
****
**OT-101:
Pediatric DIPG**
DIPG,
the second most common malignant pediatric brain tumor, has a dismal outcome with available standard treatment modalities. No significant
therapeutic advances have been accomplished in the treatment of this poor prognosis brain tumor and the average overall survival has
remained <1 year with a 2-year survival rate of <10%. In solid tumors, the expression level of the TGF has been identified
as a significant contributor to disease progression and poor prognosis as well as resistance to standard therapy and metastasis. In particular,
TGF has been implicated in treatment resistance to targeted therapeutics, chemotherapy as well as immune-oncology drugs. Importantly,
TGF restrains anti-tumor immunity by restricting cytotoxic T-cell infiltration, recruiting regulatory T-cells, and inhibiting the
maturation as well as function of natural killer (*NK*) cells. Amplified activity of the TGF-Smad signaling
pathway enhances tumor growth, invasion, as well as angiogenesis and has been implicated in the malignant phenotype and poor prognosis
of high-grade gliomas in adults. Therefore, TGF- has emerged as an attractive target for the therapeutic intervention of high-grade
gliomas.
We
performed a meta-analysis of TGF2 gene expression in primary tumor specimens from 29 pediatric DIPG patients in the publicly available
archived datasets. Our data provided unprecedented evidence that TGF2 is expressed at high levels in pediatric DIPG. Three TGF2
probe sets exhibited 1.8-2.5-fold increased levels of expression in DIPG patients. Our meta-analysis provided new evidence that TGF2
gene and its interactome are expressed in pediatric DIPG at significantly higher levels than in normal tissues or low-grade gliomas.
Hence, TGF2 is an attractive molecular target for immunotherapy of pediatric DIPG.
The
US FDA granted the Company a RPD for pediatric DIPG, which was transferred to the JV as part of the JV Agreement. The Company is likely
to receive 50% of the value of the RPD, upto a maximum of $50 million, upon the RPD being sold to a third party should the JV decide
to do so.
**OT-101
for Treatment of Advanced or Metastatic Cancers**
****
In March 2025, the Company announced successfully completing a Phase 1 clinical trial evaluating OT-101, in combination with IL-2 for advanced or metastatic solid tumors,
on behalf of the JV. These results set the stage for new studies that combine OT-101, an antisense therapeutic targeting Transforming
Growth Factor Beta 2 (TGF2), with checkpoint inhibitors (CKIs) and recombinant IL-2 (aldesleukin) (IL-2).
The Phase 1 trial (ClinicalTrials.gov ID: NCT04862767) investigated the safety and tolerability of OT-101 in combination with recombinant
IL-2 in patients with advanced or metastatic solid tumors. The combination showed a tolerable safety profile at the planned dosing schedule,
with no unexpected safety signals identified. Based on the favorable safety data, the JV, through the Company, plans to advance OT-101
plus IL-2 into further clinical studies, exploring synergies with CKIs such as PD-1 blockers.
**OT-101
for Treatments of Corona Viruses**
A
Phase 2 study for COVID-19 was completed for OT-101 in South America, that can expand into a Phase 3 trial in the event there is a resurgence
in COVID-19. Based on the final results of the trial, the trial was planned to be expanded into a Phase 3 trial; however with the impact
of COVID-19 reducing in the past year, the Company will be re-evaluating this treatment for further development upon the occurrence or
recurrence of the COVID-19 or any similar virus. We were conducting an observational study, looking at OT-101 and long COVID-19, in conjunction
with the BARDA For more information on OT-101 for the treatment of Corona Viruses, refer
to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
**Additional
Nanoparticle Platform for Treatment of Various Cancers**
****
In
late 2023, the JV initiated a plan to start evaluating various nanoparticles that could treat various cancers. In this regard, the JV
identified a total of 4 compounds, in addition to OT-101, which had the potential of significant revenue generation for the JV. In the
same year, the JV signed a lease agreement to set up a GMP manufacturing facility in San Diego, California. The main purpose of this
facility was to initially commence an aggressive formulation development of newly planned nanoparticle platform (*Nano Platform*).
The GMP manufacturing facility was initiated in January 2024. Upon the initiation of this facility by the JV, the JV commenced the development
work on two of the four identified compounds, as well as other activities, in tandem with the development of OT-101.
| 10 | |
The
JV has since completed the formulation development of one of the products and is moving to complete the formulation development for the
three additional products. The JV is also working on improved formulations for OT-101 with new nanoparticle sizes. The JV also has started
clinical development for OT-101 for pancreatic cancer. Significant progress has been made in the development of the products and the
JV anticipates to complete the formulation development work in 2025 and pushing to initiate clinical trials for the various compounds.
In late
2024, the GMP facility in San Diego (*SD*), California was issued a Drug Manufacturing License by the State of California
Department of Public Health and Food and Drug Branch. Further, in late 2024, the JV identified a sixth candidate as a compound for development
for the JV and has already started to work on the formulation development of that compound as well. A lot of manufacturing, including
Phase 1 clinical trial materials, will be performed at the SD site.
In early 2025, we announced that
we had entered into a strategic partnership with Shanghai Medicilon, Inc. (*Medicilon*) to access its industry-leading
rapid investigational new drug (*IND*) development platform to support up to 20 IND projects. All six of our compounds
the JV is developing are planned to be these INDs, and are focused on next-generation anticancer agents.
The JV anticipates that all these
six anticancer agents have the potential to become significant growth contributors to the JV, which in turn would add substantial value
to the Company, as the Company is a 45% owner of the JV. Preliminary valuation assessment place this in significant multiples of the original
valuation of the JV, which could in turn mean a significant valuation for the Company. However, until there is a transaction to validate
the increase in the valuation, we will continue to measure the value of the Companys investment in the JV as was originally assessed
upon the formation of the JV.
**Artemisinin
for Treatment of COVID-19**
Artemisinin
derived from Chinese herb Artemisia annua L. (Sweet wormwood) has been used medicinally to treat fevers for centuries in China. Like
other potential COVID-19 therapeutic agents such as Hydrochloroquine and Remdesivir, the efficacy of Artemisinin remains to be tested
in well controlled and sufficiently powered clinical trials. With the impact of COVID-19 reducing in the past year, the Company will
be re-evaluating this treatment for further development upon the occurrence or recurrence of the COVID-19 or any similar virus. For more
information on Artemisinin for the treatment of COVID-19, refer to our Annual Report on Form 10-K filed with the SEC on April 14, 2023.
**Product
Portfolio for Treatment of Various Cancers**
****
The
JV is developing a range of products for the treatment of various cancers. One of the products is ready to enter into clinical trials
and other drugs are in various stages of development. The JV has evaluated the development process, as well as the appropriate regulatory
pathways, for the development of those drugs. The clinical pathway is also being designed for the other products. Individually, each
of the drug products has the potential to be successful drugs.
**AI/Blockchain:
PointR/EdgePoint**
**AI/Blockchain: PointR/EdgePoint**
****
PointR, an acquisition made in
November of 2019, develops, and deploys high performance cluster computers and artificial intelligence (*AI*) technologies
for inference processing of a camera-grid that are interconnected to create 360-degree vision-grid to track men and materials indoors.
The scope was expanded to include the entire life cycle of a drug: discovery, clinical trials, and manufacturing. In addition, AI is
being targeted to provide support for clinical trials and pre-clinical research. The deployment of AI technology for data capture and
insight extraction in real time in blocks which are chained into blockchain ledger records serving as immutable transactions for stakeholders
such as regulatory agencies, caretakers, insurers, payers, and manufacturers. For more information on AI/Blockchain, refer to our 2002
Annual Report on Form 10-K filed with the SEC on April, 14, 2023.
| 11 | |
**Manufacturing
AI Deployment:**
Leveraging its partnerships with industry leaders, the AI team plans to
combine its own AI technology with industry standard Blockchain to transform drug manufacturing. This will be advanced through our JV
at an appropriate time, as our JV has acquired non-exclusive rights to the technology.
**Market**
Human
labor costs represent the most expensive element in drug manufacturing. In the $70.0 billion CDMO (contract development manufacturing
operations) industry, personnel costs of $30 billion are ripe for computer automation. Until now, computer technologies like MRP and
ERP created more problems than resolved. The labor problem is compounded by the cost of personnel onboarding and turnover. It takes 6-9
months to train a quality control employee only to lose them to a competitor. At this time, this technology is being evaluated for being
upgraded for future uses. This will be advanced through our JV at an appropriate time, as our JV has acquired non-exclusive rights to
the technology. For more information on AI/Blockchain, refer to our 2002 Annual Report on Form 10-K filed with the SEC on April, 14,
2023.
**Go-to-Market:**
The
Companys go-to-market plan is to execute a proof-of-concept project, possibly through a planned CDMO by the JV. As part of the
JV Agreement, the JV has acquired a non-exclusive license for the AI platform developed by PointR/EdgePoint for implementation in a planned
CDMO. At this time, this technology is being evaluated for being upgraded for future uses. For more information on AI/Blockchain, refer to our
2002 Annual Report on Form 10-K filed with the SEC on April, 14, 2023.
| 12 | |
****
**Our
Strategy and Development Plan**
We
have been operating with significant capital constraints since the reverse merger between the Company and Oncotelic Inc, and for this
time period we have been seeking to secure sufficient funding to continue our operations while we simultaneously seek to advance our
all our investigational drugs for the treatment of cancer, coronaviruses, AI technology and more recently for PD, ED and FSD. Subject
to our ability to secure additional capital, we would seek to further develop our product candidates. However, our inability to access
capital historically has and may significantly impair our ability to develop these compounds. If we are able to advance any or all of
our drug candidates, we would seek to develop them till commercialization, however, there is no guarantee that we would be able to fully
develop our products, obtain regulatory approvals and successfully commercialize them.
We continue to discuss collaboration opportunities with other biopharmaceutical
companies, although to date have not secured any agreements with companies that are willing to purchase the products from us or license
the development and commercialization rights. We intend to continue to seek a partner to acquire the marketing rights to our product candidates
and to finance further clinical studies and will seek to complete a transaction if we are able to reach mutual agreement on terms. In
this connection, in March 2022, the Company entered into a JV with Dragon to form GMP Bio. Both entities are affiliates of GMP. GMP Bio
and the Company will work together to further the development of OT-101, wherein the Company would provide the technology and technical
expertise and GMP Bio would fund the development expenses. In December 2023, the JV initiated a GMP manufacturing facility in San Diego,
California to develop several drug candidates, which individually and collectively, could bring significant value to the JV as well as
to the Company, which was approved in the fourth quarter of 2024. 
In
addition to entering into transaction that would provide funding for the further development of the rest of our product candidates, other
elements of our development strategy would currently include:
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Initiating
clinical trials of OT-101, and various other drugs, in various cancers through our JV: We have initiated one trial for OT-101, and
we are evaluating conducting such trials in the US as well as other countries like China in conjunction with GMP Bio. We are looking
to conduct such trials in combination with other drugs like checkpoint inhibitors. We have filed the protocols for some of the trials
being planned and we hope to be able to get acceptance from the FDA and be able to initiate the trials shortly thereafter. In addition,
the JV is also working on the initiation of clinical trials for the other drugs, in various stages of development and through various
regulatory pathways. | |
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Initiating
a clinical trial of CA4P in combination with an immuno-oncology agent or seek any collaboration for the development of CA4P. | |
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Continuing
to evaluate OXi4503 in a clinical trial or seek any collaboration for the development of OXi4503. | |
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Ramping
up the apomorphine development program and initiating noninferiority trial comparing AL-101 against subcutaneous apomorphine for
the treatment of PD. We are also considering ramping up the apomorphine development programs for ED and FSD/HSDD. The development
of these products is subject to the Company being able to raise funding to support the development activities or being able to partner
with a third party to co-develop or even any type of a transaction that permits the Company to capitalize on the assets. | |
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The
Company formed Pet2DAO, as a wholly owned subsidiary. Pet2DAO is a DAO technology company,
integrating the strong governance of traditional corporations with the innovative DAO architecture looking to engage stakeholders,
to build value through the DAO, while maintaining the rigor of traditional corporations, including governance, compliance, and accountability
through a team of veterans in public companies with innovators in AI, blockchain and Web3.
Pet2DAO will initially be looking to develop products for the animal health space. | |
| 13 | |
****
**REGULATORY
MATTERS**
**Government
Regulation and Product Approval**
Government
authorities in the United States and other countries extensively regulate, among other things, the research, development, testing, manufacture,
quality control, approval, labeling, packaging, storage, record-keeping, promotion, advertising, distribution, marketing and export and
import of products such as those we are developing. Our drug candidates must be approved by the FDA through the New Drug Application
(*NDA*), process before they may be legally marketed in the United States.
**U.S.
Drug Development Process**
In
the United States, the FDA regulates drugs under the Federal Food, Drug, and Cosmetic Act (*FDCA*), and implementing
regulations. The process of obtaining regulatory approvals and the subsequent compliance with appropriate federal, state, local, and
foreign statutes and regulations require the expenditure of substantial time and financial resources. Failure to comply with the applicable
United States requirements at any time during the product development process, approval process or after approval, may subject an applicant
to administrative or judicial sanctions. These sanctions could include the FDAs refusal to review or approve pending applications,
withdrawal of an approval, a clinical hold, warning letters, product recalls, product seizures, total or partial suspension of production
or distribution injunctions, fines, refusal of government contracts, restitution, disgorgement, or civil or criminal penalties. Any agency
or judicial enforcement action could have a material adverse effect on us. The process required by the FDA before a drug may be marketed
in the United States generally involves the following:
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completion
of preclinical laboratory tests, animal studies and formulation studies according to Good Laboratory Practices (GLP)
or other applicable regulations; | |
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submission
to the FDA of an Investigational New Drug Application, or IND, which must be first approved by the FDA before human clinical trials
may begin; | |
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performance
of adequate and well-controlled human clinical trials according to Good Clinical Practices (GCP) to establish
the safety and efficacy of the proposed drug for its intended use; | |
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submission
to the FDA of an NDA; | |
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satisfactory
completion of an FDA inspection of the manufacturing facility or facilities at which the drug is produced to assess compliance with
current good manufacturing practice, or cGMP, to assure that the facilities, methods and controls are adequate to preserve the drugs
identity, strength, quality and purity; | |
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satisfactory
completion of FDA inspections of clinical sites and GLP toxicology studies; and | |
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FDA
review and approval of the NDA. | |
The
testing and approval process requires substantial time, effort and financial resources, and we cannot be certain that any approvals for
our product candidates will be granted on a timely basis, if at all.
Once
a pharmaceutical candidate is identified for development, it enters the preclinical testing stage. Preclinical tests include laboratory
evaluations of product chemistry, toxicity, and formulation, as well as animal studies. An IND sponsor must submit the results of the
preclinical tests, together with manufacturing information and analytical data, to the FDA as part of the IND. The sponsor will also
include a protocol detailing, among other things, the objectives of the clinical trial, the parameters to be used in monitoring safety,
and the effectiveness criteria to be evaluated, if the first phase lends itself to an efficacy evaluation. Preclinical testing continues
even after the IND is submitted. The IND becomes effective 30 days after receipt by the FDA, unless the FDA, within the 30-day time period,
places the clinical trial on a clinical hold. In such a case, the IND sponsor and the FDA must resolve any outstanding concerns before
the clinical trial can begin. Clinical holds also may be imposed by the FDA at any time before or during clinical trials due to safety
concerns or non-compliance.
| 14 | |
All
clinical trials must be conducted under the supervision of qualified investigators in accordance with GCP regulations. These regulations
include the requirement that all research subjects provide informed consent. Further, an institutional review board, or IRB, must review
and approve the plan for any clinical trial before it commences at any institution. An IRB considers, among other things, whether the
risks to individuals participating in the trials are minimized and are reasonable in relation to anticipated benefits. The IRB also approves
the information regarding the trial and the consent form that must be provided to each trial subject or his or her legal representative
and must monitor the clinical trial until completed.
Each
new clinical protocol must be submitted to the IND for FDA review, and to the IRBs for approval. Protocols detail, among other things,
the objectives of the clinical trial, dosing procedures, subject selection and exclusion criteria, and the parameters to be used to monitor
subject safety and efficacy in Phase 2 and 3 clinical trials.
Human
clinical trials are typically conducted in three sequential phases that may overlap or be combined:
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Phase
1: The drug is initially introduced into human subjects and tested for safety, dosage tolerance, absorption, metabolism, distribution,
and excretion. | |
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Phase
2: Involves clinical trials in a limited patient population to identify possible adverse effects and safety risks, to evaluate preliminary
efficacy of the product for specific targeted diseases and to determine dosage tolerance and optimal dosage. | |
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Phase
3: Clinical trials are undertaken to further evaluate dosage, clinical efficacy, and safety in an expanded patient population. These
studies are intended to establish the overall risk-benefit ratio of the product and provide, if appropriate, an adequate basis for
product labeling. | |
Progress
reports detailing the results of the clinical trials must be submitted at least annually to the FDA. IND Safety Reports must be submitted
to the FDA, IRBs and the investigators for (a) any suspected adverse reaction that is both serious and unexpected; (b) any findings from
epidemiological studies, pooled analysis of multiple trials, or clinical trials (other than those already reported in (a)); (c) any findings
from animal or *in vitro* testing, whether or not conducted by the sponsor, that suggest a significant risk in humans exposed to
the drug, such as reports of mutagenicity, teratogenicity, or carcinogenicity or reports of significant organ toxicity at or near the
expected human exposure; and (d) any clinically important increase in the rate of a serious suspected adverse reaction over that listed
in the protocol or investigator brochure. Phase 1, phase 2, and phase 3 testing may not be completed successfully within any specified
period, if at all. The FDA or the sponsor may suspend a clinical trial at any time on various grounds, including a finding that the research
subjects or patients are being exposed to an unacceptable health risk. Similarly, an IRB can suspend or terminate approval of a clinical
trial at its institution if the clinical trial is not being conducted in accordance with the IRBs requirements or if the drug
has been associated with unexpected serious harm to patients.
Concurrent
with clinical trials, companies usually complete additional animal studies and must also develop additional information about the chemistry
and physical characteristics of the drug and finalize a process for manufacturing the product in commercial quantities in accordance
with cGMP requirements. The manufacturing process must be capable of consistently producing quality batches of the product candidate
and, among other things, the manufacturer must develop methods for testing the identity, strength, quality and purity of the final drug.
Additionally, appropriate packaging must be selected and tested, and stability studies must be conducted to demonstrate that the product
candidate does not undergo unacceptable deterioration over its shelf life.
Entities
can also follow the 505(b)(2) pathway to regulatory approval, to further drug development in a more efficient and relatively cost effective
manner. The 505(b)(2) pathway is a regulatory route in the United States under the Federal Food, Drug, and Cosmetic Act (FDCA) that allows
for the approval of new drugs that are similar to already approved products. It is often used for drugs that have been previously approved
but require modifications, such as new indications, dosages, formulations, or routes of administration. The 505(b)(2) pathway provides
a more efficient approval process compared to the traditional New Drug Application (NDA) pathway, as it allows drug developers to rely
on existing data from previously approved drugs instead of conducting all new clinical trials. It strikes a balance between the full
NDA process and the Abbreviated New Drug Application (ANDA) for generics.
| 15 | |
Key
Features of the 505(b)(2) Pathway includes (1) allowing applicants to use published literature or data from previous studies, like studies
conducted by the original sponsor or from publicly available sources, to support their application, rather than having to repeat all
of the clinical trials. This can include data from the reference product, studies published in scientific literature, or data from other
regulatory agencies; (2) used for new formulations, like changing the dosage forms, routes of administration, new combinations of active
ingredients. It may also be used for new indications for an existing drug; (3) allows for faster approval than a full NDA because it
leverages existing data. It can be especially useful when the applicant needs to add new data or modify an already approved drug; and
(4) while the application uses data from an existing product, the 505(b)(2) pathway is not for generic drugs. A 505(b)(2) submission
often involves new clinical data or modifications that distinguish it from the original approved drug. The benefits of the 505(b)(2)
pathway to drug approval include:
| 
1. | Reduced
Clinical Trial Requirements: Instead of generating a complete set of new clinical trials,
or a significantly reduced patient population for clinical trials, applicants can use existing
data (like data from the original product or published studies), saving time and costs. | |
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2. | Innovation
and Flexibility: It allows drug developers to bring innovative new formulations, combinations,
or indications to market more quickly, which can help improve patient care. | |
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3. | Cost-Efficiency:
It can reduce the cost of development for drug companies, as it may reduce the time and amount
of clinical data they need to generate. | |
**U.S.
FDA Review and Approval Processes**
The
results of product development, preclinical studies and clinical trials, along with descriptions of the manufacturing process, analytical
tests conducted on the chemistry of the drug, proposed labeling, and other relevant information are submitted to the FDA as part of an
NDA requesting approval to market the product. The submission of an NDA is subject to the payment of user fees; a waiver of such fees
may be obtained under certain limited circumstances, which may include orphan drug status and the first NDA application for a company.
In
addition, under the Pediatric Research Equity Act, or PREA, an NDA or supplement to an NDA must contain data to assess the safety and
effectiveness of the drug for the claimed indications in all relevant pediatric subpopulations and to support dosing and administration
for each pediatric subpopulation for which the drug is safe and effective. The FDA may grant deferrals for submission of data or full
or partial waivers. Unless otherwise required by regulation, PREA does not apply to any drug for an indication for which orphan designation
has been granted.
The
FDA reviews all NDAs submitted to ensure that they are sufficiently complete for substantive review before it accepts them for filing.
The FDA may request additional information rather than accept an NDA for filing. In this event, the NDA must be resubmitted with the
additional information. The resubmitted application also is subject to review before the FDA accepts it for filing. Once the submission
is accepted for filing, the FDA begins an in-depth substantive review. The FDA also may refer the NDA to an advisory committee for review,
evaluation, and recommendation as to whether the application should be approved and under what conditions. The FDA is not bound by the
recommendation of an advisory committee, but it generally follows such recommendations. The approval process is lengthy and difficult,
and the FDA may refuse to approve an NDA at its discretion, or the FDA may require additional clinical or other data and information.
Even if such additional data and information are submitted, the FDA may ultimately decide that the NDA does not satisfy its criteria
for approval. Data obtained from clinical trials is not always conclusive, and the FDA may interpret data differently than we or others
may interpret the same data. The FDA may issue a complete response letter, which may require additional clinical or other data or impose
other conditions that must be met in order to obtain approval of the NDA. The FDA reviews an NDA to determine, among other things, whether
a product is safe and effective for its intended use and whether its manufacturing is cGMP- compliant to assure and preserve the products
identity, strength, quality, and purity. Before approving an NDA, the FDA will generally inspect the facility or facilities where the
product is manufactured. The FDA will also generally inspect selected clinical sites that participated in the clinical studies and may
inspect the testing facilities that performed the GLP toxicology studies cited in the NDA.
| 16 | |
NDAs
receive either standard or priority review. A drug representing a significant improvement in treatment, prevention or diagnosis of disease
may receive priority review. In addition, products studied for their safety and effectiveness in treating serious or life-threatening
illnesses and that provide meaningful therapeutic benefit over existing treatments may receive accelerated approval and may be approved
on the basis of adequate and well- controlled clinical trials establishing that the drug product has an effect on a surrogate endpoint
that is reasonably likely to predict clinical benefit or on the basis of an effect on a clinical endpoint other than survival or irreversible
morbidity. As a condition of approval, the FDA may require that a sponsor of a drug receiving accelerated approval perform adequate and
well-controlled post-marketing clinical trials. Priority review and accelerated approval do not change the standards for approval but
may expedite the approval process.
If
a product receives regulatory approval, the approval may be limited to specific diseases or patient subpopulations and dosages or the
indications for use may otherwise be limited, which could restrict the commercial value of the product. In addition, approval by the
FDA may include a requirement for phase 4 testing, which involves clinical trials designed to further assess a drugs safety and
effectiveness, and the FDA may require testing and surveillance programs to monitor the safety of approved products which have been commercialized.
If
an applicant decides to follow the 505(b)(2) pathway to regulatory approval for a drug, then the applicant is required to (1) request
meetings with the FDA to discuss the appropriate use of existing data and the studies they need to conduct for approval (2) submits the
505(b)(2) application, which includes clinical trial data, published studies, and other relevant data (3) The FDA reviews the data to
assess the safety, effectiveness, and quality of the drug, considering any new information provided (4) If the FDA is satisfied with
the data, it will approve the new drug or formulation. If not, additional data or studies may be requested.
**Orphan
Drug Designation**
Under
the Orphan Drug Act, the FDA may grant orphan drug designation to a drug intended to treat a rare disease or condition, which is generally
a disease or condition that affects fewer than 200,000 individuals in the United States. After the FDA grants orphan drug designation,
the identity of the therapeutic agent and its potential orphan use are disclosed publicly by the FDA. Orphan drug designation does not
convey any advantage in or shorten the duration of the regulatory review and approval process.
If
a product that has orphan drug designation subsequently receives the first FDA approval for the disease for which it has such designation,
the product is entitled to orphan product exclusivity, which means that the FDA may not approve any other applications to market the
same drug for the same indication for seven years, except in very limited circumstances.
In
the European Union and Japan, orphan drug exclusivity regulations provide for 10 years of market exclusivity.
CA4P
has been awarded orphan drug status by the FDA for the treatment of anaplastic, medullary, Stage IV papillary and Stage IV follicular
thyroid cancers, ovarian cancer, neuroendocrine tumors, and glioma. OXi4503 has been awarded orphan drug status by the FDA for the treatment
of acute myelogenous leukemia. CA4P has been awarded orphan drug status by the FDA for the treatment of pancreatic cancer, melanoma,
and glioblastoma.
CA4P
has also been awarded orphan drug status by the European Commission in the European Union for the treatment of anaplastic thyroid cancer,
ovarian cancer and neuroendocrine tumors. OXi4503 has been awarded orphan drug status by the European Commission in the European Union
for the treatment of acute myelogenous leukemia. OT-101 has been awarded orphan drug status by the European Commission in the European
Union for the treatment of pancreatic cancer, melanoma, and glioblastoma.
| 17 | |
**Rare
Pediatric Disease Designation**
The
FDA grants rare pediatric disease designation for diseases with serious or life-threatening manifestations that primarily affect people
aged from birth to 18 years, and that affect fewer than 200,000 people in the U.S. Under the FDAs Rare Pediatric Disease Priority
Review Voucher program, a sponsor who receives an approval of a new drug application or biologics license application for a product for
the prevention or treatment of a rare pediatric disease may be eligible for a voucher, which can be redeemed to obtain priority review
for any subsequent marketing application and may be sold or transferred. Such vouchers can be valued at several millions of dollars,
sometimes in excess of $100 million.
The
FDA granted Rare Pediatric Disease Designation for OT-101/Trabedersen for the treatment of DIPG as a drug for a rare pediatric disease.
The
FDA granted Rare Pediatric Disease Designation for CA4P/ Fosbretabulin tromethamine for the treatment of stage IIBIV melanoma
due to genetic mutations that disproportionately affect pediatric patients as a drug.
The
FDA granted Rare Pediatric Disease Designation for Oxi4503 for the treatment of AML as a drug for a rare pediatric disease.
**Expedited
Review and Approval**
The
FDA has various programs, including Fast Track, priority review, accelerated approval and breakthrough therapy, which are intended to
expedite or simplify the process for reviewing drugs, and/or provide for approval on the basis of surrogate endpoints. Even if a drug
qualifies for one or more of these programs, the FDA may subsequently decide the drug no longer meets the conditions for qualification
or the FDA may not shorten the review or approval time period. Generally, drugs that may be eligible for these programs are those for
serious or life-threatening conditions, those with the potential to address unmet medical needs, and those that offer meaningful benefits
over existing treatments. Fast Track designation applies to the combination of the product and the specific indication for which it is
being studied. Although Fast Track and priority review do not affect the standards for approval, the FDA will attempt to facilitate early
and frequent meetings with a sponsor of a Fast-Track designated drug and expedite review of the application for a drug designated for
priority review. Drugs that receive an accelerated approval may be approved on the basis of adequate and well-controlled clinical trials
establishing that the drug product has an effect on a surrogate endpoint that is reasonably likely to predict clinical benefit or on
the basis of an effect on a clinical endpoint other than survival or irreversible morbidity. As a condition of approval, the FDA may
require that a sponsor of a drug receiving accelerated approval perform post-marketing clinical trials.
OXi4503
has been awarded Fast Track designation for the treatment of AML.
**Foreign
Regulation**
In
addition to regulations in the United States, we are subject to a variety of foreign regulations governing clinical trials and if any
of our product candidates are approved, we will be subject to additional regulations regarding commercial sales and distribution. Whether
or not we obtain FDA approval to test a product candidate in the United States, we must obtain approval by the comparable regulatory
authorities of foreign countries before we can commence testing any product candidate in those countries. Likewise, whether we obtain
FDA approval to market a product, we must obtain approval by the comparable regulatory authorities of foreign countries before we can
commence marketing of any product candidate in those countries. The approval process varies from country to country and the time may
be longer or shorter than that required for FDA approval. The requirements governing the conduct of clinical trials, product licensing,
pricing and reimbursement vary greatly from country to country.
Under
European Union regulatory systems, a company may submit marketing authorization applications, or MAAs, either under a centralized or
decentralized procedure. The centralized procedure, which is compulsory for medicines produced by biotechnology, or those medicines intended
to treat AIDS, cancer, neurodegenerative disorders or diabetes and optional for those medicines which are highly innovative, provides
for the grant of a single marketing authorization that is valid for all European Union member states. The decentralized procedure provides
for mutual recognition of national approval decisions. Under this procedure, the holder of a national marketing authorization may apply
to the remaining member states. Within 90 days of receiving the applications and assessments report, each member state must decide whether
to recognize approval. If a member state does not recognize the marketing authorization, the disputed points are eventually referred
to the European Commission, whose decision is binding on all member states.
| 18 | |
As
in the United States, the European Medicines Agency, or EMA, may grant orphan drug status for specific indications if the request is
made before an MAA is submitted. The EMA considers an orphan medicinal product to be one that affects less than five of every 10,000
people in the European Union. A company whose application for orphan drug designation in the European Union is approved is eligible to
receive, among other benefits, regulatory assistance in preparing the marketing application, protocol assistance and reduced application
fees. Orphan drugs in the European Union receive up to ten years of market exclusivity for the approved indication.
**Reimbursement**
Sales
of any of our product candidates, if approved, will depend, in part, on the extent to which the costs of the products will be covered
by third-party payors, including government health programs such as Medicare and Medicaid, commercial health insurers and managed care
organizations. These third-party payors are increasingly challenging the prices charged for health care products and services. The U.S.
government, state legislatures and foreign governments have shown significant interest in implementing cost-containment programs, including
price controls, restrictions on reimbursement and requirements for substitution of generic products. The adoption or application of price
controls and cost-containment measures could limit our revenue. If third-party payors do not consider our products to be cost-effective,
they may not pay for our products even if we receive approval, or their level of payment may not be sufficient to allow us to sell our
products on a profitable basis.
The
Medicare Prescription Drug, Improvement, and Modernization Act of 2003, or the MMA, imposes requirements for the distribution and pricing
of prescription drugs for Medicare beneficiaries. Under Part D (the Medicare prescription drug benefit), Medicare beneficiaries may enroll
in prescription drug plans offered by private entities that provide coverage of outpatient prescription drugs not covered under Medicare
Part B. Part D prescription drug plan sponsors are not required to pay for all covered Part D drugs. Each drug plan can develop its own
drug formulary that identifies which drugs it will cover and at what tier or level. Federal regulations require Part D prescription drug
formularies to include drugs within each therapeutic category and class of covered Part D drugs, although not necessarily all the drugs
in each category or class.
In
general, government payment for some of the costs of prescription drugs may increase demand for products for which we receive marketing
approval. However, any negotiated prices for our products covered by a Part D prescription drug plan will likely be lower than the prices
we might otherwise obtain. Moreover, while the MMA applies only to drug benefits for Medicare beneficiaries, private payors often follow
Medicare coverage policy and payment limitations in setting their own payment rates. Any reduction in payment that results from the MMA
or other Medicare regulations may result in a similar reduction in payments from non-governmental payors.
The
Patient Protection and Affordable Care Act and the Health Care and Education Affordability Reconciliation Act of 2010 (collectively,
the *Affordable Care Act* or *ACA*) mandated prescription drug coverage as one of ten essential
health benefits that most health plans must offer, requiring coverage of at least one drug in every category and class. The ACA increased
in the number of individuals covered by insurance and as a result commercial insurers and government programs have increased their emphasis
on cost controls to reduce overall spending. A number of federal government leaders have expressed their intentions to repeal and replace
the ACA. If full or partial repeal is enacted, many if not all the provisions of the ACA may no longer apply to prescription drugs. As
a result, we expect that there will continue to be uncertainty regarding drug product pricing, reimbursement and other factors impacting
the revenue we may receive if our product candidates are ultimately approved, which could have a material adverse effect on our business,
financial condition, and results of operations.
In
addition, in some foreign countries, the proposed pricing for a drug must be approved before it may be lawfully marketed. The requirements
governing drug pricing vary widely from country to country. For example, the European Union provides options for its member states to
restrict the range of medicinal products for which their national health insurance systems provide reimbursement and to control the prices
of medicinal products for human use. A member state may approve a specific price for the medicinal product, or it may instead adopt a
system of direct or indirect controls on the profitability of the company placing the medicinal product on the market. There can be no
assurance that any country that has price controls or reimbursement limitations for pharmaceutical products will allow favorable reimbursement
and pricing arrangements for any of our products. Historically, products launched in the European Union do not follow price structures
of the United States and tend to be significantly lower.
| 19 | |
**PATENTS
AND PROPRIETARY RIGHTS**
We
actively seek to protect the proprietary technology that we consider important to our business, including chemical species, compositions
and forms, their methods of use and processes for their manufacture, as well as modified forms of naturally-expressed receptors, in the
United States and other jurisdictions internationally that we consider key pharmaceutical markets. We also rely upon trade secrets and
contracts to protect our proprietary information.
As
of April 14, 2025, we were the exclusive licensee, sole assignee or co-assignee of five granted U.S. patents, two pending U.S.
patent application, and granted patents and/or pending applications in several other major markets, including the European Union,
Canada and Japan. Our policy is to file U.S. and foreign patent applications to protect technology, inventions and improvements to
inventions that are commercially important to the development of our business. There can be no assurance that any of these patent
applications will result in the grant of a patent either in the United States or elsewhere, or that any patents granted will be
valid and enforceable or will provide a competitive advantage or will afford protection against competitors with similar
technologies. We also intend to rely upon trade secret rights to protect other technologies that may be used to discover and
validate targets and that may be used to identify and develop novel drugs. We seek protection, in part, through confidentiality and
proprietary information agreements.
We
consider the following U.S. patents and applications owned by or exclusively licensed to us to be particularly important to the protection
of our most advanced product candidates.
| 
Product
Candidate | 
| 
Patent
Scope | 
| 
Patent
Expiration | |
| 
CA4P | 
| 
Use
of VDAs to Enhance Immunomodulating Therapies Against Tumors | 
| 
August
2036 | |
| 
| 
| 
| 
| 
| |
| 
OT-101
through our JV | 
| 
Combination
of A Chemotherapeutic Agent and An Inhibitor of the TGF- System | 
| 
July
2030 to | |
| 
| 
| 
Combination
Therapy for Treatment of Pancreatic Cancer | 
| 
February
2036 | |
| 
| 
| 
Compositions
and Methods for Treating Cancer | 
| 
February
2036 | |
In
addition to these patents, for some of our product candidates, we have patents and/or applications that cover a particular form or composition,
use for a particular indication, use as part of combination therapy or method of preparation or use, as well as other pending patent
applications. These issued patents, including any patents that issue from pending applications, could provide additional or a longer
period of protection. We also have patent applications pending that seek equivalent or substantially comparable protection for our product
candidates in jurisdictions internationally that we consider key pharmaceutical markets.
The
patent expiration dates referenced above do not reflect any potential patent term extension that we may receive under the federal Drug
Price Competition and Patent Term Restoration Act of 1984, known as the Hatch- Waxman Act. The Hatch-Waxman Act generally permits a patent
extension term of up to five years as compensation for patent term lost during the FDA regulatory review process. Patent extension cannot
extend the remaining term of a patent beyond a total of 14 years. The patent term restoration period is generally one-half of the time
between the effective date of an investigational new drug application, or IND, and the submission date of a new drug application, or
NDA, plus the time between the submission date and approval date of an NDA. Only one patent applicable to an approved drug is eligible
for the extension, and the extension must be applied for prior to expiration of the patent. The United States Patent and Trademark Office,
in consultation with the FDA, reviews and approves applications for patent term extension.
As
previously noted, the FDA and European Union have granted CA4P and OXi4503 orphan drug status for certain indications. We are also pursuing,
and may continue to in the future to pursue, orphan drug status for other product candidates and indications. Our ability to obtain and
maintain the exclusivity for our products and product candidates by virtue of their orphan drug status is an important part of our intellectual
property strategy. Also as previously noted, we are emphasizing Rare Pediatric Designation to leverage on the regulatory exclusivity
and voucher program associated with these designations.
| 20 | |
**COMPETITION**
The
industry in which we are engaged is characterized by rapidly evolving technology and intense competition. Our competitors include, among
others, major pharmaceutical, biopharmaceutical and biotechnology companies, nearly all of which have financial, technical, and marketing
resources significantly greater than ours. In addition, many of the small companies in our industry have also formed collaborative relationships
with large, established companies to support research, development and commercialization of products that may be competitive with ours.
Academic institutions, governmental agencies and other public and private research organizations are also conducting research activities
and patenting new technologies in our line of business and any of these entities may commercialize products that may be competitive with
ours.
We
expect that, if any of our products gain regulatory approval for sale, they will compete primarily on the basis of product efficacy,
safety, patient convenience, reliability, price and patent protection. Our competitive position will also depend on our ability to attract
and retain qualified scientific and other personnel, develop effective proprietary products, and implement joint ventures or other alliances
with large pharmaceutical companies in order to jointly market and manufacture our products.
**EMPLOYEES**
We
had twenty-six full-time employees, four part-time employees and 10 consultants as of December 31, 2024; and all the employees and consultants
were compensated by the JV during the years ended December 31, 2024 and 2023, respectively. We rely on external consultants or outsource
nearly all our research, development, preclinical testing, and clinical trial activity, although we maintain managerial and quality control
over our clinical trials. We also rely on external consultants for various administrative tasks that are required for a public company.
We expect to continue to rely on external service providers and to maintain a small number of executives and other employees. Our relations
with our employees are good and we do not have any unions for the Company.
**COSTS
OF COMPLIANCE WITH ENVIRONMENTAL REGULATIONS**
We
have not incurred any costs associated with compliance with environmental regulations, nor do we anticipate any future costs associated
with environmental compliance; however, no assurances can be given that we will not incur such costs in the future.
**ITEM
1A. RISK FACTORS**
*Investing
in our common stock involves a high degree of risk. You should carefully consider the risks described below, as well as the other information
in this Annual Report, including our financial statements and the related notes thereto and Managements Discussion and
Analysis of Financial Condition and Results of Operations, before deciding whether to invest in our common stock. The occurrence
of any of the events or developments described below could harm our business, financial condition, operating results, and growth prospects.
In such an event, the market price of our common stock could decline, and you may lose part or all of your investment. Additional risks
and uncertainties not presently known to us or that we currently deem immaterial also may impair our business operations.*
| 21 | |
****
**RISKS
RELATED TO OUR BUSINESS AND INDUSTRY**
**If
we are unable to obtain additional funding, we may be forced to cease operations.**
We
have experienced net losses every year since inception. In April 2019, the Company entered into an Agreement and Plan of Merger with
Oncotelic Inc. for developing investigational drugs for the treatment of orphan oncology indications. The Company completed the Merger
and Oncotelic Inc. became a wholly-owned subsidiary of the Company. The Merger was treated as a recapitalization and reverse acquisition
for financial accounting purposes. Oncotelic was considered the acquirer for accounting purposes, and the Companys historical
financial statements before the Merger have been replaced with the historical financial statements of Oncotelic Inc. prior to the Merger
in the financial statements and filings with the Securities and Exchange Commission.
The
Company, as of December 31, 2024, had an accumulated deficit of approximately $38.0 million, including a net loss of approximately $4.8
million in 2024, which included a non-cash goodwill impairment loss of $3.2 million. We have no source of product revenue and do not
expect to receive any product revenue in the near future, except if we generate product revenues from Artemisinin in countries around
the globe other than India and which at the current time is not anticipated. We may generate revenues from services rendered in the future,
but we cannot expect that to be of a regular and of a recurring nature. If we remain in business, we expect to incur additional operating
losses over the next several years, principally as a result of our plans to continue clinical trials for our investigational drugs. As
of December 31, 2024, we had approximately $0.1 million in cash and current liabilities of approximately $16.9 million, of which $1.3
million pertains to Mateons liabilities prior to the Merger and $2.6 million of contingent liabilities, incurred upon our merger
with PointR Data, Inc. in November 2019, that would be issuable in shares of common stock of the Company to the PointR shareholders upon
satisfaction of certain conditions. Based on our planned operations, we expect our cash to only support our operations for a short period
of time. Therefore, we will need to secure near-term funding, or we will be forced to curtail or terminate operations. Because we do
not currently have a guaranteed source of capital that will sustain operations for at least the next twelve months, Management has determined
that there is substantial doubt about our ability to continue as a going concern.
The
principal source of our capital to date has been the proceeds from the sale of equity and debt, a substantial portion of which has been
provided by officers and certain insiders. If we are unable to access additional funds in the near term, whether through the sale of
additional equity, debt or another means, we may not be able to continue in business. We also may not be able to continue the development
of our investigational drugs. Any additional equity or debt financing, if available to us, may not be available on favorable terms and
would most likely be dilutive to stockholders. Any debt financing, if available, may involve restrictive covenants and also be dilutive
to current stockholders. If we obtain funds through collaborative or licensing arrangements, we may be required to relinquish rights
to some of our technologies or product candidates on terms that are not favorable to us. Our ability to access capital when needed is
not assured.
In
their audit report with regard to our Financial Statements as of and for the years ended December 31, 2024, and 2023, we, as well as
our independent registered public accountants, have expressed an opinion that substantial doubt exists as to whether we can continue
as a going concern. Because we have limited cash resources, we believe that it will be necessary for us to either raise additional capital
in the near term or to enter into a license or other agreement with a larger pharmaceutical company. If we do not succeed in doing so,
we may be required to suspend or cease our business, which would likely materially harm the value of our common stock.
**Due
in part to our limited financial resources, we may fail to select or capitalize on the most scientifically, clinically or commercially
promising or profitable indications or therapeutic areas for our product candidates, and we may be unable to pursue and complete the
clinical trials that we would like to pursue and complete.**
We
have limited financial and technical resources to determine the indications on which we should focus the development efforts for our
product candidates. Due to our limited available financial resources, we have curtailed clinical development programs and activities
that might otherwise have led to more rapid progress of our product candidates through the regulatory and development processes. We currently
have insufficient financial resources to complete any additional drug development work.
| 22 | |
If
we are able to raise funds and continue developing investigational drugs for cancer, we may make incorrect determinations with regard
to the indications and clinical trials on which to focus the available resources that we do have. Furthermore, we cannot assure you that
we will be able to retain adequate staffing levels to run our operations and/or to accomplish all the objectives that we otherwise would
seek to accomplish. The decisions to allocate our research, management and financial resources toward particular indications or therapeutic
areas for our product candidates may not lead to the development of viable commercial products and may divert resources from better opportunities.
Similarly, our decisions to delay or terminate drug development programs may also cause us to miss valuable opportunities. In addition,
from time to time, we may in-license or otherwise acquire product candidates to supplement our internal development activities. Those
activities may use resources that otherwise would have been devoted to our internal programs, and with research and development programs
there is no way to assure that the outcome of any trials or other activities will be positive, whether the program was internally generated
or in-licensed.
**We
may encounter difficulties in expanding our operations successfully if and when we evolve from a company that is primarily involved in
clinical development to a company that is also involved in commercialization.**
As
we advance our product candidates through later stages of clinical trials, we will need to expand our development, regulatory, manufacturing,
marketing and sales capabilities or contract with third parties to provide these capabilities for us. As our operations expand, we expect
that we will need to manage additional relationships with such third parties, as well as additional collaborators, distributors, marketers,
and suppliers.
Maintaining
third party relationships for these purposes will impose significant added responsibilities on members of our management and other personnel.
We must be able to manage our development efforts effectively, manage our participation in the clinical trials in which our product candidates
are involved effectively, and improve our managerial, development, operational and finance systems, all of which may impose a strain
on our administrative and operational infrastructure.
If,
following any approval of our product candidates, we enter into arrangements with third parties to perform sales, marketing or distribution
services, any product revenues that we receive, or the profitability of these product revenues to us, are likely to be lower than if
we were to market and sell any products that we develop ourselves. In addition, we may not be successful in entering into arrangements
with third parties to sell and market our products or in doing so on terms that are favorable to us. We likely will have little control
over such third parties, and any of them may fail to devote the necessary resources and attention to sell and market our products effectively.
If we do not establish sales and marketing capabilities successfully, either on our own or in collaboration with third parties, we will
not be successful in commercializing our products.
If
we were to submit an NDA for our drug candidates in the United States or a marketing application in the EU, we would need to undertake
commercial scale manufacturing activities at significant expense to us in order to proceed with the application for approval for commercialization.
We or our external vendors may encounter technical difficulties that preclude us from successfully manufacturing the required registration
and validation batches of active pharmaceutical ingredient, or API, and/or drug product and we may be unable to recover any financial
losses associated with the manufacturing activities. Further, our research or product development efforts may not be successfully completed,
any compounds currently under development by us may not be successfully developed into drugs, any potential products may not receive
regulatory approval on a timely basis, if at all, and competitors may develop and bring to market products or technologies that render
our potential products obsolete. If any of these problems occur, our business would be materially and adversely affected.
**We
may not be able to partner with other pharmaceutical companies or even form any types of alliances with third parties.**
As
we plan to advance our product candidates through later stages of clinical trials but with lack of adequate capital resources, we will
need to form alliances or enter into partnerships with other pharmaceutical companies or even other third parties. We cannot assure you
that we would be able to do so at terms beneficial to the Company or at all.
| 23 | |
****
**We
may not be able to successfully set up an IPO with third parties.**
As
we plan to advance our product candidates through later stages of clinical trials but with lack of adequate capital resources, we will
need to form alliances or enter into partnerships with other pharmaceutical companies or even other third parties and create shareholder
value, including through IPOs. We cannot assure you that we would be able to do so at terms beneficial to the Company or at all. While
the Company has formed a joint venture with Dragon Overseas and GMP Bio, and plans on taking that through an IPO, there can be no assurances
that such IPO will be made or will be successful.
**We
may not be able to successfully develop the product portfolio through our JV.**
As
we plan to advance the product candidates being established through our JV, through later stages of development, manufacturing of the
products for clinical trials and ultimately commercial manufacturing, we may need to form alliances or enter into partnerships with other
pharmaceutical companies or even other third parties to work with us in the JVs endeavors to achieve success for the Product. That would
ensure success for the JV and create shareholder value for our Company. We cannot assure you that the JV would be able to do so and the
Company gets the benefits of that at all.
**We
have no manufacturing capacity and have relied on, and expect to continue to rely on, third-party manufacturers to produce our product
candidates.**
We
do not own or operate manufacturing facilities for the production of clinical or commercial quantities of our product candidates or any
of the compounds that we are testing in our preclinical programs, and we lack the resources and the capabilities to do so. As a result,
we currently rely, and we expect to rely for the foreseeable future, on third-party manufacturers to supply our product candidates. Reliance
on third-party manufacturers entails risks to which we would not be subject if we manufactured our product candidates or products ourselves,
including:
| 
| 
| 
reliance
on third-parties for manufacturing process development, regulatory compliance and quality assurance; | |
| 
| 
| 
| |
| 
| 
| 
limitations
on supply availability resulting from capacity and scheduling constraints of third-parties; | |
| 
| 
| 
| |
| 
| 
| 
the
possible breach of manufacturing agreements by third-parties because of factors beyond our control; and | |
| 
| 
| 
| |
| 
| 
| 
the
possible termination or non-renewal of the manufacturing agreements by the third-party, at a time that is costly or inconvenient
to us. | |
If
we do not maintain our developed important manufacturing relationships, we may fail to find replacement manufacturers or develop our
own manufacturing capabilities, which could delay or impair our ability to obtain regulatory approval for our products and substantially
increase our costs or deplete profit margins, if any. If we do find replacement manufacturers, we may not be able to enter into agreements
with them on terms and conditions favorable to us, and there could be a substantial delay before new facilities could be qualified and
registered with the FDA, EMA and other foreign regulatory authorities.
The
FDA, EMA and other foreign regulatory authorities require manufacturers to register manufacturing facilities. The FDA and corresponding
foreign regulators also inspect these facilities to confirm compliance with current good manufacturing practices, or cGMPs. Contract
manufacturers may face manufacturing or quality control problems causing drug substance production and shipment delays or a situation
where the contractor may not be able to maintain compliance with the applicable cGMP requirements. Any failure to comply with cGMP requirements
or other FDA, EMA and comparable foreign regulatory requirements could adversely affect our clinical research activities and our ability
to develop our product candidates and market our products after approval.
Our
current and anticipated future dependence upon others for the manufacture of our product candidates may adversely affect our ability
to develop our product candidates, our ability to commercialize any products that receive regulatory approval and our potential future
profit margins on these products.
| 24 | |
**Our
product candidates have not completed clinical trials and may never demonstrate sufficient safety and efficacy in order to do so.**
Our
product candidates are in the clinical stage of development. In order to achieve profitable operations, we alone or in collaboration
with others, must successfully develop, manufacture, introduce and market our products. The time frame necessary to achieve market success
for any individual product is long and uncertain. The products currently under development by us may require significant additional research
and development and additional preclinical and clinical testing prior to application for commercial use. A number of companies in the
biotechnology and pharmaceutical industries have suffered significant setbacks in clinical trials, even after showing promising results
in early or later-stage studies or clinical trials. Although we have obtained some favorable results to date in preclinical studies and
clinical trials of certain of our potential products, such results may not be indicative of results that will ultimately be obtained
in or throughout such clinical trials, and clinical trials may not show any of our products to be safe or capable of producing a desired
result. Additionally, we may encounter problems in our clinical trials that may cause us to delay, suspend or terminate those clinical
trials.
Adverse
events observed to date and associated with CA4P and OXi4503 have generally been found to be manageable for drugs treating the indications
for which we are developing our product candidates. However, we will be required to continue to test and evaluate the safety of our product
candidates in additional clinical trials, and to demonstrate their safety to the satisfaction of appropriate regulatory agencies, as
a condition to receipt of any regulatory approvals. In clinical trials to date, transient hypertension believed to be associated with
CA4P and OXi4503 has been effectively managed through pre-treatment with anti-hypertensive medication. We cannot assure you, however,
that we will be able to make the necessary demonstrations of safety to allow us to receive regulatory approval for our product candidates
in any indication.
**We
only have a limited number of employees to manage and operate our business.**
We
had a combined total of 40 full-time, part-time employees and consultants as of December 31, 2024; however, all the employees have
been compensated through the JV since March 2022. We rely on external consultants or outsource nearly all our research, development,
preclinical testing, and clinical trial activity, although we maintain managerial and quality control over our clinical trials. We
expect to continue to rely on external service providers and to maintain a small number of executives and other employees. Our
limited financial resources require us to manage and operate our business in a highly efficient manner. We cannot assure you that we
will be able to retain adequate staffing levels to run our operations and/or to accomplish all the objectives that we otherwise
would seek to accomplish.
**We
depend on our executive officers and principal consultants and the loss of their services could materially harm our business.**
We
believe that our success depends, and will likely continue to depend, upon our ability to retain the services of our current executive
officers, particularly our Chief Executive Officer, Chief Business Officer, Chief Medical Officer, Chief Regulatory Officer and Chief
Financial Officer, our principal consultants, and others. This increases the risk that we may not be able to retain their services. The
loss of the services of any of these individuals could have a material adverse effect on our business. In addition to these key service
providers, we have established relationships with universities, hospitals and research institutions, which have historically provided,
and continue to provide, us with access to research laboratories, clinical trials, facilities and patients. Additionally, we believe
that we may, at any time and from time to time, materially depend on the services of consultants and other unaffiliated third parties.
We cannot assure you that consultants and other unaffiliated third parties will provide the level of service to us that we require in
order to achieve our business objectives.
**Our
industry is highly competitive, and our product candidates may become obsolete.**
We
are engaged in a rapidly evolving field. Competition from other pharmaceutical companies, biotechnology companies and research and academic
institutions is intense and likely to increase. Many of those companies and institutions have substantially greater financial, technical,
and human resources than we do. Many of those companies and institutions also have substantially greater experience in developing products,
conducting clinical trials, obtaining regulatory approval and in manufacturing and marketing pharmaceutical products. Our competitors
may succeed in obtaining regulatory approval for their products more rapidly than we do. Competitors have developed or are in the process
of developing technologies that are, or in the future may be, the basis for competitive products. Some of these competitive products
may have an entirely different approach or means of accomplishing the desired therapeutic effect than products being developed by us.
Our competitors may succeed in developing products that are more effective and/or cost competitive than those we are developing, or that
would render our product candidates less competitive or even obsolete. In addition, one or more of our competitors may achieve product
commercialization or patent protection earlier than we do, which could materially adversely affect us.
| 25 | |
**If
clinical trials or regulatory approval processes for our product candidates are prolonged, delayed or suspended, we may be unable to
out-license or commercialize our product candidates on a timely basis, which would require us to incur additional costs and delay or
prevent our receipt of any proceeds from potential license agreements or product sales.**
We
cannot predict whether we will encounter problems with any of our completed, ongoing or planned clinical trials that will cause us or
any regulatory authority to delay or suspend those clinical trials or delay or invalidate the analysis of data derived from them. A number
of events, including any of the following, could delay the completion of our other ongoing and planned clinical trials and negatively
impact our ability to obtain regulatory approval for, and to market and sell, a particular product candidate:
| 
| 
| 
conditions
imposed on us by the FDA, EMA or another foreign regulatory authority regarding the scope or design of our clinical trials; | |
| 
| 
| 
| |
| 
| 
| 
delays
in obtaining, or our inability to obtain, required approvals from institutional review boards or other reviewing entities at clinical
sites selected for participation in our clinical trials; | |
| 
| 
| 
| |
| 
| 
| 
insufficient
supply of our product candidates or other materials necessary to conduct and complete our clinical trials; | |
| 
| 
| 
| |
| 
| 
| 
slow
enrollment and retention rate of subjects in clinical trials; | |
| 
| 
| 
| |
| 
| 
| 
any
compliance audits and pre-approval inspections by the FDA, EMA or other regulatory authorities; | |
| 
| 
| 
| |
| 
| 
| 
negative
or inconclusive results from clinical trials, or results that are inconsistent with earlier results; | |
| 
| 
| 
| |
| 
| 
| 
serious
and unexpected drug-related side effects; and | |
| 
| 
| 
| |
| 
| 
| 
failure
of our third-party contractors to comply with regulatory requirements or otherwise meet their contractual obligations to us. | |
Commercialization
or licensure of our product candidates may be delayed or prevented by the imposition of additional conditions on our clinical trials
by the FDA, EMA or another foreign regulatory authority or the requirement of additional supportive clinical trials by the FDA, EMA,
or another foreign regulatory authority. In addition, clinical trials require sufficient patient enrollment, which is a function of many
factors, including the size of the patient population, the nature of the trial protocol, the proximity of patients to clinical sites,
the availability of effective treatments for the relevant disease, the conduct of other clinical trials that compete for the same patients
as our clinical trials, and the eligibility criteria for our clinical trials. Our failure to enroll patients in our clinical trials could
delay the completion of the clinical trial beyond our expectations, or it could prevent us from being able to complete the clinical trial.
In addition, the FDA and EMA could require us to conduct clinical trials with a larger number of subjects than we have projected for
any of our product candidates. We may not be able to enroll a sufficient number of patients in a timely or cost-effective manner. Furthermore,
enrolled patients may drop out of our clinical trials, which could impair the validity or statistical significance of the clinical trials.
We
do not know whether our clinical trials will begin as planned, will need to be restructured, or will be completed on schedule, if at
all. Delays in our clinical trials will result in increased development costs for our product candidates, and our financial resources
may be insufficient to fund any incremental costs. In addition, if our clinical trials are delayed, our competitors may be able to bring
products to market before we do, and the commercial viability of our product candidates could be limited.
| 26 | |
**If
physicians and patients do not accept our future products or if the market for indications for which any product candidate is approved
is smaller than expected, we may be unable to generate significant revenue, if any.**
Even
if any of our product candidates obtain regulatory approval, they may not gain market acceptance among physicians, patients, and third-party
payers. Physicians may decide not to prescribe our drugs for a variety of reasons including:
| 
| 
| 
timing
of market introduction of competitive products; | |
| 
| 
| 
| |
| 
| 
| 
demonstration
of clinical safety and efficacy compared to other products; | |
| 
| 
| 
| |
| 
| 
| 
cost-effectiveness; | |
| 
| 
| 
| |
| 
| 
| 
limited
or no coverage by third-party payers; | |
| 
| 
| 
| |
| 
| 
| 
convenience
and ease of administration; | |
| 
| 
| 
| |
| 
| 
| 
prevalence
and severity of adverse side effects; | |
| 
| 
| 
| |
| 
| 
| 
restrictions
in the label of the drug; | |
| 
| 
| 
| |
| 
| 
| 
other
potential advantages of alternative treatment methods; and | |
| 
| 
| 
| |
| 
| 
| 
ineffective
marketing and distribution support of our products. | |
If
any of our product candidates is approved, but fails to achieve market acceptance, we may not be able to generate significant revenue
and our business would suffer.
**The
uncertainty associated with pharmaceutical reimbursement and related matters may adversely affect our business.**
Market
acceptance and sales of any one or more of our product candidates that we develop will depend on reimbursement policies and may be affected
by future healthcare reform measures in the United States and in foreign jurisdictions. Government authorities and third-party payers,
such as private health insurers and health maintenance organizations, decide which drugs they will cover and establish payment levels.
We cannot be certain that reimbursement will be available for any product candidates that we develop. Also, we cannot be certain that
reimbursement policies will not reduce the demand for, or the price paid for, our products. If reimbursement is not available or is available
on a limited basis, we may not be able to successfully commercialize any product candidates that we develop.
In
the United States, the Medicare Prescription Drug, Improvement, and Modernization Act of 2003, also called the Medicare Modernization
Act, or MMA, changed the way Medicare covers and pays for pharmaceutical products. The legislation established Medicare Part D, which
expanded Medicare coverage for outpatient prescription drug purchases by the elderly but provided authority for limiting the number of
drugs that will be covered in any therapeutic class. The MMA also introduced a new reimbursement methodology based on average sales prices
for physician-administered drugs.
The
United States and several foreign jurisdictions are considering, or have already enacted, a number of legislative and regulatory proposals
to change the healthcare system in ways that could affect our ability to sell our products profitably. Among policy makers and payers
in the United States and elsewhere, there is significant interest in promoting changes in healthcare systems with the stated goals of
containing healthcare costs, improving quality and/or expanding access to healthcare. In the United States, the pharmaceutical industry
has been a particular focus of these efforts and has been significantly affected by major legislative initiatives. We expect to experience
pricing pressures in connection with the sale of any products that we develop due to the trend toward managed healthcare, the increasing
influence of health maintenance organizations and additional legislative proposals.
| 27 | |
In
March 2010, the Affordable Care Act, as amended by the Health Care and Education Affordability Reconciliation Act, or collectively, ACA,
became law in the U.S. The goal of ACA is to reduce the cost of health care and substantially change the way health care is financed
by both government and private insurers. While we cannot predict what impact on federal reimbursement policies this legislation will
have in general or on our business specifically, the ACA may result in downward pressure on pharmaceutical reimbursement, which could
negatively affect market acceptance of, and the price we may charge for, any products we develop that receive regulatory approval.
More
recently, a past U.S. presidential administration had made statements suggesting plans to seek repeal of all or portions of the ACA.
There could be uncertainty regarding the impact that a future Presidential administration may have on matters governed by the ACA, if
any, and any regulatory or legislative changes will likely take time to unfold. These changes could have an impact on coverage and reimbursement
for healthcare items and services covered by plans that were authorized by the ACA. However, we cannot predict the ultimate content,
timing or effect of any healthcare reform legislation or the impact of potential legislation on us. Any reduction in reimbursement from
Medicare or other government programs may result in a similar reduction in payments from private payors. The implementation of cost containment
measures or other healthcare reforms may prevent us from being able to generate revenue, attain profitability, or commercialize our products.
**Our
business and operations could suffer in the event of system failures.**
Despite
the implementation of security measures, our internal computer systems and those of our third-party CROs and other contractors and consultants
are vulnerable to damage from computer viruses, unauthorized access, natural disasters, terrorism, war and telecommunication and electrical
failures. Furthermore, we have little or no control over the security measures and computer systems of our third-party CROs and other
contractors and consultants. While we have not experienced any material system failure, accident, or security breach to date, if such
an event were to occur and cause interruptions in our operations, it could result in a material disruption of our programs. For example,
the loss of clinical trial data for our product candidates could result in delays in our marketing approval efforts and significantly
increase our costs to recover or reproduce the data. To the extent that any disruption or security breach results in a loss of or damage
to our data or applications or other data or applications relating to our technology or product candidates, or inappropriate disclosure
of confidential or proprietary information, we could incur liabilities and the further development of our product candidates could be
delayed.
**REGULATORY
AND LEGAL RISK FACTORS**
**If
we are unable to obtain required regulatory approvals, we will be unable to market and sell our product candidates.**
Our
product candidates are subject to extensive governmental regulations relating to development, clinical trials, manufacturing, oversight
of clinical investigators, recordkeeping, and commercialization. Rigorous preclinical testing and clinical trials and an extensive regulatory
review and approval process are required to be successfully completed in the United States, in the European Union and in many other foreign
jurisdictions before a new drug can be sold. Satisfaction of these and other regulatory requirements is costly, time consuming, uncertain,
and subject to unanticipated delays. The time required to obtain approval by the FDA or the European Medicines Agency, or EMA, is unpredictable
and often takes many years following the commencement of clinical trials.
In
connection with the clinical development of our product candidates, we face risks that:
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our
product candidates may not prove to be safe and efficacious; | |
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patients
may die or suffer serious adverse effects for reasons that may or may not be related to the product candidate being tested; | |
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we
fail to maintain adequate records of observations and data from our clinical trials, to establish and maintain sufficient procedures
to oversee, collect data from, and manage clinical trials, or to monitor clinical trial sites and investigators to the satisfaction
of the FDA, EMA, or other regulatory agencies; | |
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we
may not have sufficient financial resources to complete the clinical trials that would be necessary to obtain regulatory approvals; | |
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the
results of later-phase clinical trials may not confirm the results of earlier clinical trials; and | |
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the
results from clinical trials may not meet the level of statistical significance or clinical benefit-to-risk ratio required by the
FDA, EMA, or other regulatory agencies for marketing approval. | |
Only
a small percentage of product candidates for which clinical trials are initiated are the subject of NDAs and even fewer receive approval
for commercialization. Furthermore, even if we do receive regulatory approval to market a product candidate, any such approval may be
subject to limitations such as those on the indicated uses for which we may market the product.
**If
we or our JV follows certain regulatory pathways, we may not be successful in our plans and, as such, we may not be able to obtain regulatory
approval for or commercialize our product candidates.**
****
In
addition to regular pathways of filing INDs and NDAs, we, or our partners, including the JV, may also plan to follow expedited pathways such as 505(b)(2) pathway of expedited
approvals so as to get our products to market and patients for unmet medical needs on an expedited basis. However, we cannot guarantee
that the regulatory bodies would approve our approach or approve our products as planned.
****
**If
we or the third parties on which we rely for the conduct of our clinical trials and results do not perform our clinical trial activities
in accordance with good clinical practices and related regulatory requirements, we may not be able to obtain regulatory approval for
or commercialize our product candidates.**
We
currently use independent clinical investigators in all our clinical trials and, in many cases, also utilize contract research organizations,
or CROs, and other third-party service providers to conduct and/or oversee the clinical trials of our product candidates and expect to
continue to do so for the foreseeable future. We rely heavily on these parties for successful execution of our clinical trials. Nonetheless,
we are responsible for confirming that each of our clinical trials is conducted in accordance with the FDAs requirements and our
general investigational plan and protocol. Currently, we have clinical trial activities involving CA4P and OXi4503 being conducted by
clinical investigators who are independent of us, but with whom we have agreements for them to provide the results of their clinical
trials to us. In order for us to rely on data from these ongoing clinical trials in support of a New Drug Application, or NDA, for approval
of any of our product candidates by the FDA or similar types of marketing applications that are required by other regulatory authorities,
the independent investigators are required to comply with applicable good clinical practice requirements.
The
FDA and corresponding foreign regulatory authorities require us and our clinical investigators to comply with regulations and standards,
commonly referred to as good clinical practices, or GCPs, for conducting and recording and reporting the results of clinical trials to
assure that data and reported results are credible and accurate and that the trial participants are adequately protected. Our reliance
on third parties that we do not control does not relieve us of these responsibilities and requirements. Third parties may not complete
activities on schedule or may not conduct our clinical trials in accordance with regulatory requirements or the respective trial plans
and protocols. The failure of these third parties to carry out their obligations could delay or prevent the development, approval and
commercialization of our product candidates or result in enforcement action against us.
We
have taken and continue to take steps to strengthen our procedures and practices, but we cannot assure you that the FDA will be satisfied
with our procedures or that the FDA will not issue warning letters or take other enforcement action against us in the future. The steps
we take to strengthen our procedures and conduct future clinical trials necessary for approval will be time-consuming and expensive.
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**The
use of our products may result in product liability exposure, and it is uncertain whether our insurance coverage will be sufficient to
cover all claims.**
The
use of our product candidates in clinical trials may expose us to liability claims in the event such product candidates cause death,
injury or disease, or result in adverse effects. We may be exposed to liability claims even if our product did not cause death, injury
or diseases, but is merely presumed or alleged to have caused any of these. If our product candidates are ever commercially approved,
the commercial use of these products may also expose us to similar liability claims. Any of these claims could be made by health care
institutions, contract laboratories, patients or others using such products. Although we have obtained liability insurance coverage for
our ongoing clinical trials, this coverage may not be in amounts sufficient to protect us from any product liability claims or product
recalls which could have a material adverse effect on our financial condition and prospects. Further, adverse product and similar liability
claims could negatively impact our ability to obtain or maintain regulatory approvals for our technology and product candidates under
development.
**We
have been granted orphan drug status for certain of our product candidates and may seek orphan drug status for additional indications
for those product candidates or for additional product candidates. We may be unsuccessful in maintaining orphan drug exclusivity for
our product candidates and may be unsuccessful in our efforts to seek orphan drug status and orphan drug exclusivity.**
Regulatory
authorities in some jurisdictions, including the United States and the European Union, may designate drugs for relatively small patient
populations as orphan drugs. Under the Orphan Drug Act, the FDA may designate a product as an orphan drug if it is a drug intended to
treat a rare disease or condition, which is generally defined as a disease with a patient population of fewer than 200,000 individuals
in the United States. Our lead product candidate, OXi4503, has been awarded orphan drug status by the FDA and the European Commission
for the treatment of acute myelogenous leukemia. Our other product candidate, CA4P, has been awarded orphan drug status by the FDA for
the treatment of anaplastic, medullary, Stage IV papillary and Stage IV follicular thyroid cancers, ovarian cancer, neuroendocrine tumors
and glioma. CA4P has also been awarded orphan drug status by the European Commission in the European Union for the treatment of anaplastic
thyroid cancer, ovarian cancer and neuroendocrine tumors.
Generally,
if a product with an orphan drug designation subsequently receives the first marketing approval for the indication for which it has such
designation, the product is entitled to a period of marketing exclusivity, which precludes the EMA or the FDA from approving another
marketing application for the same drug for the same indication during the period of exclusivity. The applicable period is seven years
in the United States and ten years in the European Union. The European exclusivity period can be reduced to six years if a drug no longer
meets the criteria for orphan drug designation or if the drug is sufficiently profitable so that market exclusivity is no longer justified.
Orphan drug exclusivity may be lost if the FDA or the EMA determines that the request for designation was materially defective, if the
manufacturer is unable to assure sufficient quantity of the drug to meet the needs of patients with the rare disease or condition.
Even
if we obtain orphan drug exclusivity for a product candidate or additional product candidates, that exclusivity may not effectively protect
the product candidate from competition because different drugs can be approved for the same condition. Even after an orphan drug is approved,
the FDA can subsequently approve a different drug for the same condition if the FDA concludes that the later drug is clinically superior
in that it is shown to be safer, more effective or makes a major contribution to patient care.
**Our
product candidates will remain subject to ongoing regulatory review even if they receive marketing approval, and if we fail to comply
with continuing regulations, we could lose these approvals and the sale of any approved commercial products could be suspended.**
Even
if we receive regulatory approval to market a particular product candidate, the manufacturing, labeling, packaging, adverse event reporting,
storage, advertising, promotion, and record keeping related to the product will remain subject to extensive regulatory requirements.
If we fail to comply with the regulatory requirements of the FDA, EMA and other applicable domestic and foreign regulatory authorities
or previously unknown problems with any approved product, manufacturer, or manufacturing process are discovered, we could be subject
to administrative or judicially imposed sanctions, including:
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on the products, manufacturers, or manufacturing processes; | |
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warning
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civil
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injunctions; | |
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product
seizures or detentions; | |
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pressure
to initiate voluntary product recalls; | |
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suspension
or withdrawal of regulatory approvals; and | |
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refusal
to approve pending applications for marketing approval of new products or supplements to approved applications. | |
**Our
employees, principal investigators, CROs and consultants may engage in misconduct or other improper activities, including non-compliance
with regulatory standards and requirements and insider trading.**
We
are exposed to the risk that our employees, principal investigators, CROs and consultants may engage in fraudulent conduct or other illegal
activity. Misconduct by these parties could include intentional, reckless and/or negligent conduct or disclosure of unauthorized activities
to us that violate the regulations of the FDA and other regulatory authorities, including those laws requiring the reporting of true,
complete, and accurate information to such authorities; healthcare fraud and abuse laws and regulations in the United States and abroad;
or laws that require the reporting of financial information or data accurately. In particular, sales, marketing and business arrangements
in the healthcare industry are subject to extensive laws and regulations intended to prevent fraud, misconduct, kickbacks, self-dealing
and other abusive practices. Activities subject to these laws also involve the improper use of information obtained in the course of
clinical trials or creating fraudulent data in our preclinical studies or clinical trials, which could result in regulatory sanctions
and cause serious harm to our reputation.
We
have a code of conduct applicable to all of our employees, but it is not always possible to identify and deter misconduct by employees
and other third parties, and the precautions we take to detect and prevent this activity may not be effective in controlling unknown
or unmanaged risks or losses or in protecting us from governmental investigations or other actions or lawsuits stemming from a failure
to comply with these laws or regulations. Additionally, we are subject to the risk that a person could allege such fraud or other misconduct,
even if none occurred. If any such actions are instituted against us, and we are not successful in defending ourselves or asserting our
rights, those actions could have a significant impact on our business, including the imposition of civil, criminal and administrative
penalties, damages, monetary fines, possible exclusion from participation in Medicare, Medicaid and other federal healthcare programs,
contractual damages, reputational harm, diminished profits and future earnings, and curtailment of our operations, any of which could
adversely affect our ability to operate our business and our results of operations.
**RISKS
RELATED TO INTELLECTUAL PROPERTY**
**We
depend extensively on the patents and proprietary technology we license from others, and we must maintain these licenses in order to
preserve our business.**
We
have licensed rights to CA4P, OXi4503 and other programs from third parties. If our license agreements terminate or expire, we may lose
the licensed rights to our product candidates, including CA4P and OXi4503, and we may not be able to continue to develop them or, if
they are approved, we may not be able to market or commercialize them.
We
depend on license agreements with third-parties for certain intellectual property rights relating to our product candidates, including
patent rights. Currently, we have licensed certain patent rights from Arizona State University, or ASU, and the Bristol-Myers Squibb
Company for CA4P and OXi4503 and from Baylor University for other programs. In general, our license agreements require us to make payments
and satisfy performance obligations in order to keep these agreements in effect and retain our rights under them. These payment obligations
can include upfront fees, maintenance fees, milestones, royalties, patent prosecution expense, and other fees. These performance obligations
typically include diligence obligations. If we fail to pay, be diligent or otherwise perform as required under our license agreements,
we could lose the rights under the patents and other intellectual property rights covered by the agreements. While we are not currently
aware of any dispute with any licensors under our material agreements with them, if disputes arise under any of our in-licenses, including
our in-licenses from ASU, the Bristol-Myers Squibb Company, and Baylor University, we could lose our rights under these agreements. Any
such dispute may not be resolvable on favorable terms, or at all. Whether or not any disputes of this kind are favorably resolved, our
managements time and attention and our other resources could be consumed by the need to attend to and seek to resolve these disputes
and our business could be harmed by the emergence of such a dispute.
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If
we lose our rights under these agreements, we may not be able to conduct any further activities with the product candidate or program
that the license covered. If this were to happen, we might not be able to develop our product candidates further, or following regulatory
approval, if any, we might be prohibited from marketing or commercializing them. In particular, patents previously licensed to us, such
as the patents we previously licensed from Angiogene, might after termination be used to stop us from conducting activities in the patents
respective fields.
**We
depend on patents and proprietary technology in the course of our business, and we must protect those assets in order to preserve our
business.**
Although
we expect to seek patent protection for any compounds we discover and/or for any specific use we discover for new or previously known
compounds, any or all of them may not be subject to effective patent protection. Further, the development of regimens for the administration
of pharmaceuticals, which generally involve specifications for the frequency, timing and amount of dosages, has been, and we believe,
may continue to be, important to our effort, although those processes, as such, may not be patentable. In addition, the issued patents
may be declared invalid, or our competitors may find ways to avoid the claims in the patents. Further, our lack of access to adequate
capital may cause us to curtail payment of fees necessary to maintain patents that we otherwise would seek to maintain, and we may make
incorrect decisions regarding which patents to keep and which to abandon.
Our
success will depend, in part, on our ability to obtain and maintain patents, protect our trade secrets and operate without infringing
on the proprietary rights of others. We are the exclusive licensee, sole assignee, or co- assignee on a number of granted United States
patents, pending United States patent applications, and granted patents and/or pending applications in several other major markets, including
the European Union, Canada and Japan. The patent position of pharmaceutical and biotechnology firms like us is generally highly uncertain
and involves complex legal and factual questions, resulting in both an apparent inconsistency regarding the breadth of claims allowed
in United States patents and general uncertainty as to their legal interpretation and enforceability. Accordingly, patent applications
assigned or exclusively licensed to us may not result in patents being issued, any issued patents assigned or exclusively licensed to
us may not provide us with competitive protection or may be challenged by others, and the current or future granted patents of others
may have an adverse effect on our ability to do business and achieve profitability. Moreover, because some of the basic research relating
to one or more of our patent applications and/or patents were performed at various universities and/or funded by grants, one or more
of these universities, employees of such universities and/or grantors could assert that they have certain rights in such research and
any resulting products. Further, others may independently develop similar products, may duplicate our products, or may design around
our patent rights. In addition, as a result of the assertion of rights by a third-party or otherwise, we may be required to obtain licenses
to patents or other proprietary rights of others in or outside of the United States. Any licenses required under any such patents or
proprietary rights may not be made available on terms acceptable to us, if at all. If we do not obtain such licenses, we could encounter
delays in product market introductions while our attempts to design around such patents or could find that the development, manufacture,
or sale of products requiring such licenses is foreclosed. In addition, we could incur substantial costs in defending ourselves in suits
brought against us or in connection with patents to which we hold licenses or in bringing suit to protect our own patents against infringement.
We
require employees and the institutions that perform our preclinical and clinical trials to enter into confidentiality agreements with
us. Those agreements provide that all confidential information developed or made known to a party to any such agreement during the course
of the relationship with us be kept confidential and not be disclosed to third-parties, except in specific circumstances. Any such agreement
may not provide meaningful protection for our trade secrets or other confidential information in the event of unauthorized use or disclosure
of such information.
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**RISKS
RELATED TO OUR STOCK AND FINANCING ACTIVITIES**
**The
price of our common stock is volatile and is likely to continue to fluctuate due to reasons beyond our control; a limited public trading
market may cause volatility in the price of our common stock.**
The
market price of our common stock has been, and likely will continue to be, highly volatile. Factors, including our financial results
or our competitors financial results, clinical trial and research development announcements and government regulatory action affecting
our potential products in both the United States and foreign countries, have had, and may continue to have, a significant effect on our
results of operations and on the market price of our common stock. We cannot assure you that an investment in our common stock will not
fluctuate significantly. One or more of these factors could significantly harm our business and cause a decline in the price of our common
stock in the public market. Substantially all of the shares of our common stock issuable upon exercise of outstanding options and warrants
have been registered or are likely to be registered for resale or are available for sale pursuant to Rule 144 under the Securities Act
and may be sold from time to time. As of December 31, 2024, we had approximately 289.5 million shares of common stock underlying currently
outstanding convertible debt, warrants and options. Sales of any of these shares on the market, as well as future sales of our common
stock by existing stockholders, or the perception that sales may occur at any time, could adversely affect the market price of our common
stock.
Our
common stock is currently quoted on the OTCQB Market. The quotation of our common stock on the OTCQB Market does not assure that a meaningful,
consistent, and liquid trading market currently exists, and in recent years such market has experienced extreme price and volume fluctuations
that have particularly affected the market prices of many smaller companies like us. Our common stock is subject to this volatility.
Sales of substantial amounts of common stock, or the perception that such sales might occur, could adversely affect prevailing market
prices of our common stock and our stock price may decline substantially in a short time and our stockholders could suffer losses or
be unable to liquidate their holdings.
*The
price of our common stock may be volatile and fluctuate substantially, which could result in substantial losses for purchasers of our
common stock.*
Our
stock price may be volatile. The stock market in general and the market for smaller specialty pharmaceutical companies and biotechnology,
in particular, have experienced extreme volatility that has often been unrelated to the operating performance of particular companies
or the quality of the underlying assets. As a result of this volatility, you may not be able to sell your common stock at or above the
price you paid for such shares. The market price for our common stock may be influenced by many factors, including but not limited to:
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reduction
in stock price could indicate impairment of the goodwill and intangible assets; | |
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market
conditions in the pharmaceutical and biotechnology sectors; | |
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general
economic, industry, and market conditions; and | |
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the
other factors described in this Risk Factors section. | |
**We
will require additional capital funding, the receipt of which may impair the value of our common stock.**
Our
future capital requirements depend on many factors, including our research, development, sales, and marketing activities. We will need
to raise additional capital through public or private equity or debt offerings or through arrangements with strategic partners or other
sources in order to continue to develop our product candidates. There can be no assurance that additional capital will be available when
needed or on terms satisfactory to us, if at all. To the extent we raise additional capital by issuing equity securities, our shareholders
may experience substantial dilution and the new equity securities may have greater rights, preferences, or privileges than our existing
common stock.
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**Our
common stock is currently subject to the Penny Stock Rules of the SEC and the trading market in our securities is limited,
which makes transactions in our stock cumbersome and may reduce the value of an investment in our stock.**
As
of December 31, 2024, we had net assets of approximately $7.5 million and our common stock had a market price per share of less
than $5.00. As a result, transactions in our common stock are subject to the SECs penny stock rules. The
designation of our common stock as a penny stock likely limits the liquidity of our common stock. Prices for penny
stocks are often not available to buyers and sellers and the market may be very limited. Penny stocks are among the riskiest equity
investments. Broker-dealers who sell penny stocks must provide purchasers of these stocks with a standardized risk-disclosure
document prepared by the SEC. The document provides information about penny stocks and the nature and level of risks involved in
investing in the penny stock market. A broker must also provide purchasers with bid and offer quotations and information regarding
broker and salesperson compensation and make a written determination that the penny stock is a suitable investment for the purchaser
and obtain the purchasers written agreement to the purchase. Many brokers choose not to participate in penny stock
transactions. Because of the penny stock rules, there may be less trading activity in penny stocks. Because shares of our common
stock are currently subject to these penny stock rules, your ability to trade or dispose of shares of our common stock may be
adversely affected.
**We
may not be able to achieve secondary trading of our stock in certain states because our common stock is no longer nationally traded,
which could subject our stockholders to significant restrictions and costs.**
Our
common stock is not currently eligible for trading on the Nasdaq Capital Market or on a national securities exchange. Therefore, our
common stock is subject to the securities laws of the various states and jurisdictions of the United States in addition to federal securities
law. While we may register our common stock or qualify for exemptions for our common stock in one of more states, if we fail to do so
the investors in those states where we have not taken such steps may not be allowed to purchase our stock or those who presently hold
our stock may not be able to resell their shares without substantial effort and expense. These restrictions and potential costs could
be significant burdens on our stockholders.
**If
we fail to maintain an effective system of internal controls over financial reporting, we may not be able to accurately report our financial
results. As a result, current and potential stockholders could lose confidence in our financial reporting, which could harm our business
and the trading price of our stock.**
Effective
internal controls over financial reporting are necessary for us to provide reliable financial reports. If we cannot maintain effective
controls and reliable financial reports, our business and operating results could be harmed. For example, our small size and limited
staffing levels do not allow for segregation of duties that exist at larger companies. We have conducted an evaluation of the effectiveness
of our internal control over financial reporting as of December 31, 2024, based on the criteria established in Internal Control - Integrated
Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission (2013 Framework). Based on that evaluation,
our management concluded that our internal controls over financial reporting were not effective as of December 31, 2024. While we continue
to work on remedying our weaknesses and maintaining effective internal controls over financial reporting; however, there can be no assurance
that a material weakness will not occur in the future, or our material weaknesses would be rectified. Any failure to implement and maintain
controls over our financial reporting or difficulties encountered in the implementation of improvements in our controls could cause us
to fail to meet our reporting obligations. Any failure to maintain our internal controls over financial reporting or to address identified
weaknesses in the future, if they were to occur, could also cause investors to lose confidence in our reported financial information,
which could have a negative impact on the trading price of our stock.
**Issuance
of additional equity securities may adversely affect the market price of our common stock.**
We
were authorized to issue up to 750,000,000 shares of our common stock. As of December 31, 2024, we had approximately 407.3 million shares
of common stock issued and outstanding, including approximately 1 million shares of common stock to be issued. As of December 31, 2024,
we also had approximately 31.9 million warrants outstanding, approximately 24 million options and approximately 233.4 million shares
of common stock issuable upon conversion of convertible notes.
To
the extent that additional shares of common stock are issued, or options and warrants are exercised, holders of our common stock will
experience dilution. In addition, in the event of any future issuances of equity securities or securities convertible into or exchangeable
for common stock, holders of our common stock may experience dilution.
Our
Board of Directors is authorized to issue preferred stock without any action on the part of our stockholders. Our Board of Directors
also has the power, without stockholder approval, to set the terms of any such preferred stock that may be issued, including voting rights,
conversion rights, dividend rights, preferences over our common stock with respect to dividends or if we liquidate, dissolve, or wind
up our business and other terms. If we issue preferred stock in the future that has preference over our common stock with respect to
the payment of dividends or upon our liquidation, dissolution or winding up, or if we issue preferred stock with voting rights that dilute
the voting power of our common stock, the market price of our common stock could decrease. Any provision permitting the conversion of
any such preferred stock into our common stock could result in significant dilution to the holders of our common stock.
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We
also consider from time-to-time various strategic alternatives that could involve issuances of additional common or preferred stock,
including but not limited to acquisitions and business combinations.
**We
have no plans to pay dividends on our common stock, and you may not receive funds without selling your common stock.**
We
have not declared or paid any cash dividends on our common stock, nor do we expect to pay any cash dividends on our common stock for
the foreseeable future. We currently intend to retain any future earnings, if any, to finance our operations and growth and, potentially,
for future stock repurchases and, therefore, we have no plans to pay cash dividends on our common stock. Any future determination to
pay cash dividends on our common stock will be at the discretion of our Board of Directors and will be dependent on our earnings, financial
condition, operating results, capital requirements, any contractual restrictions, and other factors that our board of directors deems
relevant.
Accordingly,
you may have to sell some or all of your common stock in order to generate cash from your investment in the Company. You may not receive
a gain on your investment when you sell our common stock and may lose the entire amount of your investment.
**The
Company will require additional capital funding, the receipt of which may impair the value of our Common Stock and EdgePoints
Common Stock.**
Our
future capital requirements and EdgePoints future capital requirements depend on many factors, including our research, development,
sales, and marketing activities as well as the development of EdgePoints business. We and EdgePoint will need to raise additional
capital through public or private equity or debt offerings or through arrangements with strategic partners or other sources in order
to continue to develop our product candidates. There can be no assurance that additional capital will be available when needed or on
terms satisfactory to us or EdgePoint, if at all. To the extent we and/or EdgePoint raise additional capital by issuing equity securities,
our shareholders and EdgePoints shareholders may experience substantial dilution and the new equity securities may have greater
rights, preferences, or privileges than our existing Common Stock and EdgePoints Common Stock and the Securities contemplated
to be issued as described in this Confidential Offering Memorandum.
**GENERAL
RISK FACTORS**
**Unfavorable
global epidemic or pandemic conditions could adversely affect our business, financial condition or results of operations.**
Our
operations and the financial results of our operations could be adversely affected by general conditions in the global economy and in
the global financial markets. Global financial concerns have caused, and may continue to cause, extreme volatility and disruptions in
the capital and credit markets. A severe or prolonged economic downturn could result in a variety of risks to our business, including
our ability to raise additional capital when needed on acceptable terms, if at all. We cannot currently anticipate all the ways in which
the current economic climate and financial market conditions could adversely impact our business.
**Our
business may suffer from the severity or longevity of the COVID-19 Global Outbreak.**
While
the COVID-19 pandemic has become less effective, the after effects of the pandemic continue impacting countries, communities, supply
chains and markets, as well as the global financial markets. To date, COVID-19 has not had a material impact on the Company, other than
as set forth above. However, the Company cannot predict whether COVID-19, or any other global pandemic, will have a material impact on
our financial condition and results of operations due to understaffing, disruptions in government spending, among other factors.
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**A
material amount of our assets represents intangible assets, and our net income would be reduced, or our net loss would be increased, if our intangible assets became impaired.**
As
of December 31, 2024, our gross intangible assets and goodwill from our 2019 PointR acquisition represented approximately $1.1 million
and approximately $2.8 million, respectively and after recording an impairment loss of $3.2 million; and the fair value of our investment
in our JV was approximately $22.7 million, representing approximately 99% of our total assets. Goodwill is generated in our acquisitions
when the cost of an acquisition exceeds the fair value of the net tangible and identifiable intangible assets we acquire. Goodwill and
indefinite-lived intangible assets are subject to an impairment analysis at least annually based on fair value. Intangible assets relate
primarily to in-process research and development (*IPR&D*) and patents acquired by us as part of our acquisitions
of other companies and are subject to an impairment analysis whenever events or changes in circumstances exist that indicate that the
carrying value of the intangible asset might not be recoverable. If market and economic conditions or business performance deteriorate,
the likelihood that we would record an impairment charge would increase, which impairment charge could materially and adversely affect
our financial condition and operating results. As the market capitalization of our Company was adversely impacted due to a reduction
in the stock price of our Common Stock, during the year ended December 31, 2024, we recorded an impairment of approximately $3.2 million
on the goodwill representing the difference in net assets over the fair value of the Company, based on our market capitalization.
**We,
or the third parties upon whom we depend, may be adversely affected by earthquakes or other natural disasters and our business continuity
and disaster recovery plans may not adequately protect us from a serious disaster.**
Earthquakes
or other natural disasters could severely disrupt our operations and have a material adverse effect on our business, results of operations,
financial condition, and prospects. If a natural disaster, power outage or other event occurred that prevented us from using all or a
significant portion of our headquarters, that damaged critical infrastructure, such as the manufacturing facilities of our third-party
contract manufacturers, or that otherwise disrupted operations, it may be difficult or, in certain cases, impossible for us to continue
our business for a substantial period of time. The disaster recovery and business continuity plan we have in place may prove inadequate
in the event of a serious disaster or similar event. We may incur substantial expenses as a result of the limited nature of our disaster
recovery and business continuity plans, which could have a material adverse effect on our business.
**We
have formed a DAO company to operate with a DAO infrastructure within the rigor of a corporation.**
In
November 2022, the Company formed a DAO entity, Pet2DAO Inc., as a wholly owned subsidiary. Pet2DAO is a DAO technology company, integrating
the strong governance of traditional corporations with the innovative DAO architecture. The Company will look to engage stakeholders,
to build value through the DAO, while maintaining the rigor of traditional corporations, including governance, compliance, and accountability
through a team of veterans in public companies with innovators in AI, blockchain and Web3. Pet2DAO
will initially be looking to develop products for the animal health space. The Company will initially issue regular tokens and NFTs of
Pet2DAO called PDAO to its employees, shareholders and KOLs and use the Tokens to propose and vote on various animal health related programs.
In the future, the Company will evaluate and plan to register these tokens with the SEC to make such Tokens freely tradable at a future
point in time. The Company cannot predict the outcome of Pet2DAO as an entity, how investors will look at this new development, especially
with what is happening in the crypto currency environment, the success of the tokens, whether we will be able to register the tokens
as securities or the success to make these tokens freely tradable. Any failure of a DAO could cause investors of the Company to discontinue
to be invested in the Company, and which could have a negative impact on the trading price of our stock.
**ITEM
1B. UNRESOLVED STAFF COMMENTS**
None.
**ITEM 1C. CYBERSECURITY RISK MANAGEMENT, STRATEGY,
AND GOVERNANCE.**
****
**Risk management and strategy**
The Company recognizes the critical importance of
developing, implementing, and maintaining robust cybersecurity measures to safeguard our information systems and protect the confidentiality,
integrity, and availability of our data.
**
*Managing Material Risks & Integrated Overall
Risk Management*
The Company has strategically integrated cybersecurity
risk management into our broader risk management framework to promote a company-wide culture of cybersecurity risk management. This integration
ensures that cybersecurity considerations are an integral part of our decision-making processes at every level. Our risk management team
works to continuously evaluate and address cybersecurity risks in alignment with our business objectives and operational needs.
**
*Engage Third-parties on Risk Management, as required*
Recognizing the complexity and evolving nature of
cybersecurity threats, the Company plans to engage external experts, including cybersecurity assessors and auditors in evaluating and
testing our risk management systems. These partnerships would enable us to leverage specialized knowledge and insights, ensuring our cybersecurity
strategies and processes remain at the forefront of industry best practices. Our possible collaborations with these third-parties will
innclude regular audits, threat assessments, and consultation on security enhancements.
*Oversee Third-party Risk*
Because we are aware of the risks associated with
third-party service providers, the Company plans to implement processes to oversee and manage these risks. We plan to conduct thorough
security assessments of all third-party providers before engagement and maintain ongoing monitoring to ensure compliance with our cybersecurity
standards. The monitoring will include periodic assessments by our Chief Executive Officer (CEO). This approach will be
planned to design to mitigate risks related to data breaches or other security incidents originating from third-parties.
**
| 36 | |
*Risks from Cybersecurity Threats*
We have not encountered cybersecurity challenges
that have materially impaired our operations or financial standing.
****
**Governance**
The Board of Directors is acutely aware of the critical
nature of managing risks associated with cybersecurity threats. The Board plans to establish robust oversight mechanisms to ensure effective
governance in managing risks associated with cybersecurity threats because we recognize the significance of these threats to our operational
integrity and stakeholder confidence,
**
*Board of Directors Oversight*
The Audit Committee is central to the Boards
oversight of cybersecurity risks and bears the primary responsibility for this domain. The Audit Committee is composed of board members
with diverse expertise including, risk management, technology, and finance, equipping them to oversee cybersecurity risks effectively.
In the absence of a functional Audit Committee at this time, the full Board of Directors will be responsible to oversight the cybersecurity
risks for the Company.
**
*Managements Role Managing Risk*
The CEO plays a pivotal role in informing the Board
of Directors on cybersecurity risks. The CEO provides comprehensive briefings to the Audit Committee on a regular basis, with a minimum
frequency of once per year. These briefings encompass a broad range of topics, including:
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Current cybersecurity landscape and emerging threats; | |
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Status of ongoing cybersecurity initiatives and strategies; | |
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Incident reports and learnings from any cybersecurity events; and | |
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Compliance with regulatory requirements and industry standards. | |
**ITEM
2. PROPERTIES**
Our
office is located in Agoura Hills, California, where we lease about 2,000 square feet of general office space. The lease for this office
is on a month-to-month basis. We consider our office space to be adequate for our current needs. We believe that other suitable office
space would be available if we moved to a different location upon the expiration of our current lease.
**ITEM
3. LEGAL PROCEEDINGS**
From
time to time, we may become involved in legal proceedings arising in the ordinary course of our business. Historically, the outcome of
all such legal proceedings has not, in the aggregate, had a material adverse effect on our business, financial condition, results of
operations or liquidity. Other than as set forth below, there is no additional material pending or threatened legal proceedings at this
time.
One
of the Companys ex-employees has made a breach of employment contract claim against the Company. The Company and its legal counsel
are evaluating the validity of the claim, as the Company believes that such claim has limited merits and is hopeful to attain a positive
outcome for such claim. Since the Company and its legal counsel are still evaluating the claim, we are unable to quantify the amount
such claim would be settled at, if at all settled.
**ITEM
4. MINE SAFETY DISCLOSURES**
Not
applicable.
**PART
II**
**ITEM
5. MARKET FOR REGISTRANTS COMMON EQUITY, RELATED STOCKHOLDER MATTERS AND ISSUER PURCHASES OF EQUITY SECURITIES**
The
Companys common stock trades on the OTCQB market, operated by OTC Markets, under the symbol OTLC.
**Holders**
As
of April 14, 2025, there were 78 stockholders of record of the 408,292,450 outstanding shares of the Companys common stock, including 1,019,303 shares pending to be issued to certain dissenting shareholders.
**Dividends**
The
Company has not declared or paid any cash dividends on its common stock since its inception in 1988 and does not expect to pay cash dividends
in the foreseeable future. The Company presently intends to retain future earnings, if any, to finance the growth and development of
its business.
**Securities
Authorized for Issuance Under Equity Compensation Plans**
Information
relating to compensation plans under which our equity securities are authorized for issuance is presented in Part III, Item 12 of this
Annual Report on Form 10-K.
| 37 | |
****
**Unregistered
Sales of Securities**
No
unregistered securities were issued during the fiscal year that were not previously reported in a Quarterly Report on Form 10-Q or Current
Report on Form 8-K.
**ITEM
6. RESERVED**
**ITEM
7. MANAGEMENTS DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS**
*Note
Regarding Forward-Looking Statements*
This
Annual Report on Form 10-K (the *Annual Report* or *Report*) includes a number of forward-looking
statements that reflect managements current views with respect to future events and financial performance. Forward- looking statements
are projections in respect of future events or our future financial performance. In some cases, you can identify forward-looking statements
by terminology such as may, should, expects, plans, anticipates,
believes, estimates, predicts, potential or continue or the negative
of these terms or other comparable terminology. Those statements include statements regarding the intent, belief or current expectations
of us and members of our management team, as well as the assumptions on which such statements are based. For a more detailed discussion
on our forward-looking statements, kindly refer to Forward Looking Statements prior to Item 1: Part I: Business contained
in this Annual Report.
Although
we believe that the expectations reflected in the forward-looking statements are reasonable, we cannot guarantee future results, levels
of activity, or performance. These statements are only predictions and involve known and unknown risks, uncertainties, and other factors.
Some of these risks are included in the section entitled Risk Factors set forth in this Annual Report and in other reports
that we file with the SEC. The occurrence of any of these risks, or others of which we are currently unaware, may cause our companys
actual results, levels of activity, performance, or achievements to be materially different from any future results, levels of activity,
performance or achievements expressed or implied by these forward-looking statements. These risks include, by way of example and without
limitation:
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our
ability to successfully commercialize our products and services on a large enough scale to generate profitable operations; | |
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our
ability to maintain and develop relationships with customers and suppliers; | |
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our
ability to successfully integrate acquired businesses or new products, or to realize anticipated synergies in connection with acquisitions
of businesses or products; | |
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expectations
concerning our ability to raise additional funding and to continue as a going concern; | |
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our
ability to successfully implement our business plan; | |
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our
ability to successfully operate GMP Biotechnology Limited (GMP Bio), our joint venture (JV)
with Dragon Overseas Limited (Dragon), to develop and commercialize the JVs nanoparticle product portfolio,
or to have a successful IPO for GMP Bio as planned; | |
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our
ability to avoid, or to adequately address any intellectual property claims brought by third parties; and | |
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the
anticipated impact of any changes in industry regulation. | |
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building
and the success of our nanoparticle platform and the related success of launching the platform | |
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the
success of the launch of a company with a DAO infrastructure, the success of the entity and the plans surrounding the pet and animal
health, the ability for the Company to register the tokens of Pet2Dao, the actual filing of a registration statement and approval
of the tokens as registrable securities with the SEC through a registration statement, the ability of the tokens to be tradable or
any value such tokens may have if they become tradable. | |
| 38 | |
Readers
are urged to carefully review and consider the various disclosures made by us in this Annual Report and in our other reports filed with
the SEC. We undertake no obligation to update or revise forward-looking statements to reflect changed assumptions, the occurrence of
unanticipated events or changes in the future operating results over time except as required by law. We believe that our assumptions
are based upon reasonable data derived from and known about our business and operations. No assurances are made that the actual results
of operations or the results of our future activities will not differ materially from our assumptions.
*Corporate
History*
Oncotelic
Therapeutics, Inc. (*Oncotelic*), was formed in the State of New York in 1988 as OXiGENE, Inc., was reincorporated
in the State of Delaware in 1992, and changed its name to Mateon Therapeutics, Inc. in 2016, and Oncotelic Therapeutics, Inc. in November
2020. Oncotelic conducts business activities through Oncotelic and its wholly-owned subsidiaries, Oncotelic, Inc., a Delaware corporation,
PointR Data, Inc. (*PointR*), a Delaware corporation, Pet2DAO Inc., a Delaware corporation and EdgePoint AI, Inc.
(*Edgepoint*), a Delaware Corporation for which there are non-controlling interests, (Oncotelic, Oncotelic Inc., PointR,
Pet2DAO and Edgepoint are collectively called the *Company* or *We*). The Company completed a reverse
merger with Oncotelic Inc in April 2019, a merger with PointR in November 2019 and formed a subsidiary Edgepoint in February 2020. For
more information on these mergers, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
*Company
Overview*
We
are a clinical stage biopharmaceutical company developing drugs for the treatment of cancer. Our goal is to advance our drug candidates
into late-stage pivotal clinical trials and either sell marketing rights to a larger pharmaceutical company or seek FDA approval ourselves.
The
Company is currently developing OT-101, through its JV with Dragon, and GMP Bio and its wholly owned subsidiaries, both affiliates
of Golden Mountain Partners (*GMP*), for various cancers and COVID-19, Artemisinin for COVID-19 and 5 additional nanoparticle
products for treatments of various cancers; our portfolio products Apomorphine for various indications; OXi4503, as a treatment for acute
myeloid leukemia and myelodysplastic syndromes; CA4P, in combination with a checkpoint inhibitor for the treatment of advanced metastatic
melanoma; and AI technologies for clinical development and manufacturing. The Company is also planning to develop OT-101 for certain
animal health indications and contemplating using crypto currencies for that platform. The Company has acquired apomorphine for Parkinsons
Disease, erectile dysfunction and female sexual dysfunction. In addition, the Company is evaluating the further development of its product
candidates OXi4503 as a treatment for acute myeloid leukemia and myelodysplastic syndromes and CA4P in combination with a checkpoint
inhibitor for the treatment of advanced metastatic melanoma.
In
2020, the Company had entered into an agreement and supplemental agreement with GMP for a total of $1.2 million to render services for
the development of OT-101 for COVID-19. The Company had also secured various financings from GMP between 2020 and early 2022, primarily
in this connection. For more information on the GMP debt financing and the JV, refer to Notes 5 and 6 of the Notes to the Consolidated
Financial Statements.
In
November 2022, the Company formed a Decentralized autonomous organization (*DAO*) entity, Pet2DAO, Inc. (*Pet2DAO*),
as a wholly owned subsidiary. For more information on Pet2DAO, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April
12, 2024.
Since
April 2019, we have been operating under significant capital constraints, which has curtailed our ability to achieve meaningful progress
in either of the Companys two clinical programs one of which is developing OXi4503 as a treatment for acute myeloid leukemia
and myelodysplastic syndromes and the other of which is developing CA4P in combination with a checkpoint inhibitor for the treatment
of advanced metastatic melanoma. We believe that the merger of Oncotelic and Oncotelic Inc. creates a combined company that has potential
to generate shareholder value through a promising pipeline of next generation immunotherapies targeting several significant cancer markets
where there is a lack of therapeutic options and lack of an effective immunotherapy protocol.
| 39 | |
Forever
Prosperity, LLC (previously GMP) Note purchase agreements and unsecured notes
Between
June 2020 and January 2022, the Company entered into various purchase agreements and promissory notes with GMP, cumulatively totaling
$4.5 million. Such notes were assigned to Forever Prosperity, LLC, an affiliated entity of GMP.
For
more information on the Forever Prosperity, LLC debt financing, refer to Note 5 of the Notes to the Consolidated Financial Statements.
*Joint
Venture*
In
March 2022, the Company entered into (i) a joint venture (the *JV*) agreement with Dragon and GMP Bio, both affiliates
of GMP, (and the Company, Dragon and GMP Bio are collectively called the *Parties*) (the *JVA*),
(ii) a license agreement for rights to OT-101 (the *US License Agreement*) for the territory within the United States
of America (the *US*) with Sapu Holdings, LLC, a subsidiary of GMP Bio and (iii) a license agreement for rights to
OT-101 for the rest of the world with GMP Bio (the *Ex-US Rights Agreement*, and the US License Agreement and the
Ex-US License Agreement are collectively called the *Agreements*). For more information on the JV, JVA, and Agreements,
refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
The
JV is conducting a clinical trial for OT-101 for pancreatic cancer in the US and which the JV is planning to expand to other countries
in eastern Europe. In addition, OT-101 is also being evaluated for treatments of gliomas and pediatric DIPG. In late 2023, the JV initiated
a plan to start evaluating various nanoparticles that could treat various cancers. In this regard, the JV identified a total of 4 compounds,
in addition to OT-101, which had the potential of significant revenue generation for the JV. In the same year, the JV signed a lease
agreement to set up a GMP manufacturing facility in San Diego (*SD*), California. The main purpose of this facility
was to initially commence an aggressive formulation development of newly planned nanoparticle platform (*Nano Platform*).
The GMP manufacturing facility was initiated in January 2024. Upon the initiation of this facility by the JV, the JV commenced the development
work on two of the four identified compounds, as well as other activities, in tandem with the development of OT-101. The JV has since
completed the formulation development of one of the products and is moving to complete the formulation development for the three additional
products. The JV is also working on improved formulations for OT-101 with new nanoparticle sizes. The JV also has started clinical development
for OT-101 for pancreatic cancer. Significant progress has been made in the development of the products and the JV anticipates to complete
the formulation development work in 2025 and pushing to initiate clinical trials for the various compounds. In late 2024, the GMP facility
in SD was issued a Drug Manufacturing License by the State of California Department of Public Health and Food and Drug Branch. Further,
in late 2024, the JV identified a sixth candidate as a compound for development for the JV and has already started to work on the formulation
development of that compound as well. A lot of the manufacturing, including Phase 1 clinical trial materials, will be performed at the
SD site.
Further, in late 2024, the JV identified a
sixth candidate as a compound for development for the JV and has already started to work on the formulation development of that
compound as well. In early 2025, the Company announced that it had entered into a strategic partnership with Shanghai Medicilon, Inc.
(*Medicilon*) to access its industry-leading rapid investigational new drug (*IND*)
development platform to support up to 20 IND projects, the support of which can even be used by the JV. All six of our compounds the JV is developing are planned to be these INDs,
and are focused on next-generation anticancer agents. The JV anticipates that all these six anticancer agents have the potential to
become significant growth contributors to the JV, which in turn would add substantial value to the Company. In March 2025, the Company announced successfully completing a Phase
1 clinical trial evaluating OT-101, in combination with IL-2 for advanced or metastatic solid tumors, on behalf of the JV. These results
set the stage for new studies that combine OT-101, an antisense therapeutic targeting Transforming Growth Factor Beta 2 (TGF2),
with checkpoint inhibitors (CKIs) and recombinant IL-2 (aldesleukin) (IL-2). The Phase 1 trial (ClinicalTrials.gov
ID: NCT04862767) investigated the safety and tolerability of OT-101 in combination with recombinant IL-2 in patients with advanced or
metastatic solid tumors. The combination showed a tolerable safety profile at the planned dosing schedule, with no unexpected safety signals
identified. Based on the favorable safety data, the JV, through the Company, plans to advance OT-101 plus IL-2 into further clinical studies,
exploring synergies with CKIs such as PD-1 blockers.
**
| 40 | |
**
*New
Private Placement with JH Darbie*
In
July 2023, the Company entered into a series of subscription agreements with 15 accredited investors which resulted in a conversion of
a gross amount of $1.0 million, consisting of 40 notes, under the prior JH Darbie Financing into new debt to the Company. JH Darbie and
the Company are parties to a March 2023 placement agent agreement (Agreement) pursuant to which JH Darbie has the right
to sell/convert a minimum of 10 Units and a maximum of 200 Units on a best-efforts basis. Further, in October 2023, the Company entered
into a series of subscription agreements with 27 accredited investors which resulted in a conversion of a gross amount of $1.05 million,
consisting of 42 notes, under the prior JH Darbie Financing into new debt to the Company. Additionally, in January 2024, Company entered
into a series of subscription agreements with 4 accredited investors which resulted in a conversion of a gross amount of $0.3 million,
consisting of 12 notes. The July 2023, October 2023 and January 2024 conversions fully converted JH Darbie PPM-1 notes into PPM-2 notes.
For more information on the new JH Darbie Financing, refer to Note 8 of these Notes to the Consolidated Financial Statements.
*August
2021 Notes*
In
August 2021, the Company entered into Note Purchase Agreements with Autotelic, the Companys CFO, and certain other accredited
investors. Under the terms of the Note Purchase Agreements, the Company issued an aggregate of $698,500 (the *Principal Amount*)
in debt in the form of unsecured convertible promissory notes (collectively, the *August 2021 Notes*). For more information
on the August 2021 Notes, refer to Note 5 of the current Notes to the Consolidated Financial Statements.
*November
/ December 2021 and March 2022 Financing*
In
November / December 2021, the Company entered into securities purchase agreement with five institutional investors, whereby the Company
issued five convertible notes in the aggregate principal amount of $1,250,000 convertible into shares of common stock of the Company.
The convertible notes carry a twelve (12%) percent coupon and a default coupon of 16% and mature at the earliest of one year from issuance
or upon event of default. Investors has the right at any time following issuance date to convert all or any part of the outstanding and
unpaid amount of the note into the Companys common stock at a conversion price established at a fixed rate of $0.07. The Company
granted a total number of 9,615,385 warrants convertible into an equivalent number of the Company Common Stock at a strike price of $0.13
up to five years after issuance. The Placement agent was also granted a total of 961,540 warrants convertible into an equivalent number
of the Company Common Stock at a strike price of $0.13 up to five years after issuance, as part of a finders fee agreement.
During
the year ended December 31, 2023, the Company converted the balance of approximately $243,000 of Blue Lake November / December 2021 convertible
notes, inclusive of accrued interest, into 3,466,583 shares of the Companys Common Stock, which fully retired the convertible
notes as of December 31, 2023. Further, during the year ended December 31, 2023, the Company fully converted the balance of Fourth Man
convertible note of approximately $127,000 into 1,820,395 shares of the Companys common stock, which fully retired the convertible
note as of December 31, 2023
In
March 2022, the Company entered into a Securities Purchase Agreement with Fourth Man, pursuant to which the Company issued convertible
promissory note in the aggregate principal amount of $0.25 million, convertible into shares of common stock of the Company. The convertible
notes carry a twelve (12%) percent coupon and a default coupon of 16% and mature at the earliest of one year from issuance or upon event
of default. As of December 31, 2023, this note was in default. The investors have the right at any time following issuance date to convert
all or any part of the outstanding and unpaid amount of the note into the Companys Common Stock at a conversion price established
at a fixed rate of $0.10. The Company granted a total number of 1,250,000 warrants convertible into an equivalent number of the Company
common shares at a strike price of $0.20 up to five years after issuance. The Placement agent was also granted a total of 125,000 warrants
convertible into an equivalent number of the Company Common Stock at a strike price of $0.20 up to five years after issuance, as part
of a finders fee agreement. In February 2024, the Company converted $35,000 in principal, legal fees and accrued interest of the
Fourth Man March 2022 note, into 500,000 shares of common stock.
For
more information on the November-December 2021 and March 2022 Financing, refer to Note 5 of current Notes to the Consolidated Financial
Statements.
| 41 | |
*May
2022 Note*
In
May 2022, the Company entered into a securities purchase agreement with one institutional investor, whereby the Company issued one convertible
note in the aggregate principal amount of $0.6 million, convertible into shares of common stock of the Company (May 2022 Mast
Note). The convertible notes carry a twelve (12%) percent coupon and a default coupon of 16% and mature at the earliest of one
year from issuance or upon event of default. Investor has the right at any time following issuance date to convert all or any part of
the outstanding and unpaid amount of the note into the Companys common stock at a conversion price established at a fixed rate
of $0.10. The Company granted a total number of 3,025,000 warrants convertible into an equivalent number of Company common shares at
a strike price of $0.20 up to five years after issuance. The Placement agent was also granted a total of 302,500 warrants convertible
into an equivalent number of the Company Common Stock at a strike price of $0.20 up to five years after issuance, as part of a finders
fee agreement. A portion of the proceeds were used to retire some of the November/December 2021 notes. In May 2024, the May 2022 Note
was extended till May 2025, at a cost of 10% of the outstanding Note amount, including interest and penalty.
For
more information on the May 2022 Financing, refer to Note 5 of current Notes to the Consolidated Financial Statements.
*June
2022 Note*
In
June 2022, the Company entered into a securities purchase agreement with one institutional investor, whereby the Company issued one convertible
note in the aggregate principal amount of $335,000 convertible into shares of common stock of the Company (June 2022 Blue Lake
Note). The convertible notes carry a twelve (12%) percent coupon and a default coupon of 16% and mature at the earliest of one
year from issuance or upon event of default. The investor has the right at any time following issuance date to convert all or any part
of the outstanding and unpaid amount of the note into the Companys common stock at a conversion price established at a fixed rate
of $0.10. The Company granted a total number of 837,500 warrants convertible into an equivalent number of the Company common shares at
a strike price of $0.20 up to five years after issuance. The Placement agent was also granted a total of 83,750 warrants convertible
into an equivalent number of the Company Common Stock at a strike price of $0.20 up to five years after issuance, as part of a finders
fee agreement. A portion of the proceeds were used to retire some of the November/December 2021 notes. In May 2024, Blue Lake converted
remainder of their debt balance, including accrued interest and penalty, of approximately $531,000 into 7,605,760 shares of the Companys
Common Stock.
For
more information on the June 2022 Financing, refer to Note 5 of current Notes to the Consolidated Financial Statements.
*Short-term
loans from related parties / families*
In
May 2021, Autotelic provided an additional short-term funding of approximately $0.3 million to the Company, which was converted into
the August 2021 Notes. Autotelic provided an additional $0.1 million short term loan to the Company during the year ended December 31,
2022. During the year ended December 31, 2023, Autotelic provided $1.4 million in various short-term loans to the Company. During the
year ended December 31, 2024 Autotelic Inc. provided additional short-term funding of $656,000 to the Company. As such, approximately
$2.1 million was outstanding and payable to Autotelic at December 31, 2024.
The
Companys CFO was owed approximately $25 thousand at December 31, 2022. During the year ended December 31, 2023, the companys
CFO provided additional short-term advance of $10 thousand. During the year ended December 31, 2024, the CFO provided additional short-term
funding of $41 thousand. As such, approximately $76 thousand was outstanding from the Companys CFO at December 31, 2024.
In December
2023, the Company received $50 thousand from the companys CEO. As such, $50 thousand was outstanding to the Companys CEO
at December 31, 2024. As of December 31, 2024 and December 31, 2023, respectively, approximately $210,000 was outstanding as short-term
advances from certain bridge investors.
| 42 | |
*Equity
Purchase Agreement*
In
May 2021, the Company entered into an Equity Purchase Agreement (the *EPL*) and Registration Rights Agreement (the
*Registration Rights Agreement*) with Peak One Opportunity Fund, L.P. (*Peak One*), pursuant to
which the Company shall have the right, but not the obligation, to direct Peak One to purchase up to $10.0 million (the *Maximum
Commitment Amount*) in shares of the common stock, par value $0.01 per share (*Common Stock*) in multiple
tranches. The Company filed a post-effective amendment for the EPL on April 12, 2024 with the SEC and the SEC has made the post-effective
amendment effective on April 22, 2024. The Company filed a prospectus under rule 424b3 with the SEC on April 26, 2024. For more information
on the EPL, refer to Note 10 of the Notes to the Unaudited Consolidated Financial Statements.
**
*Mosaic
ImmunoEngineering, Inc. Term Sheet*
In
April 2024, the Company entered into a binding term sheet (the *Term Sheet*) with Mosaic ImmunoEngineering, Inc. (*Mosaic*).
For more information on the Term Sheet, refer to the Current Report on Form 8-K filed with the SEC on April 29, 2024. In August 2024,
Mosaic and the Company mutually agreed to extend the date of the Term Sheet to expire at the earlier of (1) the signing of definitive
agreements or (2) December 31, 2024. Mosaic and the Company further agreed to extend the Term Sheet to expire at the earlier of (1) the
signing of definitive agreements or (2) June 30, 2025. This was to allow for both Companies to complete due diligence as well as agree
and finalize the definitive agreements.
**Critical
Accounting Policies and Significant Judgments and Estimates**
The
preparation of financial statements in accordance with U.S. generally accepted accounting principles (*US GAAP*) requires
us to make estimates and assumptions that affect the reported amounts of assets and liabilities and the disclosure of contingent assets
and liabilities at the date of the financial statements, as well as the reported revenues and expense during the reporting periods. We
base our estimates on historical experience and on various other assumptions that we believe to be reasonable under the circumstances
at the time we make such estimates. Actual results and outcomes may differ materially from our estimates, judgments, and assumptions.
We periodically review our estimates considering changes in circumstances, facts, and experience. The effects of material revisions in
estimates are reflected in the financial statements prospectively from the date of the change in estimate. Our significant accounting
policies are more fully described in Note 2 to our financial statements included elsewhere in this Annual Report.
We
define our critical accounting policies as those accounting principles that require us to make subjective estimates and judgments about
matters that are uncertain and are likely to have a material impact on our financial condition and results of operations, as well as
the specific manner in which we apply those principles. We believe the critical accounting policies used in the preparation of our financial
statements that require significant estimates and judgments are the following:
**Impairment
of Long-Lived Assets**
The
Company reviews long-lived assets, including definite-lived intangible assets, for impairment whenever events or changes in circumstances
indicate that the carrying amount of such assets may not be recoverable. The recoverability of these assets is determined by comparing
the forecasted undiscounted net cash flows of the operation to which the assets relate to the carrying amount. If the operation is determined
to be unable to recover the carrying amount of its assets, then these assets are written down first, followed by other long-lived assets
of the operation to fair value. Fair value is determined based on discounted cash flows or appraised values, depending on the nature
of the assets.
**Intangible
Assets**
The
Company records its intangible assets at cost in accordance with ASC 350, Intangibles Goodwill and Other. The Company reviews
the intangible assets for impairment on an annual basis or if events or changes in circumstances indicate it is more likely than not
that they are impaired. These events could include a significant change in the business climate, legal factors, a decline in operating
performance, competition, sale, or disposition of a significant portion of the business, or other factors.
| 43 | |
**Goodwill**
Goodwill
represents the excess of the purchase price of acquired business over the estimated fair value of the identifiable net assets acquired.
Goodwill is not amortized but is tested for impairment at least once annually, at the reporting unit level or more frequently if events
or changes in circumstances indicate that the asset might be impaired. The goodwill impairment test is applied by performing a qualitative
assessment before calculating the fair value of the reporting unit. If, on the basis of qualitative factors, it is considered not more
likely than not that the fair value of the reporting unit is less than the carrying amount, further testing of goodwill for impairment
would not be required. Otherwise, goodwill impairment is tested using a two-step approach.
The
first step involves comparing the fair value of the reporting unit to its carrying amount. If the fair value of the reporting unit is
determined to be greater than its carrying amount, there is no impairment. If the reporting units carrying amount is determined
to be greater than the fair value, the second step must be completed to measure the amount of impairment, if any. The second step involves
calculating the implied fair value of goodwill by deducting the fair value of all tangible and intangible assets, excluding goodwill,
of the reporting unit from the fair value of the reporting unit as determined in step one. The implied fair value of the goodwill in
this step is compared to the carrying value of goodwill. If the implied fair value of the goodwill is less than the carrying value of
the goodwill, an impairment loss equivalent to the difference is recorded.
**Convertible
Instruments**
The
Company evaluates and accounts for conversion options embedded in its convertible instruments in accordance with ASC 815 Derivatives
and Hedging.
ASC
815 generally provides three criteria that, if met, require companies to bifurcate conversion options from their host instruments and
account for them as free standing derivative financial instruments. These three criteria include circumstances in which (a) the economic
characteristics and risks of the embedded derivative instrument are not clearly and closely related to the economic characteristics and
risks of the host contract, (b) the hybrid instrument that embodies both the embedded derivative instrument and the host contract is
not re-measured at fair value under otherwise applicable generally accepted accounting principles with changes in fair value reported
in earnings as they occur, and (c) a separate instrument with the same terms as the embedded derivative instrument would be considered
a derivative instrument. Professional standards also provide an exception to this rule when the host instrument is deemed to be conventional
as defined under professional standards.
The
Company accounts for convertible instruments (when it has determined that the embedded conversion options should not be bifurcated from
their host instruments) in accordance with ASC 470-20 Debt Debt with Conversion and Other Options. Accordingly,
the Company records, when necessary, discounts to convertible notes for the intrinsic value of conversion options embedded in debt instruments
based upon the differences between the fair value of the underlying common stock at the commitment date of the note transaction and the
effective conversion price embedded in the note. Original issue discounts under these arrangements are amortized over the term of the
related debt to their earliest date of redemption. The Company also records, when necessary, deemed dividends for the intrinsic value
of conversion options embedded in preferred shares based upon the differences between the fair value of the underlying common stock at
the commitment date of the note transaction and the effective conversion price embedded in the note.
ASC
815-40 Derivatives and Hedging Contracts in Entitys Own Equity provides that, among other things, generally,
if an event is not within the entitys control could or require net cash settlement, then the contract shall be classified as an
asset or a liability.
**Derivative
Financial Instruments Indexed to the Companys Common Stock**
We
have generally issued derivative financial instruments, such as warrants, in connection with our equity offerings. We evaluate the terms
of these derivative financial instruments in order to determine their accounting treatment in our financial statements. Key considerations
include whether the financial instruments are freestanding and whether they contain conditional obligations. If the warrants are freestanding,
do not contain conditional obligations and meet other classification criteria, we account for the warrants as an equity instrument. However,
if the warrants contain conditional obligations, then we account for the warrants as a liability until the conditional obligations are
met or are no longer relevant. Because no established market prices exist for the warrants that we issue in connection with our equity
offerings, we must estimate the fair value of the warrants, which is as inherently subjective as it is for stock options, and for similar
reasons as noted in the stock-based compensation section above. For financial instruments which are accounted for as a liability, we
report any changes in their estimated fair values as gains or losses in our Consolidated Statement of Income.
| 44 | |
**Variable
Interest Entity (VIE) Accounting**
We
evaluate our ownership, contractual relationships and other interests in entities to determine the nature and extent of the interests,
whether such interests are variable interests and whether the entities are VIEs in accordance with ASC 810, Consolidations. These evaluations
can be complex and involve Management judgment as well as the use of estimates and assumptions based on available historical information,
among other factors. Based on these evaluations, if the Company determines that it is the primary beneficiary of a VIE, the entity is
consolidated into the financial statements.
**Investments
- Equity Method**
The
Company accounts for equity method investments at cost, adjusted for the Companys share of the investees earnings or losses,
which are reflected in the consolidated statements of operations. The Company periodically reviews the investments for other than temporary
declines in fair value below cost and more frequently when events or changes in circumstances indicate that the carrying value of an
asset may not be recoverable.
The
Investment in GMP Bio represents the investment into equity securities for which the Company elected the fair value option pursuant to
ASC 825-10-15 and subsequent fair value changes in the GMP Bio shares are included in the result from continuing operations. Refer to
Note 6 of these Notes to the Consolidated Financial Statements.
**Joint
Venture agreement**
We
have equity interest in unconsolidated arrangement that is primarily engaged in the business of drug discovery, development, and commercialization,
including but not limited to development and commercialization of TGF-beta therapeutics as well as establishing and operating contract
development and manufacturing organization (CDMO) facilities and capabilities. The Company first reviewed the arrangement to determine
if it meets the definition of an accounting joint venture pursuant to ASC 323-10-20. In order to meet the definition of a joint venture,
the arrangement must have all of the following characteristics, (i) the arrangement is organized within a separate legal entity, (ii)
the entity is under the joint control of the venturers, (iii) the venturers must be able to exercise joint control through their equity
investments, (iv) the qualitative characteristics of the entity, including its purpose and design must be consistent with the definition
of a joint venture
We
consolidate arrangements that are considered to be VIEs where we are the primary beneficiary. We analyze our investments in joint ventures
to determine if the joint venture is considered a VIE and would require consolidation. We (i) evaluate the sufficiency of the total equity
investment at risk, (ii) review the voting rights and decision-making authority of the equity investment holders as a group and whether
there are limited partners (or similar owning entities) that lack substantive participating or kick out rights, guaranteed returns, protection
against losses, or capping of residual returns within the group and (iii) establish whether activities within the venture are on behalf
of an investor with disproportionately few voting rights in making this VIE determination. To the extent that we own interests in a VIE
and we (i) have the power to direct the activities that most significantly impact the economic performance of the VIE and (ii) have the
obligation or rights to absorb losses or receive benefits that could potentially be significant to the VIE, then we would be determined
to be the primary beneficiary and would consolidate the VIE. To the extent that we own interests in a VIE, then at each reporting period,
we re-assess our conclusions as to which, if any, party within the VIE is considered the primary beneficiary. To the extent that our
arrangements do not qualify as VIEs, they are consolidated if we control them through majority ownership interests or if we are the managing
entity (general partner or managing member) and our partner does not have substantive participating rights. Control is further demonstrated
by our ability to unilaterally make significant operating decisions, refinance debt, and sell the assets of the joint venture without
the consent of the non- managing entity and the inability of the non-managing entity to remove us from our role as the managing entity.
We use the equity method of accounting for those arrangements where we exercise significant influence but do not have control. Under
the equity method of accounting, our investment in each arrangement is included on our consolidated balance sheet; however, the assets
and liabilities of the joint ventures for which we use the equity method are not included on our consolidated balance sheet.
| 45 | |
When
we sell or contribute properties to unconsolidated arrangements and retain a non-controlling ownership interest in such assets, we recognize
the difference between the consideration received and the carrying amount of the asset sold or contributed when its derecognition criteria
are met. The equity method investment we retain in such partial sale transactions is noncash consideration and is measured at fair value.
As a result, the accounting for a partial sale will result in the recognition of a full gain or loss. When circumstances indicate there
may have been a reduction in the value of an equity investment, we evaluate whether the loss in value is other than temporary. If we
conclude it is other than temporary, we recognize an impairment charge to reflect the equity investment at fair value. The Company elected
the fair value option under the fair value option Subsection of Section 825-10-15 to account for its equity-method investment.
**Research
and Development Expense**
Research
and development expense consists of costs we incur for the development of our investigational drugs and, to a lesser extent, for preclinical
research activities. Research and development costs are expensed as incurred. Research and development expense include clinical trial
costs, salaries, and benefits of employees, including associated stock-based compensation, payments to clinical investigators, drug manufacturing
costs, laboratory supplies and facility costs. Clinical trial costs are a significant component of our research and development expenses,
and these can be difficult to accurately estimate. Included in clinical trial costs are fees paid to other entities that conduct certain
research and development activities on our behalf, such as clinical research organizations, or CROs. We estimate clinical trial expense
based on the services performed pursuant to contracts with research institutions such as CROs and the actual clinical investigators.
These estimates are based on actual time and expenses incurred by the CRO and the clinical investigators. Also included in clinical trial
expense are costs based on the level of patient enrollment into the clinical trial and the actual services performed under the related
clinical trial agreement. Changes in clinical trial assumptions, such as the length of time estimated to enroll all patients, rate of
screening failures, patient drop-out rates, number and nature of adverse event reports and the total number of patients enrolled can
impact the average and expected cost per patient and the overall cost of the clinical trial. Based on patient enrollment reports and
services provided, we may periodically adjust estimates for the clinical trial costs. If we do not identify costs that we have begun
to incur or if we underestimate or overestimate the level of services performed, the length of time for these services or the costs of
these services, our actual expenses could differ from our estimates.
**Share-Based
Compensation**
We
record the estimated fair value of all share-based payments issued to employees and other service providers. Our share-based payments
consist primarily of stock options. The valuation of stock options is an inherently subjective process, since market values are not available
for any stock options in our equity securities. Market values are also not available on long-term, non-transferable stock options in
other equity securities. With no market values on options to trade in our common stock and no comparable market values on any long-term
non-transferable stock options, the process of valuing our stock options is even more uncertain and subjective. Accordingly, we use a
Black-Scholes option pricing model to derive an estimated fair value of the stock options which we issue. The Black-Scholes option pricing
model requires certain input assumptions, including the expected term of the options and the expected volatility of our common stock.
Changes in these assumptions could have a material impact on the estimated fair value that we record for share-based payments that we
issue. We determine the term of the options based on the simplified method, which averages the vesting period and the contractual life
of the stock option. We determine the expected volatility based on the historical volatility of our common stock over a period commensurate
with the options expected term. The Black-Scholes option pricing model also requires assumptions for risk-free interest rates
and the expected dividend yield of our common stock, but we feel that these values are more objective and note that changes in these
values do not have a significant impact on the estimated value of the options when compared to the volatility and term assumptions.
We
are also required to estimate the level of award forfeitures expected to occur and record compensation expense only for those awards
that are ultimately expected to vest. Accordingly, we perform a historical analysis of option awards that are forfeited prior to vesting,
and record total stock option expense that reflects this estimated forfeiture rate.
| 46 | |
*Results
of Operations*
**Years
Ended December 31, 2024, and 2023.**
A
comparison of the Companys operating results for the year ended December 31, 2024, and 2023, respectively, is as follows.
| 
| | 
December 31, 2024 | | | 
December 31, 2023 | | | 
Variance | | |
| 
Service revenue | | 
| - | | | 
| 70,000 | | | 
| (70,000 | ) | |
| 
Total revenue | | 
| | | | 
| 70,000 | | | 
| | | |
| 
Operating expense: | | 
| | | | 
| | | | 
| | | |
| 
Research and development | | 
$ | - | | 
$ | 61,143 | | | 
$ | (61,143 | ) | |
| 
General and administrative | | 
| 376,013 | | | 
| 573,726 | | | 
| (197,713 | ) | |
| 
Goodwill impairment | | 
| 3,200,000 | | | 
| 6,083,146 | | | 
| (2,883,146 | ) | |
| 
Total operating expense | | 
| 3,576,013 | | | 
| 6,718,015 | | | 
| (3,142,002 | ) | |
| 
| | 
| | | | 
| | | | 
| | | |
| 
Income (loss) from operations | | 
| (3,576,013 | ) | | 
| (6,648,015 | ) | | 
| 3,072,002 | | |
| 
Interest expense, net | | 
| (857,723 | ) | | 
| (1,044,786 | ) | | 
| 187,063 | | |
| 
Reimbursement for expenses related party | | 
| 22,937 | | | 
| 72,246 | | | 
| (49,309 | ) | |
| 
Change in fair value of investment in GMP Bio | | 
| - | | | 
| 12,706 | | | 
| (12,706 | ) | |
| 
Change in the value of derivatives on debt | | 
| (280,402 | ) | | 
| (225,074 | ) | | 
| (55,328 | ) | |
| 
Loss on debt conversion | | 
| (88,258 | ) | | 
| (373,142 | ) | | 
| 284,884 | | |
| 
| | 
| | | | 
| | | | 
| | | |
| 
Net loss before controlling interests | | 
$ | (4,779,459 | ) | | 
$ | (8,206,065 | ) | | 
$ | 3,426,606 | | |
Net
Loss
We
recorded a net loss of approximately $4.8 million for the year ended December 31, 2024 compared to a net loss of approximately $8.2
million for same period in 2023. The lower net loss of approximately $3.4 million for the year ended December 31, 2024, as compared
to the same period of 2023 was primarily due to recording of lower impairment to goodwill in 2024 by approximately $2.9 million,
approximately $0.1 million of lower research and development expenses and $0.2 million of lower general and
administrative expenses, offset by lower loss recorded on conversion of debt of approximately $0.3
million, lower interest expense by approximately $0.2 million, offset by lower reimbursement for expenses from a related party of
approximately $50 thousand and higher change in value of derivatives on debt by approximately $55 thousand.
Service
Revenue
During
the year ended December 31, 2024, no service revenue was recorded, as compared to a service revenue of $70,000 received from the
Biomedical Advanced Research and Development Authority for certain services related to our work on their Long COVID-19 research, for
the year ended December 31, 2023.
Research
and Development Expense
Research
and Development (*R&D*) expense decreased by approximately $62 thousand, due to a reversal of expenses of approximately
$1 thousand for the year ended December 31, 2024, as compared to $61 thousand for the year ended December 31, 2023, primarily due to other
operational expenses related to OT-101 being borne by the JV.
As
previously disclosed, and as a result of our JV, we expect our R&D expense to decrease for the remainder of the year 2024, specifically
for activities related to OT-101, including the initiation of new clinical trials. Any other development expenses will be subject to
our continuing ability to secure sufficient funding to continue planned operations.
| 47 | |
General
and Administrative Expense
General
and administrative (*G&A*) expense decreased by approximately $0.2 million, to approximately $0.4 million for
the year ended December 31, 2024, as compared to approximately $0.6 million for the same period of 2023, due to lower administrative
expenses.
Goodwill
Impairment
We
recorded a goodwill impairment of approximately $3.2 million on the approximately $16.2 million goodwill, which we recorded upon our
acquisition of PointR, for the year ended December 31, 2024, compared to impairment of $6.1 million recorded during the same period in
2023.
During
2024, our stock price, solely based on the market capitalization of our Company, and the general economic conditions, which adversely
impacted the majority of the pharmaceutical and biotechnology industry, were indicative of a potential impairment of our goodwill. While
we evaluated and concluded that the AI technologies related to the PointR acquisition are not adversely impacted at this time, and the
Company continues to develop other AI technologies, the significant reduction of our market capitalization required us to record an impairment
on the goodwill to the extent of the difference between the net assets of the Company over the fair value based on the market capitalization
during the year.
Interest
Expense
We
recorded interest expense, including amortization of debt costs, of approximately $0.9 million for the year ended December 31, 2024,
primarily in connection with debt raised from various convertible notes and the two private placements through JH Darbie, November/December
2021 Financing and May/June 2022 financing as compared to approximately $1.0 million for the same period of 2023, in connection with
debt raised from convertible notes and JH Darbie during 2023. For more information on debt raised from convertible notes and the JH Darbie
Financing, see Note 5, Note 7 and Note 8 of the Consolidated Financial Statements of this Annual Report.
Reimbursement
of expenses
The
Company was reimbursed approximately $20 thousand, by Autotelic Inc. a related party, during the year ended December 31, 2024 for expenses
incurred by the Company on behalf of our JV, compared to reimbursement of approximately $72 thousand during the year ended December 31,
2023.
Change
in fair value of investment in GMP Bio
We
have recorded no change in fair value of our investment in GMP Bio for the year ended December 31, 2024, compared to a change of approximately
$13,000 for the year ended December 31, 2023, based on third-party fair valuation of GMP Bio in accordance with US GAAP. As of December
31, 2024, the Company assessed the fair value of its investment in the JV and determined that no change in the fair value was required,
until a triggering event has occurred, similar to, but not limited to, any fund raising event, entering into an IPO or any other major
event enabling the Company to reassess the fair value of its investment in the JV.
Change
in value of derivatives
During
the year ended December 31, 2024, we recorded a loss of approximately $0.3 million, as compared to approximately $0.2 million recorded
during the year ended December 31, 2023, due to the change in value of derivatives on the notes issued to our CEO and the bridge investors.
| 48 | |
Loss
on Conversion of Debt
During
the year ended December 31, 2024, we recorded a loss on conversion of debt of approximately $0.1 million, as compared to a similar loss
of approximately $0.4 million during the same period of 2023.
**Liquidity,
Financial Condition and Capital Resources ($s in 000s)**
| 
| | 
December 31, | | | 
December 31, | | |
| 
| | 
2024 | | | 
2023 | | |
| 
Cash, including restricted cash | | 
$ | 106 | | | 
$ | 190 | | |
| 
Working capital | | 
| (19,065 | ) | | 
| (16,233 | ) | |
| 
Stockholders Equity | | 
| 8,252 | | | 
| 11,611 | | |
The
Company has experienced net losses every year since inception and as of December 31, 2024, had an accumulated deficit of approximately
$38 million, including approximately $3.2 million goodwill impairment recorded during the year 2024. As of December 31, 2024, the Company
had approximately $0.1 million in cash and current liabilities of approximately $19.2 million, of which approximately $1.3 million are
net assumed liabilities of the Company as part of the Oncotelic Inc. reverse merger, $4.7 million of debt, including accrued interest,
related to debt for conducting clinical trials for OT-101 from GMP and $2.6 million is contingent liability to issue common shares of
the Company to PointR shareholders upon achievement of certain milestones. Management expects to incur significantly lower costs losses,
especially due to the transfer of costs over to the JV, especially in connection with the development of OT-10, in the foreseeable future
but also recognizes the need to raise capital to remain viable. The Companys limited capital resources, history of recurring losses
and uncertainties as to whether the Companys operations will become profitable raise substantial doubt about its ability to continue
as a going concern. The financial statements contained in this report do not include any adjustments related to the recoverability of
assets or classifications of liabilities that might be necessary should the Company be unable to continue as a going concern.
The
principal source of the Companys working capital deficit to date has been the issuance of convertible notes, a substantial part
of which has been provided by officers and certain insiders, and sale of equity under the EPA with Peak One. The Company will need to
raise additional capital in order to fund its operations and continue development of its product candidates. The Company is evaluating
the options to further the development of the Companys product candidates, AL-101, Artemisinin for COVID-19, developing AI technologies
to support the COVID-19 therapies; in addition to evaluating the development pathway of its product candidates; OXi4503 and/or CA4P.
The Company is also independently planning to develop OT-101 for certain animal health indications and contemplating using crypto currencies
for that platform. The Company has been developing OT-101 for various cancers, as well as a nanoparticle platform through the JV. Substantial
development on that front has occurred during the past year.
The
Company anticipates raising substantial additional capital through the sale of equity securities and/or debt, but no new financing arrangements
are in place at this time.
If
the Company is unable to access additional funds when needed, it may not be able to continue the development of these investigational
drugs and the Company could be required to delay, scale back or eliminate some or all of its development programs and operations. Any
additional equity financing, if available, would be dilutive to the current stockholders and may not be available on favorable terms.
Additional debt financing, if available, may involve restrictive covenants and could also be dilutive. The Companys ability to
access capital is not assured and, if access is not achieved on a timely basis, would materially harm the Companys financial condition,
the value of its common stock and its business prospects.
**Cash
Flows ($s in 000s)**
| 
| | 
Year ended December 31, | | |
| 
| | 
2024 | | | 
2023 | | |
| 
Net cash used in operating activities | | 
$ | (740 | ) | | 
$ | (1,321 | ) | |
| 
Net cash provided by financing activities | | 
| 656 | | | 
| 1,250 | | |
| 
Increase/ (decrease) in cash | | 
$ | (84 | ) | | 
$ | (71 | ) | |
| 49 | |
****
Operating
Activities
For
the year ended December 31, 2024, net cash used in operating activities was approximately $0.7 million. This was due to the net loss
of approximately $4.8 million, primarily reduced by approximately $3.2 million of goodwill impairment, approximately $0.3 million due
to a change in fair value of derivatives, approximately $0.1 million of amortization of debt and finance discounts, approximately $0.1
million of loss on conversion of debt and increased by approximately $0.3 million due to changes in operating assets and liabilities.
For
the year ended December 31, 2023, net cash used in operating activities was approximately $1.3 million. This was due to the net loss
of approximately $8.2 million, primarily reduced by approximately $0.2 million due to a change in fair value of derivatives, approximately
$6.1 million of goodwill impairment, approximately $0.3 million of amortization of debt and finance discounts, approximately $0.4 million
of loss on conversion of debt and increased by approximately $0.1 million due to changes in operating assets and liabilities.
Financing
Activities
For
the year ended December 31, 2024, net cash provided by financing activities was approximately $0.7 million due to approximately $0.7
million raised through short term loans.
For
the year ended December 31, 2023, net cash provided by financing activities was approximately $1.3 million. Net cash provided was due
to approximately $1.4 million raised through short term loans and repayments of approximately $0.1 million.
*Off-Balance
Sheet Arrangements*
We
have no off-balance sheet arrangements.
*Effects
of Inflation*
We
do not believe that inflation has had a material impact on our business, revenues or operating results during the periods presented.
**Contractual
Obligations**
Our
current drug development programs are based on a series of compounds called combretastatins, which we have exclusively licensed from
Arizona State University, or ASU. If our current drug candidates are approved, we will be required to pay low to mid-single-digit royalties
on future net sales of products associated with the ASU patent rights until these patent rights expire.
We
also have an exclusive license from Bristol-Myers Squibb, or BMS, for certain patent rights to particular combretastatins, including
CA4P. If CA4P is approved, we will be required to pay low-single-digit royalties on future net sales of products associated with the
BMS patent rights until these patent rights expire.
**ITEM
7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK**
Our
cash is maintained in U.S. dollar accounts. We have adopted a policy for the cash that we hold, and also for any cash equivalents and
investments that we may hold, the primary objective of which is to preserve principal, while also maintaining liquidity to meet our operating
needs and maximize yields to the extent possible. Although our investments can be subject to credit risk, we follow procedures to limit
the amount of credit exposure in any single issue, issuer or type of investment. Our investments are also subject to interest rate risk
and would be likely to decrease in value if market interest rates increase. However, due to the generally conservative nature of our
investments and relatively short duration, we believe that interest rate risk is mitigated.
Although
we may, from time-to-time, manufacture drugs and conduct preclinical or clinical trials outside of the United States, we believe our
exposure to foreign currency risk to be immaterial.
| 50 | |
**ITEM
8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA**
See
Item 15 for a list of our Financial Statements and Schedules and any supplementary financial information filed as part of this Annual
Report.
**ITEM
9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE**
None
**ITEM
9A. CONTROLS AND PROCEDURES**
*Evaluation
of Disclosure Controls and Procedures*
We
maintain disclosure controls and procedures that are designed to ensure that information required to be disclosed in our reports under
the Exchange Act is recorded, processed, summarized and reported within the time periods specified in the SECs rules and forms,
and that such information is accumulated and communicated to our management, including our principal executive officer and principal
financial officer, as appropriate, to allow timely decisions regarding required disclosures. In designing disclosure controls and procedures,
our management was required to apply its judgment in evaluating the cost-benefit relationship of possible disclosure controls and procedures.
The design of any disclosure controls and procedures also is based in part upon certain assumptions about the likelihood of future events,
and there can be no assurance that any design will succeed in achieving its stated goals under all potential future conditions. Any controls
and procedures, no matter how well designed and operated, can provide only reasonable, not absolute, assurance of achieving the desired
control objectives.
As
required by Rule 13a-15(b) under the Securities Exchange Act of 1934, as amended (the *Exchange Act*) our Chief Executive
Officer (*CEO*) and our Chief Financial Officer (*CFO*) conducted an evaluation as of the end of
the period covered by this Annual Report on Form 10-K, of the effectiveness of our disclosure controls and procedures as defined in Rules
13a-15I and 15d-15(e) under the Exchange Act. Based on that evaluation, our CEO and our CFO each concluded that our disclosure controls
and procedures are not effective to provide reasonable assurance that information required to be disclosed in the reports that we file
or submit under the Exchange Act, (i) is recorded, processed, summarized and reported within the time periods specified in the Securities
and Exchange Commissions rules and forms and (ii) is accumulated and communicated to our management, including our CEO and our
CFO, as appropriate to allow timely decisions regarding required disclosure.
*Material
Weaknesses in Internal Control over Financial Reporting*
Management
conducted an assessment of the effectiveness of our internal control over financial reporting as of December 31, 2024 based on the framework
established in Internal ControlIntegrated Framework (2013) issued by the Committee of Sponsoring Organizations of the Treadway
Commission. Based on this assessment, management has determined that the Registrants internal control over financial reporting
as of December 31, 2024, was not effective as a result of certain material weaknesses.
A
material weakness is a deficiency, or a combination of deficiencies, in internal control over financial reporting such that there is
a reasonable possibility that a material misstatement of our annual or interim financial statements will not be prevented or detected
on a timely basis.
The
ineffectiveness of our internal control over financial reporting was due to the following material weaknesses which are observed in many
small companies with a small number of accounting and financial reporting staff:
| 
| 
Lack
of formal policies and procedures; | |
| 
| 
| |
| 
| 
Lack
of adequate independent directors on the Companys board of directors and committees to oversee financial reporting responsibilities; | |
| 51 | |
| 
| 
Inadequate
or lack of segregation of duties; | |
| 
| 
| |
| 
| 
Lack
of dedicated resources and experienced personnel to design and implement internal control procedures to support financial reporting
objectives; | |
| 
| 
| |
| 
| 
Lack
of risk assessment procedures on internal controls to detect financial reporting risks on a timely manner. | |
*Managements
Plan to Remediate the Material Weaknesses*
Management
continues to plan implementing and continues to implement measures, subject to the availability of resources required to design and maintain
such controls, designed to ensure that control deficiencies contributing to the material weakness are remediated, such that these controls
are designed, implemented, and operating effectively. The implementation and remediation measures are planned subject to the availability
of financial and therefore human resources. The remediation actions planned include:
| 
| 
Continue
to search for, evaluate and recruit qualified independent outside directors; | |
| 
| 
| |
| 
| 
Once
independent directors are on Board, to augment or replace the non-independent directors to the Audit Committee and other committees. | |
| 
| 
| |
| 
| 
Identify
gaps in our skills base and the expertise of our staff required to meet the financial reporting requirements of a public company;
and | |
| 
| 
| |
| 
| 
Continue
to develop policies and procedures on internal control over financial reporting and monitor the effectiveness of operations on existing
controls and procedures. | |
*Changes
in Internal Control over Financial Reporting*
During
the year ended December 31, 2024, we continued to work on our planned implementation and remediation actions which are all intended to
strengthen our overall control environment, within the limited resources available to us. We have made some progress in our planned remediation
efforts, and we expect the Company to complete its planned execution of internal controls over financial reporting depending on the availability
of resources.
We
are committed to maintaining a strong internal control environment and believe that these remediation efforts will represent significant
improvements in our control environment. Our management will continue to monitor and evaluate the relevance of our risk-based approach
and the effectiveness of our internal controls and procedures over financial reporting on an ongoing basis and is committed to taking
further action and implementing additional enhancements or improvements, as necessary and as funds allow.
**ITEM
9B. OTHER INFORMATION**
None.
| 52 | |
****
**PART
III**
**ITEM
10. DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE**
The
following table sets forth certain information about our current directors and executive officers followed by individual biographies
of the directors and executive officers of the Company, including their business experience and other relevant information as of December
31, 2024.
| 
Name | 
| 
Age | 
| 
Position | |
| 
Vuong
Trieu, Ph. D. | 
| 
60 | 
| 
Chairman
of the Board and Chief Executive Officer | |
| 
Amit
Shah | 
| 
58 | 
| 
Chief
Financial Officer | |
| 
Saran
Saund | 
| 
67 | 
| 
Chief
Business Officer | |
| 
Anthony
E. Maida III | 
| 
72 | 
| 
Chief
Medical Officer Translation Medicine & Director | |
| 
Steven
W. King | 
| 
60 | 
| 
Director
and Consultant | |
| 
Seymour
Fein, M.D. | 
| 
76 | 
| 
Chief
Regulatory Officer and Chief Medical Officer (Consultant) | |
*Vuong
Trieu, Ph.D.* was the founder and Chairman of the Board of Directors of Oncotelic Inc., having served in such capacity since 2014,
and now serves as the Companys Chief Executive Officer (*CEO*) and Chairman of the Board of Directors. Dr.
Trieu has been involved in drug discovery, development, and commercialization for over 25 years, including his contributions as co-inventor
of Abraxane. He previously served as Executive Chairman and Interim CEO of Marina Biotech, Inc. from 2016 to 2018. Marina Biotech
was a developer of tkRNA for the treatment of FAP/CRC (Familial adenomatous polyposis/ Colorectal Cancer). Prior to that, he also served
as President and CEO of IgDraSol, Inc. a developer of a 2nd generation Abraxanebeginning in 2012 until its acquisition
by Sorrento Therapeutics, Inc. in 2013. He served as Chief Scientific Officer for Sorrento Therapeutics, Inc. and a member of that companys
board of directors from 2013 until 2014. Previously, Dr. Trieu was Senior Director of Pharmacology/Biology at Abraxis Bioscience/Celgene,
where he led the preclinical, clinical and PK/biomarker development of Abraxane, and was the co-inventor of the intellectual property
covering Abraxane. Earlier in his career, Dr. Trieu held positions at Genetic Therapy/Sandoz (leading the adenoviral gene therapy program
against atherosclerosis), Applied Molecular Evolution (AME)/Lily (leading the expression, purification, and preclinical testing of mAb
therapeutics) and Parker Hughes Institute (Director of Cardiovascular Biology program that evaluated a series of small molecules and
biologics against preclinical models of atherosclerosis, dyslipidemia, stroke, ALS, and restenosis). Dr. Trieu holds a PhD in Microbiology,
BS in Microbiology and Botany. He is a member of ENDO, ASCO, AACR, and many other professional organizations. Dr. Trieu is published
widely in oncology, cardiovascular, and drug development.
Dr.
Trieu has over 100 patent applications and 39 issued U.S. patents.
The
Board believes that Dr. Trieus extensive experience as an executive at various biotechnology and biopharmaceutical companies as
well as his service on private and public company boards qualifies him to serve on the Board.
*Amit
Shah* was appointed as our Chief Financial Officer effective in July 2019. Mr. Shah has served as a senior financial officer for a
number of life science companies, including Chief Financial Officer at Marina Biotech, Inc., a publicly traded biotechnology company
from 2017 to 2018; Vice President of Finance & Accounting Insightra Medical Inc. from 2014 to 2015, Acting Chief Financial Officer
of Insightra Medical Inc. in 2015; VP Finance and Acting Chief Financial Officer at IgDraSol Inc. in 2013; Corporate Controller &
Director of Finance at ISTA Pharmaceuticals from 2010 to 2012; Corporate Controller at Spectrum Pharmaceuticals from 2007 to 2010: and
as Controller / Senior Manager Internal Audits at Caraco Pharmaceuticals Laboratories from 2000 to 2007. In addition to his work with
life sciences companies, Mr. Shah served as the Chief Financial Officer at Eagle Business Performance Services, a management consulting
and business advisory firm from end of 2018 through March 2019 and as a consultant and ultimately Senior Director of Finance 
ERP, at Youngs Market Company from 2015 to 2017. Mr. Shah received a Bachelors of Commerce degree from the University of
Mumbai, and is an Associate Chartered Accountant from The Institute of Chartered Accountants of India. Mr. Shah is also an inactive CPA
from Colorado, USA.
| 53 | |
*Saran
Saund*has served as the Chief Business Officer of the Company since November 2019. Prior to that, he was the Chief Executive Officer
and Founder of PointR Data Inc. from 2016 to 2019 where the revenue generating startup developed an innovative AI for cashier-less automated
retail stores. From 2013 to 2016 Saran Saund served as managing partner of Astralync LLC that specialized in open source AI frameworks
and developed an industry consortium. Previously, Saran Saund held positions as General Manager, founder and CEO at various companies,
including Cambridge Silicon Radio (acquired by Qualcomm), Marvell Semiconductors Inc., and PicoMobile Inc (acquired by Marvell). Mr.
Saund received his MSc. Tech in Computer Science from BITS Pilani (India) and MS Computer Science from Penn State University.
*Anthony
E. Maida III, Ph.D., M.A., M.B.A.*was appointed to the Board in May 2020. Dr, Maida was also appointed as a consultant Chief Medical
Officer of the Company in April 2020. Dr. Maida has been involved in the clinical development of immunotherapy for over 27 years in various
executive management positions. Since June 2010 till June 2020, Dr. Maida served as Senior Vice President, Clinical Research for Northwest
Biotherapeutics, Inc., a cancer vaccine company focused on therapy for patients with glioblastoma multiforme and prostate cancer. From
June 2009 through June 2010, Dr. Maida served as Vice President of Clinical Research and General Manager, Oncology, Worldwide for PharmaNet,
Inc., a clinical research organization. From 1997 through 2010, Dr. Maida served as Chairman, Founder and Director of BioConsul Drug
Development Corporation and Principal of Anthony Maida Consulting International, advising pharmaceutical and investment firms, in the
clinical development of therapeutic products and product/company acquisitions. From 1992 to September of 1999, Dr. Maida was President
and Chief Executive Officer of Jenner Biotherapies, Inc., an immunotherapy company. Dr. Maida is currently a member of the board of directors
and audit chair of Spectrum Pharmaceuticals, Inc. and Vitality Biopharma, Inc. (OTCQB: VBIO) and was formerly a member of the board of
directors and audit chair of OncoSec Medical Inc. (OTCQB: ONCS). Dr. Maida holds a B.A. in Biology and History, an M.B.A., an M.A. in
Toxicology and a Ph.D. in Immunology. He is a member of the American Society of Clinical Oncology, the American Association for Cancer
Research, the Society of Neuro-Oncology, the International Society for Biological Therapy of Cancer and the American Chemical Society.
The
Board believes that Dr. Maida is qualified to serve on the Board and as the consultant Chief Medical Officer due to his extensive experience
as an executive at various biotechnology and biopharmaceutical companies as well as his service on private and public company boards.
*Steven
W. King*was appointed to the Board in May 2020. He previously served as the CEO of Peregrine Pharmaceuticals, Inc. and its wholly
owned biomanufacturing subsidiary Avid Bioservices, Inc., during which time the company advanced its lead compound through Phase 3 development,
while growing revenues to over $55 million. Prior to joining Peregrine, Mr. King was employed at Vascular Targeting Technologies, Inc.,
which was acquired by Peregrine in 1997. Mr. King served in a variety of executive roles at Peregrine, including Director of Research
and Development from 1997 to 2000; Vice President Technology and Product Development from 2000 to 2002; Chief Operating Officer from
2002 to 2003; and Chief Executive Officer from 2003 to 2017. Mr. King served on the board of directors of Peregrine from 2003 until 2017.
Mr. King previously worked at the University of Texas Southwestern Medical Center and is co-inventor on over 40 U.S. and foreign patents
and patent applications in the vascular targeting agent field. Mr. King received his Bachelors and Masters degrees from
Texas Tech University in Cell and Molecular Biology. The Board believes Mr. King is qualified to serve as a director because of his extensive
scientific understanding of technologies in development and expertise in developing and manufacturing biologics, combined with the perspective
and experience he brings from having previously served on the boards of public companies.
*Seymour
Fein, M.D.* was appointed to in May 2022 as the Companys Consulting Chief Regulatory Officer. Dr. Fein has been managing partner
of the clinical and regulatory consulting organization, CNF Pharma, LLC for the last 20 years and in that capacity has worked closely
with numerous new drug reviewing divisions at the FDA including the divisions of oncologic drug products. Dr. Feins professional
activities have been focused on drug development research for over 35 years. He has been extensively involved in the successful development
of numerous drugs, biologics and medical devices during this time leading to FDA approvals for over 20 drugs (NDAs, sNDAs, BLAs) and
devices (PMAs). Dr. Fein began his career at Hoffmann-La Roche Ltd. as a senior research physician and was responsible for a clinical
development program that led to U.S. Food and Drug Administration (FDA) approval of recombinant interferon-alpha for cancer treatment.
Dr. Fein was also the medical director of Bayer Healthcare Pharmaceuticals (U.S.) where he was responsible for therapeutic areas including
gastroenterology, oncology, and cardiology. He later served as medical director for Rorer Group (now part of Sanofi) and Ohmeda (now
part of Baxter). Dr. Fein founded and has been managing partner of a clinical and regulatory consulting organization and has worked closely
with the numerous new drug review divisions at the FDA including the divisions of oncologic drug products. Dr. Fein has successfully
overseen entrepreneurial drug development leading to the FDA approval of two orphan drug products in the field of gastroenterology and
the first drug approved for the treatment of nocturia in the field of urology. Dr. Fein received his B.A. degree from the University
of Pennsylvania and his M.D. degree with honors from New York Medical College. He completed a three-year residency in internal medicine
at Dartmouth and a three-year fellowship in medical oncology and hematology at Harvard Medical School, where he served as an instructor
of medicine during his final fellowship year. Dr. Fein is board-certified in both oncology and internal medicine.
| 54 | |
The
Board had three standing committees, which consisted of the Audit Committee, the Compensation Committee and the Nominating and Corporate
Governance Committee (collectively, the *Committees*), We have discontinued all the Committees since July 2021 and
since that date, the full Board serves in lieu of all Committees. Once we engage new directors to the Board, we will restart the Committees,
and the members will serve on these committees until their resignation or as otherwise determined by our Board.
*Audit
Committee*
For
the year ended December 2024, the full Board acted in lieu of an Audit Committee. The full Board met four times during the year ended
December 31, 2024 in lieu of the Audit Committee.
Our
Audit Committee had the authority to retain and terminate the services of our independent registered public accounting firm, reviews
our annual financial statements, considers matters relating to accounting policy and internal controls, and reviews the scope of our
annual audits. Such functions are currently being managed by our full Board.
The
Board had adopted a charter for the Audit Committee, which is to be reviewed and reassessed annually by the Audit Committee. Due to a
lack of the Committee, such review and evaluation has not been done. A copy of the Audit Committees written charter is publicly
available on our website at www.oncotelic.com.
*Compensation
Committee*
For
the year ended December 2024, the full Board acted in lieu of Compensation Committee. The full Board did not meet during the year ended
December 31, 2024, since there were no compensation-based decisions to be made considering all the employees of the Company being paid
by the JV.
The
Compensation Committees responsibilities include making recommendations to the Board regarding the compensation philosophy and
compensation guidelines for our executives, the role and performance of our executive officers, and appropriate compensation levels for
our CEO, which are determined without the CEO present, and other executives based on a comparative review of compensation practices of
similarly situated businesses. The Compensation Committee also makes recommendations to the Board regarding the design and implementation
of our compensation plans and the establishment of criteria and the approval of performance results relative to our incentive plans.
Our Compensation Committee also administers our 2005 Stock Plan, our 2015 Equity Incentive Plan and our 2017 Equity Incentive Plan. Currently,
none of the members of the Compensation Committee qualifies as independent under the definition promulgated by The NASDAQ Stock Market
and qualifies as a Non-Employee Director within the meaning of Rule 16b-3 under the Exchange Act.
The
Compensation Committee shall review and assess the three main components of each named executive officers compensation: base salary,
incentive compensation, and equity compensation. Adjustments to base salary are generally only made when there has been a change in the
scope of the responsibilities of the named executive officer or when, based on a review of the base salary component of executive officers
in companies of a similar size and stage of development, the Compensation Committee members believe that an adjustment is warranted in
order to remain competitive. The executive management of the Company determines and agrees with the Compensation Committee on its corporate
goals and objectives for the ensuing year. At the end of each year, the attainment of each objective is assessed and incentive awards
may be made to each executive based on his or her contribution to achieving the objectives. Awards are made based on either provision
of an executives employment agreement, or an assessment of each executives equity compensation position relative to the
Companys other executives.
The
Compensation Committee also typically reviews our director compensation on at least an annual basis. The Compensation Committee has the
authority to directly retain the services of independent consultants and other experts to assist in fulfilling its responsibilities.
Currently there are no independent compensation consultants retained by the Company.
| 55 | |
*Nominating
and Governance Committee*
For
the year ended December 2024, the Company had no Nominating and Governance Committee. The full Board acted in lieu of the Nominating
and Governance Compensation Committee. The full Board did not meet during the year ended December 31, 2024, since there were no nominating
or governance based decisions to be made.
The
Nominating and Governance Committees responsibilities include making recommendations to the full Board as to the size and composition
of the Board and making recommendations as to particular nominees to the Board. All members of the Nominating and Governance Committee
qualify as independent under the definition promulgated by The NASDAQ Stock Market.
**Board
Attendance at Board of Directors, Committee and Stockholder Meetings**
Our
Board met 5 times, which included 4 times in lieu of the Audit Committee, approved certain corporate actions by unanimous written consents
1 time during the fiscal year ended December 31, 2024. Each of our directors serving during fiscal 2024 attended all the meetings of
the Board and in lieu of the Committees of the Board upon which such director served and that were held during the year ended December
31, 2024.
Although
we do not have a formal policy regarding attendance by members of the Board at our annual meeting of stockholders, directors are encouraged
to attend.
**Board
Leadership Structure**
Our
Board has the discretion to determine whether to separate or combine the roles of Chair of the Board and Chief Executive Officer. Dr.
Trieu has served in both roles since his appointment to the Board after the reverse merger with Oncotelic and our Board continues to
believe that his combined role is most advantageous to the Company and its stockholders. Dr. Trieu possesses in-depth knowledge of the
issues, opportunities and risks facing us, our business and our industry and is best positioned to fulfill the Board Chairs responsibility
to develop meeting agendas that focus the Boards time and attention on critical matters and to facilitate constructive dialogue
among Board members on strategic issues.
In
addition to Dr. Trieus leadership, the Board maintains effective independent oversight through a number of governance practices,
including, open and direct communication with management, input on meeting agendas, and regular executive sessions.
**Risk
Oversight**
Our
Board oversees a company-wide approach to risk management, determines the appropriate risk level for us generally, and assesses the specific
risks faced by us to reviews the steps taken by management to mitigate those risks. Although our Board has ultimate oversight responsibility
for the risk management process, its committees oversee risk in certain specified areas.
Specifically,
our Compensation Committee is responsible for overseeing the management of risks relating to our executive compensation plans and arrangements,
and the incentives created by the compensation awards it administers and our Audit Committee oversees management of enterprise risks
and financial risks, as well as potential conflicts of interests. The Board will be responsible for overseeing the management of risks
associated with the independence of our Board.
****
**Compensation
Committee Interlocks and Insider Participation**
None
of our executive officers, except Dr. Trieu, served as a member of the Board or Compensation Committee, or other committee serving an
equivalent function, of any entity that has an executive officer and who serves on our Board or Compensation Committee since 2019. After
the merger of the Company with Oncotelic Inc., our Chief Executive Officer, Dr. Trieu has been identified and is a control person of
Autotelic, Inc.
| 56 | |
Also,
Mr. Steven King, was the CEO of Edgepoint Inc., an AI company that is a non-controlling interest subsidiary of the Company. Dr. Maida
is currently consulting as the Chief Medical Officer Translation Medicine with the Company in regards to its planned trials for
OT-101 for our oncology indications.
**Corporate
Code of Ethics**
We
have adopted a Corporate Code of Conduct and Ethics (the *Code of Conduct*) that applies to all of our employees,
including our CEO and CFO. The text of the Code of Conduct had been filed as an exhibit to our Annual Report on Form 10-K for the year
ended December 31, 2014, and is posted on our website at www.oncotelic.com. Disclosure regarding any amendments to, or waivers
from provisions of the code of conduct and ethics that apply to our directors and principal executive and financial officers will be
included in a Current Report on Form 8-K within four business days following the date of the amendment or waiver.
**Section
16(a) Beneficial Ownership Reporting Compliance**
Section
16(a) of the Exchange Act requires our directors, executive officers and persons who own more than 10% of our common stock to file with
the SEC and us initial reports of beneficial ownership and reports of changes in beneficial ownership of our common stock and other equity
securities. For these purposes, the term other equity securities would include options granted under the Companys
2005 Stock Plan (the *2005 Stock Plan*), the Companys 2015 Equity Incentive Plan (the *2015 Plan*)
and the Companys 2017 Equity Incentive Plan (the *2017 Plan*). To our knowledge, based solely on a review of
the forms and written representations received by us from our Section 16 reporting persons, during the fiscal year ended December 31,
2019, all Section 16(a) filing requirements applicable to the reporting persons were properly and timely satisfied.
**ITEM
11. EXECUTIVE COMPENSATION**
**Summary
Compensation Table**
The
following table provides information regarding the compensation paid during the years ended December 31, 2024, and 2023 to our principal
executive officer, principal financial officer and certain of our other executive officers, who are collectively referred to as named
executive officers elsewhere in this Annual Report.
| 
Name and Principal Position | | 
Year | | | 
Salary $(1) | | | 
Bonus $ | | | 
Stock Awards $(2) | | | 
All Other Compensation $ | | | 
Total $ | | |
| 
Vuong Trieu, Ph. D. | | 
| 2024 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
President and Chief Executive Officer | | 
| 2023 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
| | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Anthony E. Maida III, Ph. D., M.D. MBA | | 
| 2024 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Chief Medical Officer (May 2020) Consultant | | 
| 2023 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
| | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Saran Saund | | 
| 2024 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Chief Business Officer | | 
| 2023 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
| | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Amit Shah | | 
| 2024 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Chief Financial Officer | | 
| 2023 | | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
(1)
Assuming the continuation of the cash compensation and benefits continue to be borne by the JV, the Company will not report such compensation
information as part of the Companys Executive Compensation.
(2)
During the years 2024 and 2023, the Company has not granted any stock awards to any of its executive officers or directors, as the Company
does not have a sufficient pool under the stock option plans to make such awards.
| 57 | |
**Narrative
Disclosure to Summary Compensation Table**
*Vuong
Trieu, Ph. D., Saran Saund and Amit Shah*
Commencing
in August 2019, the Company entered into Employment Agreements and incentive compensation arrangements with each of its executive officers.
The Employment Agreements provide for annual base salaries for each year of the term, subject to review and adjustment by the Board or
the Compensation Committee from time to time. Each Employment Agreement provides that the executive shall be eligible for an annual discretionary
cash bonus expressed as a percentage the executives base salary, subject to their achievement of performance targets and goals
established by the Board or the Compensation Committee. Mr. Saund was appointed as an Executive Officer in November 2019 after the PointR
merger. Dr. Maida was appointed as our consultant Chief Medical Officer Translation Medicine in May 2020 and does not have an
Employment Agreement. Each of the executive officers entered into the Companys standard form of indemnification agreement.
Dr.
Fein was appointed as the Chief Regulatory Officer in May 2022. Further, Dr. Fein was appointed as Chief Medical Officer in February
2023.
The
initial base salaries and discretionary cash bonus amounts had been set for the executives as follows:
| 
Executive | | 
Title | | 
Initial Base Salary | | | 
Discretionary Bonus (% of Base) | | |
| 
Vuong Trieu | | 
Chief Executive Officer | | 
$ | 450,000 | | | 
| 50 | % | |
| 
Amit Shah | | 
Chief Financial Officer | | 
$ | 320,000 | | | 
| 40 | % | |
| 
Saran Saund | | 
Chief Business Officer | | 
$ | 230,000 | | | 
| 40 | % | |
| 
Anthony E. Maida III(1) | | 
Chief Medical Officer | | 
$ | 180,000 | | | 
| NA | | |
| 
| 
(1) | 
Dr.
Maida is a consultant to the Company and currently does not have an Employment Agreement. | |
The
Company did not grant any increases in cash compensation to any of its Executive Officers, other than Mr. Saund whose compensation was
increased to $320,000 in 2023, since the initial employment agreement due to the financial condition of the Company. However, such compensation
was paid to Mr. Saund by the JV and hence not reported above. Further, as disclosed previously, our JV has paid the cash compensation
to our employees, including all the other executive officers named above, since the first quarter of 2023.
The
stock-based compensation on the issuance the stock options has been reported under Summary Compensation Table above, if and when granted.
| 58 | |
****
**Outstanding
Equity Awards at Fiscal Year-End**
The
following table shows all outstanding grants of stock options as of December 31, 2024, to each of the executive officers named in the
Summary Compensation Table. The table below reflects the options and restricted shares that are issuable to Messrs. Trieu, Maida, Saund
and Shah.
| 
| | 
Option Awards | |
| 
Name | | 
Type | | 
Number of Securities Underlying Unexercised Options Exercisable | | | 
Number of Securities Underlying Unexercised Options Exercisable | | | 
Option Exercise Price | | | 
Option Expiration Date | |
| 
Vuong Trieu, Ph. D. (1) | | 
| | 
| | | | 
| | | | 
| | | | 
| |
| 
Chief Executive Officer & President- 2022 | | 
ISO | | 
| 200,000 | | | 
| 800,000 | | | 
$ | 0.10 | | | 
7/22/2032 | |
| 
2021 | | 
ISO | | 
| 360,000 | | | 
| | | | 
$ | 0.1398 | | | 
7/8/2031 | |
| 
2021 | | 
ISO | | 
| 200,000 | | | 
| | | | 
$ | 0.1626 | | | 
9/3/2031 | |
| 
| | 
| | 
| | | | 
| | | | 
| | | | 
| |
| 
Saran Saund (1) | | 
| | 
| | | | 
| | | | 
| | | | 
| |
| 
Chief Business Officer- 2022 | | 
ISO | | 
| 200,000 | | | 
| 800,000 | | | 
$ | 0.10 | | | 
7/22/2032 | |
| 
2021 | | 
ISO | | 
| 675,000 | | | 
| | | | 
$ | 0.1398 | | | 
7/8/2031 | |
| 
2021 | | 
ISO | | 
| 100,000 | | | 
| | | | 
$ | 0.1626 | | | 
9/3/2031 | |
| 
| | 
| | 
| | | | 
| | | | 
| | | | 
| |
| 
Anthony Maida (1) 2022 | | 
| | 
| | | | 
| | | | 
| | | | 
| |
| 
Chief Medical Officer Consultant- 2022 | | 
ISO | | 
| 200,000 | | | 
| 800,000 | | | 
$ | 0.10 | | | 
7/22/2032 | |
| 
2021 | | 
NQSO | | 
| 400,000 | | | 
| | | | 
$ | 0.1398 | | | 
7/8/2031 | |
| 
2021 | | 
NQSO | | 
| 400,000 | | | 
| | | | 
$ | 0.1626 | | | 
9/3/2031 | |
| 
| | 
| | 
| | | | 
| | | | 
| | | | 
| |
| 
Amit Shah (1) | | 
| | 
| | | | 
| | | | 
| | | | 
| |
| 
Chief Financial Officer- 2022 | | 
ISO | | 
| 200,000 | | | 
| 800,000 | | | 
$ | 0.10 | | | 
7/22/2031 | |
| 
2021 | | 
ISO | | 
| 400,000 | | | 
| | | | 
$ | 0.1626 | | | 
7/8/2031 | |
| 
(1) | 
The
stock awards had been approved by the board. The stock compensation thereon has been computed and expensed when granted and reported
in the Summary Compensation Table. | |
**Pension
Benefits**
We
do not have any qualified or non-qualified defined benefit plans.
****
**Nonqualified
Deferred Compensation**
We
do not have any non-qualified defined contribution plans or other deferred compensation plans.
| 59 | |
****
**Potential
Payments Upon Termination or Change-In-Control**
We
have entered into certain agreements and maintain certain plans that may require us to make certain payments and/or provide certain benefits
to Dr. Trieu, Mr. Saund and Mr. Shah in the event of a termination of their employment or a change of control of the Company. The following
table summarizes the potential payments to Dr. Trieu; and Messrs. Saund and Shah assuming that one of the described termination events
occurs. The table assumes that the event occurred on December 31, 2024, the last day of our fiscal year and that each of the named officers
were eligible to earn the full initial base compensation. On the final trading day of our fiscal year the closing price of our common
stock on OTCQB Market was $0.04 per share.
The
Employment Agreements each have a term that continues until terminated by the Company or the executive. In the event that the Company
terminates an executive for Cause, or an executive voluntarily resigns his employment, on termination the executive will
be entitled to receive all accrued and unpaid base salary, any accrued and unused paid time off, and reimbursement of outstanding business
expenses. If the Employment Agreements are terminated by the Company without Cause or the executive resigns for Good
Reason (each as defined in the Employment Agreement) then the executive will be entitled to additional severance benefits including:
(a) a lump sum payment equal to 12 months of the executives then current base salary (18 months in the case of Dr. Trieu);
(b) accelerated vesting of all outstanding stock options and incentive compensation awards, and (c) insurance benefits or COBRA coverage
for 12 months (18 months in the case of Dr. Trieu) in addition to payment of accrued and unpaid personal time.
**Vuong
N. Trieu, Ph. D.**
| 
Executive Benefits and Payments Upon Termination | | 
Termination within 12 months Following Change in Control | | | 
Voluntary Termination by Executive or Death | | | 
Involuntary Not for Cause Termination or Termination by Executive with Good Reason | | | 
For CauseTermination | | | 
Disability | | |
| 
Base Salary | | 
$ | 675,000 | | | 
$ | | | | 
$ | 675,000 | | | 
$ | | | | 
$ | | | |
| 
Annual Bonus (50% of Base Salary) | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| N/A | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | |
| 
Acceleration of Vesting of Equity | | 
| 100 | % | | 
| 0 | % | | 
| 100 | % | | 
| 0 | % | | 
| 0 | % | |
| 
Stock Options: | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Number of Stock Option | | 
| 1,998,255 | | | 
| | | | 
| 1,998,255 | | | 
| | | | 
| | | |
| 
Value upon Termination* | | 
$ | 79,930 | | | 
$ | | | | 
$ | 79,930 | | | 
$ | | | | 
$ | | | |
| 
Vested Stock / Received: | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Number of Shares | | 
| 1,198,255 | | | 
| | | | 
| 1,198,255 | | | 
| | | | 
| | | |
| 
Value upon Termination* | | 
$ | 47,930 | | | 
$ | | | | 
$ | 47,930 | | | 
$ | | | | 
$ | | | |
| 
Relocation Reimbursement | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 
Deferred Compensation Payout | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 
Post-Term Health Care | | 
| Up to 18 months | | | 
| N/A | | | 
| Up to 18 months | | | 
| N/A | | | 
| N/A | | |
| 
| | 
$ | 18,964 | | | 
$ | | | | 
$ | 18,964 | | | 
$ | | | | 
$ | | | |
| 
Excise Tax Gross Up | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 60 | |
**Saran
Saund**
| 
Executive Benefits and Payments Upon Termination | | 
Termination within 12 months Following Change in Control | | | 
Voluntary Termination by Executive or Death | | | 
Involuntary Not for Cause Termination or Termination by Executive with Good Reason | | | 
For CauseTermination | | | 
Disability | | |
| 
Base Salary | | 
$ | 320,000 | | | 
$ | | | | 
$ | 320,000 | | | 
$ | | | | 
$ | | | |
| 
Annual Bonus (40% of Base Salary) | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| N/A | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | |
| 
Acceleration of Vesting of Equity | | 
| 100 | % | | 
| 0 | % | | 
| 100 | % | | 
| 0 | % | | 
| 0 | % | |
| 
Stock Options: | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Number of Stock Options (1) | | 
| 1,993,798 | | | 
| | | | 
| 1,993,798 | | | 
| | | | 
| | | |
| 
Value upon Termination* | | 
$ | 79,752 | | | 
$ | | | | 
$ | 79,752 | | | 
$ | | | | 
$ | | | |
| 
Vested Stock Received: | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Number of Shares (1) | | 
| 1,193,798 | | | 
| | | | 
| 1,193,798 | | | 
| | | | 
| | | |
| 
Value upon Termination* | | 
$ | 49,752 | | | 
$ | | | | 
$ | 49,752 | | | 
$ | | | | 
$ | | | |
| 
Relocation Reimbursement | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 
Deferred Compensation Payout | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 
Post-Term Health Care | | 
| Up to 12 months | | | 
| N/A | | | 
| Up to 12 months | | | 
| N/A | | | 
| N/A | | |
| 
| | 
$ | 5,671 | | | 
$ | | | | 
$ | 5,671 | | | 
$ | | | | 
$ | | | |
| 
Excise Tax Gross Up | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 61 | |
****
**Amit
Shah**
| 
Executive Benefits and Payments Upon Termination | | 
Termination within 12 months Following Change in Control | | | 
Voluntary Termination by Executive or Death | | | 
Involuntary Not for Cause Termination or Termination by Executive with Good Reason | | | 
For CauseTermination | | | 
Disability | | |
| 
Base Salary | | 
$ | 320,000 | | | 
$ | | | | 
$ | 320,000 | | | 
$ | | | | 
$ | | | |
| 
Annual Bonus (50% of Base Salary) | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | | 
| N/A | | | 
| Executive entitled to Annual Bonus related to most recently completed calendar year if earned and not already paid | | |
| 
Acceleration of Vesting of Equity | | 
| 100 | % | | 
| 0 | % | | 
| 100 | % | | 
| 0 | % | | 
| 0 | % | |
| 
Stock Options: | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Number of Stock Options (1) | | 
| 1,997,093 | | | 
| | | | 
| 1,997,093 | | | 
| | | | 
| | | |
| 
Value upon Termination* | | 
$ | 79,884 | | | 
$ | | | | 
$ | 79,884 | | | 
$ | | | | 
$ | | | |
| 
Vested Stock Received: | | 
| | | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Number of Shares (1) | | 
| 1,197,093 | | | 
| | | | 
| 1,197,093 | | | 
| | | | 
| | | |
| 
Value upon Termination* | | 
$ | 47,884 | | | 
$ | | | | 
$ | 47,884 | | | 
$ | | | | 
$ | | | |
| 
Relocation Reimbursement | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 
Deferred Compensation Payout | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
| 
Post-Term Health Care | | 
| Up to 12 months | | | 
| N/A | | | 
| Up to 12 months | | | 
| N/A | | | 
| N/A | | |
| 
| | 
$ | 11,208 | | | 
$ | | | | 
$ | 11,208 | | | 
$ | | | | 
$ | | | |
| 
Excise Tax Gross Up | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | | 
| N/A | | |
*Based
on the stock price of the Company as of December 31, 2024, of $0.04 and assuming the number of shares granted are vested and earned.
Assuming that the JV would be responsible for the cash compensation and the health benefits that any of the executive officers named
above, that cost may not be paid for by the Company Dr. Maida is a consultant Chief Medical Officer Translation Medicine and
is not subject to potential payments upon termination or change-in-control, and as such his information has not been compiled for this
table.
The
information set forth above is described in more detail in the Narrative Disclosure to the Summary Compensation Table.
As
defined in the employment agreements, a Change in Control means the following during the employment term:
| 
(1) | 
any
Person (as such term is used in Sections 13(d) and 14(d) of the Exchange Act) becomes the Beneficial Owner
(as defined in Rule 13d-3 under said Act), directly or indirectly, of securities of the Company representing more than fifty percent
of the total voting power represented by the Companys then outstanding voting securities (excluding for this purpose any such
voting securities held by the Company or its affiliates or by any employee benefit plan of the Company) pursuant to a transaction
or a series of related transactions which the Board of Directors does not approve; or | |
| 62 | |
| 
(2) | 
a
merger or consolidation of the Company whether or not approved by the Board of Directors, other than a merger or consolidation which
would result in the voting securities of the Company outstanding immediately prior thereto continuing to represent (either by remaining
outstanding or by being converted into voting securities of the surviving entity or the parent of such corporation) at least fifty
percent of the total voting power represented by the voting securities of the Company or such surviving entity or parent of such
corporation, as the case may be, outstanding immediately after such merger or consolidation; or | |
| 
| 
| |
| 
(3) | 
the
stockholders of the Company approve an agreement for the sale or disposition by the Company of all or substantially all of its assets;
or | |
| 
| 
| |
| 
(4) | 
a
change in the composition of the Board of Directors, as a result of which fewer than a majority of the directors are Incumbent Directors,
and provided in each such case the Change in Control also meets the requirements of a Change in Control Event within
the meaning of Section 409A(a)(2)(A)(v) of the Code and Treasury Regulation Section 1.409A-3(i)(5). Incumbent Directors
mean the directors who either (A) are directors of the Company as of the date of this Agreement, or (B) are elected, or nominated
for election, to the Board of Directors with the affirmative votes of at least a majority of the Incumbent Directors at the time
of such election or nomination (but shall not include an individual whose election or nomination is in connection with an actual
or threatened proxy
contest
relating to the election of directors to the Company). | |
In
each such case the Change of Control must also meet the requirements of a Change of Control Event within the meaning of
Section 409(a)(2)(A)(v) of the Code.
Each
of Drs. Trieu, Saund and Mr. Shah will be entitled to certain benefits as described in the table above if his employment is terminated
by the Company for reasons other than cause or by him with good reason. Cause, as defined in the employment agreements,
means:
| 
(1) | 
Substantial
failure to perform any of his duties or to follow reasonable, lawful directions of the Board or any officer to whom the party reports; | |
| 
| 
| |
| 
(2) | 
willful
misconduct or willful malfeasance in connection with his employment; | |
| 
| 
| |
| 
(3) | 
commission
of, conviction of, or plea of nolo contendere to, any crime constituting a felony under the laws of the United States or any state
thereof, or any other crime involving moral turpitude; | |
| 
| 
| |
| 
(4) | 
material
breach of any provision of the employment agreement, the By-laws or any other written agreement with the Company; | |
| 
| 
| |
| 
(5) | 
engaging
in misconduct that causes significant injury to the Company, financial or otherwise, or to its reputation; or | |
| 
| 
| |
| 
(6) | 
any
act, omission or circumstance constituting cause under the law governing the employment agreement. | |
Good
Reason, as defined in the employment agreements, means the Company:
| 
(1) | 
materially
reduces the officers title or responsibilities; | |
| 
| 
| |
| 
(2) | 
relocates
its headquarters more than sixty (60) miles from their current location (unless the relocation results in the headquarters being
closer to the officers residence); | |
| 
| 
| |
| 
(3) | 
materially
reduces the officers base salary; or | |
| 
| 
| |
| 
(4) | 
breaches
a material term of the officers employment agreement. | |
Good
Reason must also meet the requirements for a good reason termination in accordance with Code Section 409A, and any successor statute,
regulation and guidance thereto.
| 63 | |
**Director
Compensation**
For
the year ended December 31, 2024, and 2023, none of the non-employee directors were paid in cash or stock awards
| 
| | 
Fees Earned or Paid in | | |
| 
| | 
Cash(1) | | | 
Option Awards(2) | | | 
Total | | |
| 
| | 
| | | 
| | | 
| | |
| 
Steven King 2021/22 | | 
$ | - | | | 
$ | - | | | 
$ | - | | |
We
granted Mr. King 500,000 options for his services through the end of fiscal year 2022. Although the initial terms of the options, when
granted, provide that they vest one year subsequent to grant, pursuant to rules of the SEC the fair market value for the options granted
represents the full value at the grant date only and the values do not take into account subsequent increases or decreases in actual
value to the recipient. See also our discussion of stock- based compensation under Managements Discussion and Analysis
of Financial Condition and Results of OperationsCritical Accounting Policies and Significant Judgments and Estimates in
the Form 10-K.
The
following is a description of the standard compensation arrangements under which our non-employee directors have been compensated for
their service as directors, including as members of the various Committees of our Board.
*Fees*.
In October 2016, the Board amended and restated its director compensation policy. For more details on the Fees, kindly refer to our 2020
Annual Report on 10-K for filed with the SEC on April 15, 2021. However, due to the financial condition of the Company, we have discontinued
cash compensations for the independent Board Members or Committee members. The Board intends to re-evaluate compensation, including non-employee
director compensation, following the reconstitution of its Compensation Committee.
*Equity
Grants*.
In
October 2016, the Board amended and restated its director compensation policy.
The
Board intends to re-evaluate compensation, including non-employee director compensation, following the reconstitution of its Compensation
Committee. For more information on our prior policy, please refer to our 2021 Annual Report on Form 10-K filed with the SEC on April
15, 2022.
**ITEM
12. SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT AND RELATED STOCKHOLDER MATTERS**
**Security
Ownership of Certain Beneficial Owners and Management**
The
following table sets forth information, as of April 12, 2025, regarding the beneficial ownership of our common stock by:
| 
| 
| 
each
of our directors and our director nominees; | |
| 
| 
| 
each
of our executive officers; | |
| 
| 
| 
our
directors and executive officers as a group; and | |
| 
| 
| 
each
person known to us to beneficially own more than 5% of our common stock. | |
The
address for each beneficial owner listed is c/o Oncotelic Therapeutics, Inc. 29397 Agoura Road, Suite 107, Agoura Hills, California,
91301. Each of the stockholders listed has sole voting and investment power with respect to the shares beneficially owned by the stockholder,
subject to community property laws where applicable.
| 64 | |
In
accordance with applicable SEC rules, the number of shares reflected as beneficially owned by each entity, person, director or executive
officer is determined in accordance with the rules of the SEC. Under those rules, beneficial ownership includes any shares over which
the individual has sole or shared voting power or investment power as well as any shares that the individual has the right to acquire
within 60 days after the Record Date through the exercise of any stock option, warrants or other rights.
We
have computed the percentage of shares beneficially owned on the basis of 408,292,450 shares of our Common Stock outstanding as of April
12, 2025. Shares of our Common Stock that a person has the right to acquire within 60 days after the Record Date through other means,
such as a stock option or warrant, are deemed outstanding for purposes of computing the percentage ownership of the person holding such
rights, but are not deemed outstanding for purposes of computing the percentage ownership of any other person (other than the percentage
ownership of all directors and executive officers as a group).
| 
Name of Beneficial Owner | | 
Common Stock Beneficially Owned | | | 
Percentage of Common Stock | | |
| 
Directors and Officers: | | 
| | | | 
| | | |
| 
Vuong Trieu | | 
| 132,244,387 | (1) | | 
| 32.4 | % | |
| 
Steven W. King | | 
| 4,188,059 | (2) | | 
| 1.0 | % | |
| 
Anthony E. Maida III | | 
| 3,137,314 | (3) | | 
| 0.8 | % | |
| 
Amit Shah | | 
| 2,584,871 | (4) | | 
| 0.6 | % | |
| 
Saran Saund | | 
| 18,347,759 | (5) | | 
| 4.5 | % | |
| 
Seymour Fein, MD | | 
| - | | | 
| 0.0 | % | |
| 
All officers and directors as a group (6 persons) | | 
| 160,502,390 | (6) | | 
| 39.3 | % | |
| 
| | 
| | | | 
| | | |
| 
Beneficial owners of more than 5% | | 
| | | | 
| | | |
| 
Vuong Trieu | | 
| 132,244,387 | (1) | | 
| 32.5 | % | |
| 
Balaji Bhakta | | 
| 43,575,256 | (7) | | 
| 10.7 | % | |
| 
Larn Hwang | | 
| 25,714,323 | (8) | | 
| 6.3 | % | |
| 
Chao Hsiao | | 
| 22,406,942 | (9) | | 
| 5.5 | % | |
*
< 1%
| 
(1) | 
Includes:
(a) 92,544,217 shares owned directly and beneficially by the reporting person; 11,669,415 shares of common shares issuable upon conversion
of debt, 1,738,953 shares issuable upon exercise of stock options and 1,250,000 shares of common shares issuable upon exercise of
warrants; (b) 16,780,384 shares registered in the name of Autotelic, Inc., and 1,388,889 shares issuable upon conversion of debt,
and (c) 6,872,529 shares registered in the name of Dr. Trieus spouse. Dr. Trieu is the Chief Executive Officer of Autotelic,
Inc. and in that capacity has the sole authority to control the voting and the disposition of Common Stock and Preferred Stock owned
by Autotelic, Inc. Dr. Trieu disclaims beneficial ownership of the shares held by Autotelic, Inc., except to the extent of his beneficial
interest therein. | |
| 
| 
| |
| 
(2) | 
Shares
held in the name of Artius Bioconsulting, LLC, consists of (i) 3,330,647 shares of Common Stock and (ii) 857,412 shares issuable
upon exercise of stock options granted to Mr. King. | |
| 
| 
| |
| 
(3) | 
Consists
of (i) 1,137,314 shares of Common Stock and (ii) 2,000,000 shares issuable upon exercise of stock options. | |
| 
| 
| |
| 
(4) | 
Consists
of (i) 358,837 shares of Common Stock, (ii) 527,778 shares of common stock issuable upon conversion of debt and (iii) 1,698,256 shares
of common stock upon exercise of options. | |
| 
| 
| |
| 
(5) | 
Consists
of (i) 16,456,480 shares of Common Stock, and (ii) 1,891,279 shares issuable upon exercise of stock options. | |
| 65 | |
| 
(6) | 
Consists of (i) 136,980,409 shares of Common Stock, (ii) 5,838,885 shares issuable upon conversion of debt, (iii) 8,185,900 shares issuable upon exercise of options and (iv) 1,250,000 shares issuable upon exercise of warrants. | |
| 
| 
| |
| 
(7) | 
Consists of (i) 41,630,811 shares of Common Stock, (ii) (iii) 694,445 shares of common stock upon conversion of debt and 1,250,000 upon conversion of warrants. | |
| 
| 
| |
| 
(8) | 
Consists of (i) 23,455,990 shares of Common Stock, (ii) 1,208,333 shares of common stock issuable upon conversion of debt and (iii) 1,050,000 shares of common stock upon exercise of options. | |
| 
| 
| |
| 
(9) | 
Consists of (i) 17,073,604 shares of Common Stock, (ii) 3,744,449 shares of common stock issuable upon conversion of debt, (iii) 1,200,000 shares of common stock upon exercise of options, and (iv) 388,889 shares issuable upon exercise of PPM debt and warrants. | |
****
**Equity Compensation Plan Information**
****
The following table provides certain
aggregate information with respect to all of the Companys equity compensation plans in effect as of December 31, 2024.
| 
Plan Category | | 
Number of Securities to be Issued Upon Exercise of Outstanding Options, Warrants and Rights | | | 
Weighted- Average Exercise Price of Outstanding Options | | | 
Number of Securities Remaining Available for Future Issuance Under Equity Compensation Plans (Excluding Securities Reflected in Column (a)) | | |
| 
Equity compensation plans approved by security holders | | 
| 22,527,761 | | | 
$ | 0.22 | | | 
| 3,205,021 | | |
| 
Equity compensation plans not approved by security holders | | 
| 1,650,000 | | | 
| 0.30 | | | 
| 350,000 | | |
| 
| | 
| | | | 
| | | | 
| | | |
| 
Total | | 
| 24,177,761 | | | 
$ | 0.23 | | | 
| 3,555,021 | | |
In August 2020, the shareholders
of the Company approved the expansion of the number of securities to be issued upon exercise of outstanding options, warrants, restricted
stock units and warrants by 20 million. The amendment to the 2015 Plan was completed in March 2021 and as such the pool under the 2015
Plan is now 27,250,000.
**Brief Description of equity compensation plan not approved by security
holders**
****
In January 2017, the Board of
Directors adopted and approved the 2017 Plan. The 2017 Plan allows the Company, under the direction of the Compensation Committee, to
make grants of stock options, restricted and unrestricted stock awards, and other stock-based awards to employees, consultants and directors.
The purpose of these awards is to attract and retain key individuals, further align employee and stockholder interests, and provide additional
incentive for them to promote our success. The 2017 Plan provides for the issuance of up to 2,000,000 shares of the Companys common
stock. Any stock options granted under the 2017 Plan must be non-qualified stock options, which are not intended to meet the requirements
of Section 422 of the Internal Revenue code. Options generally vest over a period of time, may not be exercised unless they are vested,
and no option may be exercised after the end of the term set forth in the award agreement.
| 66 | |
**ITEM 13. CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS
AND DIRECTOR INDEPENDENCE**
Our Audit Committee reviews and
approves in advance all related person transactions.
Our Board of Directors has reviewed
the materiality of any relationship that each of our directors has with the Company, either directly or indirectly. Based upon this review,
our Board has determined that none of the directors, qualify as independent directors as defined under the OTC Market Rules
for U.S. Companies.
*Master Service Agreement with Autotelic Inc.*
**
In October 2015, Oncotelic Inc.
entered into a Master Service Agreement (the *MSA*) with Autotelic Inc. (*Autotelic*), a related
party that is partly owned by Dr. Trieu. Dr. Trieu, a related party, is a control person in Autotelic. Autotelic currently owns less than
10% of the Company. The MSA stated that Autotelic will provide business functions and services to the Company and allowed Autotelic to
charge the Company for these expenses paid on its behalf. The MSA includes personnel costs allocated based on amount of time incurred
and other services such as consultant fees, clinical studies, conferences and other operating expenses incurred on behalf of the Company.
The MSA requires a 90-day written termination notice in the event either party requires to terminate such services.
Expenses related to the MSA were
$2,000 and approximately $12,000 for the years ended December 31, 2024 and 2023, respectively. The Company owed Autotelic, Inc. approximately
$0.3 million at December 31, 2024 and December 31, 2023 respectively.
*License Agreement with Autotelic Inc.*
**
In September 2021, the Company
entered into an exclusive License Agreement with Autotelic. For more information on the exclusive license Agreement with Autotelic, refer
to our 2023 Annual Report on Form 10-K filed with SEC on April 12, 2024.
*Notes Payable and Short-Term Loan Related Party*
**
In April 2019, the Company issued
a convertible note to Dr. Trieu totaling $164,444, including OID of $16,444, receiving net proceeds of $148,000, which was used by the
Company for working capital and general corporate purposes. The Company issued a Fall 2019 Note to Dr. Trieu in the principal amount of
$250,000. Dr. Trieu also offset certain amounts due to him in the amount of $35,000 and was converted into the Fall 2019 debt. During
the year ended December 31, 2020, Dr. Trieu purchased a total of 5 Units under the private placement for a gross total of $250,000. During
the year ended December 31, 2023, Dr Trieu provided short term loan of $50 thousand to the Company.
In May 2021, Autotelic provided
an additional short-term funding of $250,000 to the Company, which was converted into the August 2021 Notes. Autotelic provided an additional
$120,000 short-term loan to the Company during the year ended December 31, 2022. During the year ended December 31, 2023, Autotelic provided
$1.4 million in short term advances to the Company. During the year ended December 31, 2024, Autotelic provided an additional $0.7 million.
As such, approximately $2.1 million was outstanding and payable to Autotelic at December 31, 2024.
*Artius Consulting Agreement*
**
On March 9, 2020, the Company
and Artius Bioconsulting, LLC (*Artius*), for which Mr. King is the Managing Member, entered into an amendment to the
Consulting Agreement dated December 1, 2018, under which Artius agreed to serve as a consultant to the Company for services related to
the Companys business from time to time, effective December 1, 2019 (the *Effective Date*) (the *Artius
Agreement*). For more information on this Agreement, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April
12, 2024.
No expense was recorded during
the year ended December 31, 2024, or 2023, respectively, related to this Agreement.
*Mosaic Consulting Agreement*
**
In July 2024, the Company and
Mosaic, for which Mr. King is the Chief Executive Officer, entered into an consulting agreement (*Mosaic Agreement*),
under which Mosaic agreed to serve as a consultant to the Company for services related to the JVs chemistry, manufacturing and
controls for the San Diego site on a month to month basis at a rate of $7,000 per month. This cost was entirely borne by the JV.
No expense was recorded during
the year ended December 31, 2024, related to the Mosaic Agreement.
| 67 | |
*Maida Consulting Agreement*
**
Effective May 5, 2020, the Company
and Dr. Maida entered into an independent consulting agreement, commencing April 1, 2020 (the Maida Agreement), under which
Dr. Maida will assist the Company in providing medical expertise and advice from time to time in the design, conduct and oversight of
the Companys existing and future clinical trials. For more information on this Agreement, refer to our 2021 Annual Report on Form
10-K filed with the SEC on April 15, 2022.
The Company recorded an expense
of $0 during the years ended December 31, 2024 and 2023, respectively, related to this Agreement. Effective April 1, 2022, Dr Maidas
compensation is being borne by the JVA with GMP Bio.
**ITEM 14. PRINCIPAL ACCOUNTING FEES AND SERVICES**
The following table presents fees
for professional audit services rendered by our independent public accounting firm, Rose Snyder and Jacobs, LLP (*RSJ*)
for the audit for the years ended December 31, 2024 and December 31, 2023, respectively, and other services rendered during that period.
| 
| 
| 
2024 | 
| 
| 
2023 | 
| |
| 
Audit fees (1) | 
| 
$ | 
99,000 | 
| 
| 
$ | 
104,600 | 
| |
| 
Audit-related fees | 
| 
| 
| 
| 
| 
| 
| 
| |
| 
Tax fees | 
| 
| 
| 
| 
| 
| 
| 
| |
| 
All other fees | 
| 
| 
| 
| 
| 
| 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
| 
| 
$ | 
99,000 | 
| 
| 
$ | 
104,600 | 
| |
| 
(1) | 
Audit fees consisted of audit work performed on the
audit of the annual financial statements, review of quarterly financial statements, as well as work that generally only the independent
registered public accounting firm can reasonably be expected to provide, such as the provision of consents in connection with the filing
of registration statements and statutory audits.
We have been invoiced $99,000 by RSJ in connection with the reviews for
the quarters ended March 31, 2024, June 30, 2024 and September 30, 2024; and for the year ended December 31, 2024.
We had been invoiced $104,600 by RSJ in connection
with the reviews for the quarters ended March 31, 2023, June 30, 2023 and September 30, 2023; and for the year ended December 31, 2023. | |
**Policy on Audit Committee Pre-Approval of Audit
and Permissible**
****
**Non-audit Services of Independent Registered Public
Accounting Firm**
****
Consistent with SEC policies regarding
auditor independence, the Audit Committee has responsibility for appointing, setting compensation, and overseeing the work of the independent
registered public accounting firm. In recognition of this responsibility, the Audit Committee has established a policy to pre-approve
all audit and permissible non-audit services provided by the independent registered public accounting firm.
Prior to engagement of the independent
registered public accounting firm for the next years audit, management will submit an aggregate of services expected to be rendered
during that year for each of four categories of services to the Audit Committee for approval.
| 
1. | 
Audit services include audit work performed in the preparation and audit of the annual financial statements, review of quarterly financial statements, as well as work that generally only the independent auditor can reasonably be expected to provide, such as the provision of consents and comfort letters in connection with the filing of registration statements. | |
| 
| 
| |
| 
2. | 
Audit-related services are for assurance and related services that are traditionally performed by the independent auditor, including due diligence related to mergers and acquisitions, employee benefit plan audits, and special procedures required to meet certain regulatory requirements. | |
| 
| 
| |
| 
3. | 
Tax services consist principally of assistance with tax compliance and reporting, as well as certain tax planning consultations. | |
| 
| 
| |
| 
4. | 
Other Fees are those associated with services not captured in the other categories. The Company generally does not request such services from the independent auditor. | |
| 68 | |
Prior to engagement, the Audit
Committee pre-approves these services by category of service. The fees are budgeted, and the Audit Committee requires the independent
registered public accounting firm and management to report actual fees versus the budget periodically throughout the year by category
of service. During the year, circumstances may arise when it may become necessary to engage the independent registered public accounting
firm for additional services not contemplated in the original pre-approval. In those instances, the Audit Committee requires specific
pre-approval before engaging the independent registered public accounting firm.
The Audit Committee may delegate
pre-approval authority to one or more of its members. The member to whom such authority is delegated must report, for informational purposes
only, any pre-approval decisions to the Audit Committee at its next scheduled meeting.
In the absence of an Audit Committee,
the responsibilities of the Audit Committee are fulfilled by the Board of Directors of the Company. As such, for the year ended December
31, 2023, the Board of Directors approved the appointment and services of RSJ.
**PART IV**
****
**ITEM 15. EXHIBITS AND FINANCIAL STATEMENT SCHEDULES**
****
| 
(a) | 
The following documents are filed as part of this Annual Report on Form 10-K. | |
****
| 
| 
(1) | 
Financial Statements | |
****
See financial statements listed
in the accompanying Index to Financial Statements covered by the Report of Independent Registered Public Accounting Firm.
| 
| 
(2) | 
Financial Statement Schedule | |
No schedules are submitted because
they are not applicable, not required or because the information is included in the Financial Statements as Notes to Financial Statements.
| 
| 
(3) | 
Exhibits | |
The exhibits below may not be
a complete list of exhibits as the relevance of the exhibits may have made them redundant over a period of time.
| 
| 
| 
| 
| 
Incorporated by Reference | 
| |
| 
Exhibit Number | 
| 
Description | 
| 
Form | 
| 
Filing Date | 
| 
Exhibit Number | 
| 
Filed Herewith | |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
2.1 | 
| 
Agreement and Plan of Merger, dated as of April 17, 2019, by and among the Company, Oncotelic and Oncotelic Acquisition Corporation. | 
| 
8-K | 
| 
4/18/2019 | 
| 
2.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
2.2 | 
| 
Agreement and Plan of Merger, dated as of April 17, 2019, by and among the Company, Oncotelic and Oncotelic Acquisition Corporation. | 
| 
8-K | 
| 
4/25/2019 | 
| 
2.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
2.3 | 
| 
Agreement and Plan of Merger, dated as of August 17, 2019, by and among the Company, PointR and Paris Acquisition Corporation. | 
| 
8-K | 
| 
8/21/2019 | 
| 
2.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
2.4 | 
| 
Agreement and Plan of Merger, dated as of August 17, 2019, by and among the Company, PointR Data, Inc. and Paris Acquisition Corp. | 
| 
8-K | 
| 
11/12/2019 | 
| 
2.1 | 
| 
| |
| 69 | |
| 
2.5 | 
| 
Amendment No. 1 to Agreement and Plan of Merger, dated as of November 1, 2019, by and among the Company, PointR Data, Inc. and Paris Acquisition Corp. | 
| 
8-K | 
| 
11/12/2019 | 
| 
2.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
3.1 | 
| 
Amended and Restated By-Laws of the Registrant. | 
| 
8-K | 
| 
6/17/2016 | 
| 
3.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
3.2 | 
| 
Restated Certificate of Incorporation of the Registrant, as amended by Certificates of Amendment dated June 22, 1995, November 15, 1996, July 14, 2005, June 2, 2009, February 8, 2010, August 5, 2010, February 22, 2011, May 29, 2012, December 27, 2012, July 17, 2013, June 16, 2016 and June 20, 2018. | 
| 
10-Q | 
| 
8/14/2018 | 
| 
3.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
3.3 | 
| 
Certificate of Designation of Preferences, Rights and Limitations of Series A Convertible Preferred Stock of the Company. | 
| 
8-K | 
| 
4/25/2019 | 
| 
3.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
3.4 | 
| 
Certificate of Designation of Preferences, Rights and Limitations of Series A Convertible Preferred Stock of the Company. | 
| 
8-K | 
| 
11/12/2019 | 
| 
3.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.1 | 
| 
Form of Series A/B Common Stock Purchase Warrant. | 
| 
8-K | 
| 
4/11/2013 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.2 | 
| 
Form of Common Stock Purchase Warrant. | 
| 
8-K | 
| 
9/20/2013 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.3 | 
| 
Form of Common Stock Purchase Warrant. | 
| 
S-1/A | 
| 
1/31/2014 | 
| 
4.9 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.4 | 
| 
Form of Placement Agent Purchase Warrant. | 
| 
S-1/A | 
| 
1/31/2014 | 
| 
4.8 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.5 | 
| 
Form of Common Stock Purchase Warrant. | 
| 
8-K | 
| 
2/14/2014 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.6 | 
| 
Form of Placement Agent Purchase Warrant. | 
| 
8-K | 
| 
2/14/2014 | 
| 
4.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.7 | 
| 
Form of Common Stock Purchase Warrant. | 
| 
8-K | 
| 
5/23/2014 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.8 | 
| 
Form of Common Stock Purchase Warrant. | 
| 
8-K | 
| 
3/20/2015 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.9 | 
| 
Specimen Common Stock Certificate. * | 
| 
10-Q | 
| 
8/2/2016 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.10 | 
| 
Form of Series A Warrant to purchase Common Stock. | 
| 
8-K | 
| 
4/16/2018 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.11 | 
| 
Form of Series B Warrant to purchase Common Stock | 
| 
8-K | 
| 
4/16/2018 | 
| 
4.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.12 | 
| 
Form of Placement Agent Purchase Warrant. | 
| 
S-1 | 
| 
6/13/2018 | 
| 
4.12 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.13 | 
| 
Form of Debenture, issued by the Company to PeakOne. | 
| 
8-K | 
| 
4/18/2019 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.14 | 
| 
Form of Debenture, issued by the Company to the Bridge Investors. | 
| 
8-K | 
| 
4/18/2019 | 
| 
4.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.15 | 
| 
Form of Debenture, issued by the Company to Peak One Opportunity Fund, L.P. and TFK Investments, LLC Ex. 4.1 Form of Debenture, issued by the Company to the Bridge Investors. | 
| 
8-K | 
| 
4/25/2019 | 
| 
4.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.16 | 
| 
Form of Debenture, issued by the Company to Peak One Opportunity Fund, L.P. and TFK Investments, LLC. | 
| 
8-K | 
| 
6/20/2019 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
4.17 | 
| 
Convertible Promissory Note between Mateon Therapeutics, Inc. and PointR Data Inc. dated July 22, 2019. | 
| 
8-K | 
| 
7/24/2019 | 
| 
4.1 | 
| 
| |
| 70 | |
| 
4.18 | 
| 
Form of Note Purchase Agreement, dated as of November 23, 2019, by and among the Company and the investors identified therein. | 
| 
8-K | 
| 
11/25/2019 | 
| 
4.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.1 | 
| 
Technology Development Agreement, dated as of May 27, 1997, between the Registrant and the Arizona Board of Regents, acting for and on behalf of Arizona State University. | 
| 
10-K | 
| 
4/15/1998 | 
| 
10.9 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.2 | 
| 
Research Collaboration and License Agreement, dated as of December 15, 1999, between OXiGENE Europe AB and Bristol-Myers Squibb Company. * | 
| 
8-K | 
| 
12/28/1999 | 
| 
99.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.3 | 
| 
Amendment and Confirmation of License Agreement No. 206-01.LIC, dated as of June 10, 2002, between the Registrant and the Arizona Board of Regents, acting for and on behalf of Arizona State University. | 
| 
10-Q | 
| 
8/14/2002 | 
| 
10.29 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.4 | 
| 
Termination Agreement by and between OXiGENE Europe AB and Bristol-Myers Squibb Company dated as of February 15, 2002. | 
| 
10-Q | 
| 
8/14/2002 | 
| 
10.14 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.5 | 
| 
License Agreement No. 206-01.LIC by and between the Arizona Board of Regents, acting on behalf of and for Arizona State University, and OXiGENE Europe AB, dated August 2, 1999. | 
| 
10-K/A | 
| 
8/12/2003 | 
| 
10.27 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.6 | 
| 
Research and License Agreement between the Registrant and Baylor University, dated June 1, 1999. | 
| 
10-K/A | 
| 
8/12/2003 | 
| 
10.28 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.7 | 
| 
Agreement to Amend Research and License Agreement between the Registrant and Baylor University, dated April 23, 2002. | 
| 
10-K/A | 
| 
8/12/2003 | 
| 
10.29 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.8 | 
| 
Addendum to Research and License Agreement between the Registrant and Baylor University, dated April 14, 2003. | 
| 
10-K/A | 
| 
8/12/2003 | 
| 
10.30 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.9 | 
| 
Form of Incentive Stock Option Agreement under Mateons 2005 Stock Plan. + | 
| 
10-K | 
| 
3/14/2006 | 
| 
10.29 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.10 | 
| 
Form of Non-Qualified Stock Option Agreement under Mateons 2005 Stock Plan. + | 
| 
10-K | 
| 
3/14/2006 | 
| 
10.30 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.11 | 
| 
Form of Restricted Stock Agreement under Mateons 2005 Stock Plan. + | 
| 
10-K | 
| 
3/14/2006 | 
| 
10.31 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.12 | 
| 
Lease between Broadway 701 Gateway Fee LLC, a Delaware Limited Liability Company, as Landlord, and the Registrant, as Tenant, dated October 10, 2008. | 
| 
10-K | 
| 
3/30/2009 | 
| 
10.59 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.13 | 
| 
Form of Indemnification Agreement. + | 
| 
10-Q | 
| 
8/13/2012 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.14 | 
| 
Third Amendment to Lease, dated as of April 1, 2013, by and between the Registrant and DWF III Gateway, LLC, a Delaware limited liability company. | 
| 
10-Q | 
| 
5/9/2013 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.15 | 
| 
Fourth Amendment to Lease, dated April 28, 2014, by and between the Registrant and DWF III Gateway, LLC. | 
| 
10-Q | 
| 
5/8/2014 | 
| 
10.1 | 
| 
| |
| 71 | |
| 
10.16 | 
| 
Employment Agreement by and between the Registrant and William D. Schwieterman, dated as of May 12, 2015. + | 
| 
10-Q | 
| 
8/6/2015 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.17 | 
| 
Employment Agreement by and between the Registrant and Matthew M. Loar, dated as of July 20, 2015. + | 
| 
10-Q | 
| 
8/6/2015 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.18 | 
| 
Form of Option Agreement under Mateons 2015 Equity Incentive Plan. + | 
| 
10-Q | 
| 
8/6/2015 | 
| 
10.6 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.19 | 
| 
Amendment No. 1 to Employment Agreement by and between William D. Schwieterman, dated as of July 31, 2015. + | 
| 
10-Q | 
| 
8/6/2015 | 
| 
10.7 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.20 | 
| 
Second Amended and Restated Employment Agreement by and between the Registrant and David J. Chaplin, effective as of January 1, 2017. + | 
| 
8-K | 
| 
10/28/2016 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.21 | 
| 
Mateon Therapeutics, Inc. Amended and Restated Non-Employee Director Compensation Policy, effective October 25, 2016. + | 
| 
8-K | 
| 
10/28/2016 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.22 | 
| 
Mateon Therapeutics, Inc. 2017 Equity Incentive Plan. + | 
| 
8-K | 
| 
1/13/2017 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.23 | 
| 
Form of Option Agreement under Mateons 2017 Equity Incentive Plan. + | 
| 
8-K | 
| 
1/13/2017 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.24 | 
| 
Mateon Therapeutics, Inc. 2005 Stock Plan (as amended and restated on January 12, 2017). + | 
| 
8-K | 
| 
1/13/2017 | 
| 
10.3 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.25 | 
| 
Amendment No. 2 to Employment Agreement by and between the Registrant and William D. Schwieterman, dated as of October 2, 2017. + | 
| 
10-Q | 
| 
11/14/2017 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.26 | 
| 
Amendment No. 1 to Employment Agreement by and between the Registrant and Matthew M. Loar, dated as of October 2, 2017. + | 
| 
10-Q | 
| 
11/14/2017 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.27 | 
| 
Amendment No. 1 to Second Amended and Restated Employment Agreement by and between the Registrant and David J. Chaplin, dated as of October 2, 2017. + | 
| 
10-Q | 
| 
11/14/2017 | 
| 
10.3 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.28 | 
| 
Mateon Therapeutics, Inc. 2015 Equity Incentive Plan (as amended and restated on May 7, 2018). + | 
| 
Definitive Proxy Statement on Schedule 14A | 
| 
05/07/2018 | 
| 
Appendix A | 
| 
| |
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| |
| 
10.29 | 
| 
Form of Subscription Agreement for private placement transaction entered into on April 12, 2018. | 
| 
8-K | 
| 
4/16/2018 | 
| 
10.1 | 
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| |
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| |
| 
10.30 | 
| 
Form of Registration Rights Agreement for private placement transaction entered into on April 12, 2018. | 
| 
8-K | 
| 
4/16/2018 | 
| 
10.2 | 
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| |
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| |
| 
10.31 | 
| 
Engagement Letter, dated February 7, 2018, by and between the Registrant and Divine Capital Markets LLC. | 
| 
8-K | 
| 
4/16/2018 | 
| 
10.3 | 
| 
| |
| 72 | |
| 
10.32 | 
| 
Separation and Release Agreement, dated April 17, 2019 by and between the Company and William D. Schwieterman, M.D. | 
| 
8-K | 
| 
4/18/2019 | 
| 
10.1 | 
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| |
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| |
| 
10.33 | 
| 
Form of Securities Purchase Agreement, dated as of April 17, 2019, by and among the Company and Peak One | 
| 
8-K | 
| 
4/18/2019 | 
| 
10.2 | 
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| |
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| |
| 
10.34 | 
| 
Form of Securities Purchase Agreement, dated as of April 17, 2019, by and among the Company and the Bridge Investors. | 
| 
8-K | 
| 
4/18/2019 | 
| 
10.3 | 
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| 
10.35 | 
| 
Contingent Value Rights Agreement, dated April 17, 2019, by and among the Company, Oncotelic and American Stock Transfer and Trust Company LLC | 
| 
8-K | 
| 
4/25/2019 | 
| 
10.1 | 
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| 
10.36 | 
| 
Form of Securities Purchase Agreement, dated as of April 17, 2019, by and among the Company and Peak One Opportunity Fund, L.P. and TFK Investments, LLC. | 
| 
8-K | 
| 
4/25/2019 | 
| 
10.2 | 
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| |
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| |
| 
10.37 | 
| 
Form of Securities Purchase Agreement, dated as of April 17, 2019, by and among the Company and the Bridge Investors | 
| 
8-K | 
| 
4/25/2019 | 
| 
10.3 | 
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| |
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| 
10.38 | 
| 
Form of Securities Purchase Agreement, dated as of April 17, 2019, by and among the Company and Peak One Opportunity Fund, L.P. and TFK Investments, LLC. | 
| 
8-K | 
| 
6/20/2019 | 
| 
10.1 | 
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| 
10.39 | 
| 
Amendment to Securities Purchase Agreement dated as of June 12, 2019 by and between the Company and Peak One Opportunity Fund, L.P. | 
| 
8-K | 
| 
6/20/2019 | 
| 
10.2 | 
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| |
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| 
10.40 | 
| 
Separation Agreement dated as of July 1, 2019 by and between the Company and Matthew M. Loar Ex. | 
| 
8-K | 
| 
7/5/2019 | 
| 
10.1 | 
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| |
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| 
10.41 | 
| 
Note Purchase Agreement between Mateon Therapeutics, Inc. and PointR Data Inc. dated July 22, 2019. | 
| 
8-K | 
| 
7/24/2019 | 
| 
10.1 | 
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| 
10.42 | 
| 
Employment Agreement dated August 23, 2019 between the Company and Dr. Vuong Trieu. | 
| 
8-K | 
| 
8/29/2019 | 
| 
10.1 | 
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| |
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| 
10.43 | 
| 
Employment Agreement dated August 23, 2019 between the Company and Dr. Fatih Uckun. | 
| 
8-K/A | 
| 
11/25/2019 | 
| 
10.2 | 
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| |
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| 
10.44 | 
| 
Employment Agreement dated August 23, 2019 between the Company and Dr. Chulho Park. | 
| 
8-K | 
| 
8/29/2019 | 
| 
10.3 | 
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| 
10.45 | 
| 
Employment Agreement dated August 23, 2019 between the Company and Mr. Amit Shah. | 
| 
8-K | 
| 
8/29/2019 | 
| 
10.4 | 
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| |
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| 
10.46 | 
| 
Investigational Product Supply and Use Authorization Agreement for OT-101 U.S. Expanded Access (IPSUA) dated September 5, 2019, between WideTrial and Oncotelic. | 
| 
8-K | 
| 
9/10/2019 | 
| 
10.1 | 
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| |
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| |
| 
10.47 | 
| 
Agreement for Delivery and Licensed Use of Data Generated from OT-101 U.S. Expanded Access (Data License 1) dated September 5, 2019 between WideTrial and Oncotelic. | 
| 
8-K | 
| 
9/10/2019 | 
| 
10.2 | 
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| |
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| |
| 
10.48 | 
| 
Agreement for Delivery and Licensed Use of WideTrial Bonus Dataset (Data License 2 Agreement) dated September 5, 2019 between WideTrial and Oncotelic. | 
| 
8-K | 
| 
9/10/2019 | 
| 
10.3 | 
| 
| |
| 73 | |
| 
10.49 | 
| 
Form of Convertible Promissory Note, issued by the Company under the Note Purchase Agreement dated as of November 23, 2019. | 
| 
8-K | 
| 
11/25/2019 | 
| 
10.1 | 
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| |
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| |
| 
10.50 | 
| 
Research and Services Agreement. | 
| 
8-K | 
| 
3/23/2020 | 
| 
10.1 | 
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| |
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| |
| 
10.51 | 
| 
Supplement Research and Services Agreement. | 
| 
8-K | 
| 
3/23/2020 | 
| 
10.2 | 
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| |
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| |
| 
10.52 | 
| 
Paycheck Protection Program Promissory Note dated April 21, 2020 between Mateon Therapeutics, Inc. and Silicon Valley Bank. | 
| 
8-K | 
| 
4/27/2020 | 
| 
10.1 | 
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| |
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| |
| 
10.53 | 
| 
Form of Series A Warrant to purchase Common Stock. | 
| 
10-Q | 
| 
06/12/2020 | 
| 
10.1 | 
| 
| |
| 
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| 
| |
| 
10.54 | 
| 
Agreement between Oncotelic Inc, Autotelic Inc. and Autotelic BIO. | 
| 
8-K | 
| 
6/16/2020 | 
| 
10.1 | 
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| |
| 
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| 
| |
| 
10.55 | 
| 
Consulting Agreement by Between the Company and Artius, dated March 9, 2020 | 
| 
8-K/A | 
| 
6/22/2020 | 
| 
10.1 | 
| 
| |
| 
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| 
| |
| 
10.56 | 
| 
Consulting Agreement by Between the Company and Dr. Maida, dated May 5, 2020 | 
| 
8-K/A | 
| 
6/22/2020 | 
| 
10.2 | 
| 
| |
| 
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| 
| |
| 
10.57 | 
| 
Loan, Secured Convertible Note Purchase, and Security Agreement between the Company and Golden Mountain Partners, LLC dated June 27, 2020 | 
| 
10-Q | 
| 
11/16/2020 | 
| 
10.57 | 
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| |
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| 
| |
| 
10.58 | 
| 
Secured Convertible Promissory Note between the Company and Golden Mountain Partners, LLC dated June 27, 2020 | 
| 
10-Q | 
| 
11/16/2020 | 
| 
10.58 | 
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| |
| 
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| 
| |
| 
10.59 | 
| 
License, Development and Commercialization Agreement between Mateon Therapeutics, Inc. and Windlas Biotech Private Limited dated November 10, 2020 | 
| 
10-Q | 
| 
11/16/2020 | 
| 
10.59 | 
| 
| |
| 
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| 
| |
| 
10.60 | 
| 
Amendment to Certificate of Incorporation | 
| 
8-K | 
| 
02/02/2021 | 
| 
10.60 | 
| 
| |
| 
| 
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| 
| |
| 
10.61 | 
| 
Subscription Agreement by and between the Company and certain accredited investors dated | 
| 
8-K | 
| 
03/26/2021 | 
| 
10.1 | 
| 
| |
| 
| 
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| 
| 
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| 
| |
| 
10.62 | 
| 
Form of Registration Statement to register additional shares of Common Stock under 2015 Equity Incentive Plan | 
| 
S-8 | 
| 
04/19/2021 | 
| 
10.62 | 
| 
| |
| 
| 
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| 
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| 
| |
| 
10.63 | 
| 
Equity Purchase Agreement by and between the Company and Peak One Opportunity Fund L.P dated May 3, 2021 | 
| 
8-K | 
| 
05/07/2021 | 
| 
10.1 | 
| 
| |
| 
| 
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| 
| |
| 
10.64 | 
| 
Form for Registration of Securities | 
| 
S-1 | 
| 
05/24/2021 | 
| 
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| 
| |
| 
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| 
| |
| 
10.65 | 
| 
Form of Securities Purchase Agreement by and between the Company and Geneva Roth Remark Holding, Inc dated May 25, 2021 | 
| 
8-K | 
| 
06/01/2021 | 
| 
10.1 | 
| 
| |
| 74 | |
| 
10.66 | 
| 
Form of Securities Purchase Agreement and by and between the Company and Geneva Roth Remark Holding, Inc dated June 28, 2021 | 
| 
8-K | 
| 
07/02/2021 | 
| 
10.66 | 
| 
| |
| 
| 
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| 
| 
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| 
| |
| 
10.67 | 
| 
Form of Note Purchase Agreement by and between the Company and Autotelic Inc. dated August 4, 2021 | 
| 
8-K | 
| 
08/05/2021 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.68 | 
| 
Licensing Agreement by and between the Company and Autotelic Inc dated August 31, 2021 | 
| 
8-K | 
| 
09/03/2021 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.69 | 
| 
Unsecured Convertible Note Purchase Agreement by and between the Company and Golden Mountain Partners LLC dated September 21, 2021 | 
| 
8-K | 
| 
09/27/2021 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.70 | 
| 
Licensing Agreement by and between the Company and Autotelic Inc dated September 30, 2021 | 
| 
8-K | 
| 
10/04/2021 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.71 | 
| 
Unsecured Convertible Note Purchase Agreement by and between the Company and Golden Mountain Partners LLC dated October 25, 2021 | 
| 
8-K | 
| 
10/28/2021 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.72 | 
| 
Form of Securities Purchase Agreement by and between the Company and certain accredited investors | 
| 
8-K | 
| 
12/01/2021 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.73 | 
| 
Form of Convertible Notes by and between the Company certain accredited investors | 
| 
8-K | 
| 
12/01/2021 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.74 | 
| 
Form of Unsecured Convertible Note Purchase Agreement between the Company and Golden Mountain Partners dated January 31, 2022 | 
| 
8-K | 
| 
02/02/2022 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.75 | 
| 
Form of Convertible Promissory Note issued by the Company dated January 31, 2022 | 
| 
8-K | 
| 
02/02/2022 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.76 | 
| 
Form of Warrants issued by the Company to certain Investors, under the extension of Notes dated February 9, 2022 of the Note Purchase Agreement dated July 23, 2020 | 
| 
8-K | 
| 
02/15/2022 | 
| 
10.76 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.77 | 
| 
Form of Securities Purchase Agreement by and between the Company and certain accredited investors dated March 29, 2022 | 
| 
8-K | 
| 
04/04/2022 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.78 | 
| 
Form of Joint Venture Agreement between the Company and Dragon Overseas Capital Limited dated March 31, 2022 | 
| 
8-K | 
| 
04/06/2022 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.79 | 
| 
License Agreement between Oncotelic Therapeutics, Inc. and GMP Biotechnology Limited dated March 31, 2022 | 
| 
8-K | 
| 
04/06/2022 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.80 | 
| 
License Agreement between Oncotelic Therapeutics, Inc. and Sapu Holdings, LLC dated March 31, 2022 | 
| 
8-K | 
| 
04/06/2022 | 
| 
10.3 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.81 | 
| 
Independent consulting agreement between Oncotelic Therapeutics, Inc. and Fatih Uckun, MD, Ph.D. dated May 1, 2022 | 
| 
8-K | 
| 
5/6/2022 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.82 | 
| 
Independent consulting agreement between Oncotelic Therapeutics, Inc. and Seymour Fein, MD dated May 1, 2022 | 
| 
8-K | 
| 
5/6/2022 | 
| 
10.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.83 | 
| 
Securities Purchase Agreement between Oncotelic Therapeutics Inc. and certain accredited investors dated May 27, 2022 | 
| 
8-K | 
| 
6/3/2022 | 
| 
10.1 | 
| 
| |
| 75 | |
| 
10.84 | 
| 
Securities Purchase Agreement between Oncotelic Therapeutics Inc. and certain accredited investors dated June 22, 2022 | 
| 
8-K | 
| 
6/27/2022 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.85 | 
| 
Amended and Restated By-Laws | 
| 
8-K | 
| 
05/19/2023 | 
| 
3.2 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.86 | 
| 
Form of Subscription Agreement | 
| 
8-K | 
| 
07/13/2023 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.87 | 
| 
Form of warrant | 
| 
8-K | 
| 
07/13/2023 | 
| 
10.3 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.88 | 
| 
Form of note | 
| 
8-K | 
| 
07/13/2023 | 
| 
10.4 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.89 | 
| 
Registration Rights Agreement | 
| 
8-K | 
| 
07/13/2023 | 
| 
10.5 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
10.90 | 
| 
Form of Subscription Agreement | 
| 
8-K | 
| 
02/02/2024 | 
| 
10.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
23.1 | 
| 
Consent of the Independent Registered Accounting Firm | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
14.1 | 
| 
Corporate Code of Conduct and Ethics. | 
| 
10-K | 
| 
3/30/2015 | 
| 
14.1 | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
31.1 | 
| 
Certification of Chief Executive Officer pursuant to Rule 13a-14(a) and 15d-14(a). | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
31.2 | 
| 
Certification of Chief Financial Officer pursuant to Rule 13a-14(a) and 15d-14(a). | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
32.1 | 
| 
Certification of Chief Executive Officer pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906 of the Sarbanes- Oxley Act of 2002. | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
32.2 | 
| 
Certification of Chief Financial Officer pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906 of the Sarbanes- Oxley Act of 2002. | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
101.1 | 
| 
Interactive Data Files for the fiscal years ended December 31, 2023 and December 31, 2022 | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
101.INS | 
| 
Inline XBRL Instance Document | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
101.SCH | 
| 
Inline XBRL Taxonomy Extension Schema | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
101.CAL | 
| 
Inline XBRL Taxonomy Extension Calculation Linkbase | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
101.DEF | 
| 
Inline XBRL Taxonomy Extension Definition Linkbase | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
101.LAB | 
| 
Inline XBRL Taxonomy Extension Label Linkbase | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
101.PRE | 
| 
Inline XBRL Taxonomy Extension Presentation Linkbase | 
| 
| 
| 
| 
| 
x | 
| 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
104 | 
| 
Cover Page Interactive Data File (embedded within the Inline XBRL document) | 
| 
| 
| 
| 
| 
| 
| 
| |
| 
* | 
Confidential treatment has been granted for portions of this Exhibit. Redacted portions filed separately with the Securities and Exchange Commission. | |
| 
+ | 
Management contract or compensatory plan or arrangement. | |
| 76 | |
****
**SIGNATURES**
****
Pursuant to the requirements of
Section 13 or 15(d) of the Securities Exchange Act of 1934, the Registrant has duly caused this report to be signed on its behalf by the
undersigned, thereunto duly authorized.
| 
| 
Oncotelic Therapeutics, Inc. | |
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(Formerly Mateon Therapeutics, Inc.) | |
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/s/ VUONG TRIEU | |
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By: | 
VUONG TRIEU, PH. D. | |
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Chief Executive Officer | |
Date: April 15, 2025
Pursuant to the requirements of
the Securities Exchange Act of 1934, this report has been signed below by the following persons on behalf of the registrant and in the
capacities and on the dates indicated.
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Signature | 
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Title | 
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Date | |
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/s/ VUONG TRIEU | 
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President, Chief Executive Officer and Chairman of | 
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April 15, 2025 | |
| 
Vuong Trieu, Ph. D. | 
| 
the Board and Director (Principal executive officer) | 
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/s/ AMIT SHAH | 
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Chief Financial Officer (Principal financial and | 
| 
April 15, 2025 | |
| 
Amit Shah | 
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accounting officer) | 
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| |
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/s/ STEVEN KING | 
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Director | 
| 
April 15, 2025 | |
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Steven King | 
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/s/ ANTHONY MAIDA | 
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Director | 
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April 15, 2025 | |
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Anthony Maida, M.D., Ph. D. | 
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****
| 77 | |
****
**Oncotelic Therapeutics, Inc.**
**Index to Financial Statements**
The following financial statements of Oncotelic Therapeutics,
Inc.:
| 
| 
Page | |
| 
Report of Independent Registered Public Accounting Firm (PCAOB ID No. 468) | 
F-2 | |
| 
Consolidated Balance Sheets as of December 31, 2024 and 2023 | 
F-4 | |
| 
Consolidated Statements of Operations for the Years Ended December 31, 2024 and 2023 | 
F-5 | |
| 
Consolidated Statements of Stockholders Equity for the Year Ended December 31, 2024 | 
F-6 | |
| 
Consolidated Statements of Stockholders Equity for the Year Ended December 31, 2023 | 
F-7 | |
| 
Consolidated Statements of Cash Flow for the Years Ended December 31, 2024 and 2023 | 
F-8 | |
| 
Notes to Consolidated Financial Statements | 
F-9 | |
| | F-1 | | |
REPORT OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING
FIRM
To the Board of Directors and Stockholders of
Oncotelic Therapeutics, Inc.
**Opinion on the Financial Statements**
****
We have audited the accompanying consolidated balance
sheet of Oncotelic Therapeutics, Inc. and Subsidiaries (the Company) as of December 31, 2024 and 2023, and the related consolidated statements
of operations, stockholders equity, and cash flows for each of the years in the two-year period ended December 31, 2024, and the
related notes (collectively referred to as the consolidated financial statements). In our opinion, the consolidated financial statements
present fairly, in all material respects, the consolidated financial position of the Company as of December 31, 2024 and December 31,
2023, and the consolidated results of its operations and its cash flows for each of the years in the two-year period ended December 31,
2024, in conformity with accounting principles generally accepted in the United States of America.
**Going Concern Uncertainty**
****
The accompanying consolidated financial statements
have been prepared assuming that the Company will continue as a going concern. As discussed in Note 1 to the consolidated financial statements,
the Company has suffered recurring losses from operations and has an accumulated deficit and a working capital deficiency that raise substantial
doubt about its ability to continue as a going concern. Managements plans regarding these matters are also described in Note 1.
The consolidated financial statements do not include any adjustments that might result from the outcome of this uncertainty.
**Basis for Opinion**
****
These consolidated financial statements are the responsibility
of the Companys management. Our responsibility is to express an opinion on the Companys consolidated financial statements
based on our audit. We are a public accounting firm registered with the Public Company Accounting Oversight Board (United States) (PCAOB)
and are required to be independent with respect to the Company in accordance with the U.S. federal securities laws and the applicable
rules and regulations of the Securities and Exchange Commission and the PCAOB.
We conducted our audit in accordance with the standards
of the PCAOB. Those standards require that we plan and perform the audit to obtain reasonable assurance about whether the consolidated
financial statements are free of material misstatement, whether due to error or fraud. The Company is not required to have, nor were we
engaged to perform, an audit of its internal control over financial reporting. As part of our audit, we are required to obtain an understanding
of internal control over financial reporting, but not for the purpose of expressing an opinion on the effectiveness of the Companys
internal control over financial reporting. Accordingly, we express no such opinion.
Our audit included performing procedures to assess
the risks of material misstatement of the consolidated financial statements, whether due to error or fraud, and performing procedures
that respond to those risks. Such procedures included examining, on a test basis, evidence regarding the amounts and disclosures in the
consolidated financial statements. Our audit also included evaluating the accounting principles used and significant estimates made by
management, as well as evaluating the overall presentation of the consolidated financial statements. We believe that our audit provides
a reasonable basis for our opinion.
**Critical Audit Matters**
****
The critical audit matter communicated below is a
matter arising from the current period audit of the consolidated financial statements that were communicated or required to be communicated
to the audit committee and that: (1) relate to accounts or disclosures that are material to the consolidated financial statements and
(2) involved our especially challenging, subjective, or complex judgments. The communication of critical audit matters does not alter
in any way our opinion on the consolidated financial statements, taken as a whole, and we are not, by communicating the critical audit
matter below, providing separate opinions on the critical audit matter or on the accounts or disclosures to which it relates.
**Evaluation of Goodwill for Impairment**
****
*Description of the Matter*
**
As discussed in Note 2 and 3 to the consolidated financial
statements, reporting unit goodwill is tested for impairment at least annually or when events or circumstances indicate the fair value
of a reporting unit may be below its carrying value. This analysis involves comparing events and circumstances such as general macroeconomic
conditions, conditions specific to the industry and market and whether there has been sustained declines in share price. These fair value
estimates are sensitive to significant assumptions and judgments, such as projections of operating expenditures, discount rates, and future
economic conditions.
| | F-2 | | |
The Company has experienced a sustained decrease in
its share price, and as of December 31, 2024, the Companys market capitalization and uncertain economic conditions, which adversely
impacted the pharmaceutical and biotechnology industry, were indicative of an impairment. Pursuant to current accounting guidance, management
performed a quantitative analysis and concluded that goodwill was impaired and the Company recorded impairment charges of
approximately $3.2 million during the year ended December 31, 2024. At December 31, 2024, the Companys goodwill balance
was approximately $2.8 million.
Auditing managements annual impairment tests
for goodwill was complex because of the significant judgment required to evaluate the management assumptions described above used to
determine the fair value of the reporting units.
*How We Addressed the Matter in our Audit*
**
Our audit procedures related to the evaluation of
goodwill for impairment included the following, among others:
| 
| 
1. | 
We evaluated managements significant accounting policies related to the impairment of goodwill and indefinite-lived intangible assets for reasonableness. | |
| 
| 
2. | 
We evaluated managements assessment of qualitative factors relating to the goodwill valuation by reviewing information regarding economic growth forecast, industry outlook, and business environment, as well as accumulating our understanding of the Companys reporting units performance. | |
| 
| 
3. | 
With respect to the Companys valuation of its sole reporting unit: | |
| 
| 
a. | 
We assessed the qualifications and competence of management | |
| 
| 
b. | 
We evaluated the methodologies used to determine the fair value of the Companys reporting unit | |
| 
| 
c. | 
We reperformed managements quantitative analysis to assess the impact of goodwill impairment | |
| 
| 
4. | 
We assessed the adequacy of the Companys disclosures regarding impairment assessments included in Note 2 and Note 3. | |
**Evaluation
of Investment in GMP Bio at Fair Value**
****
*Description
of the Matter*
As
discussed in Note 6 to the consolidated financial statements, the Company holds a 45% non-controlling interest in GMP Bio. The Company
determined that it did not control the activities of GMP Bio but that it did have significant influence over GMP Bio. As a result, the
Company accounted for its investment using the equity method of accounting. During 2022, the year GMP Bio was formed, the Company elected
the fair value option under FASB ASC 825 relating to the accounting for its equity method investment in GMP Bio. The Fair Value Option
requires management to adjust the carrying value of the investment in GMP Bio to fair value each reporting period.
Auditing
managements estimate of fair value was complex because of the significant judgment required to evaluate managements assumptions
used to determine the fair value of its investment in GMP Bio.
*How
We Addressed the Matter in our Audit*
Our
audit procedures related to the evaluation of the fair value of the investment in GMP Bio included the following, among others:
| 
1. | We
evaluated the appropriateness of managements significant accounting policies related to the
fair value of investments. | |
| 
2. | We
inquired of management of the Company and of GMP Bio regarding clinical activities, capital
fundraising, and budget to actual assessments for GMP Bios operations. | |
| 
3. | With
respect to the Companys valuation of its investment in GMP Bio: | |
| 
a. | We
assessed the qualifications and competence of management | |
| 
b. | We
evaluated the methodologies used to determine the fair value of the Companys investment
in GMP Bio | |
| 
c. | We
considered the results of our inquiries and review of financial data of GMP Bio to assess
the reasonableness of managements assumptions | |
| 
d. | We
considered whether there were any events that would contradict managements assumptions | |
| 
Rose, Snyder & Jacobs LLP | |
| 
| |
| 
We have served as the Companys auditor since 2021. | |
| 
| |
| 
Encino, CA | |
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| |
| 
April 15, 2025 | |
| F-3 | |
****
**ONCOTELIC THERAPEUTICS, INC. AND SUBSIDIARIES**
**CONSOLIDATED BALANCE SHEETS**
****
| 
| | 
December 31, | | | 
December 31, | | |
| 
| | 
2024 | | | 
2023 | | |
| 
| | 
| | | 
| | |
| 
ASSETS | | 
| | | | 
| | | |
| 
Current assets: | | 
| | | | 
| | | |
| 
Cash | | 
$ | 86,128 | | | 
$ | 170,405 | | |
| 
Restricted cash | | 
| 20,000 | | | 
| 20,000 | | |
| 
Accounts receivable | | 
| 18,976 | | | 
| 18,976 | | |
| 
Prepaid & other current assets | | 
| 9,107 | | | 
| 62,356 | | |
| 
| | 
| | | | 
| | | |
| 
Total current assets | | 
| 134,211 | | | 
| 271,737 | | |
| 
| | 
| | | | 
| | | |
| 
In process R&D | | 
| 1,101,760 | | | 
| 1,101,760 | | |
| 
Goodwill, net | | 
| 2,788,230 | | | 
| 5,988,230 | | |
| 
Investment in GMP Bio at fair value | | 
| 22,653,225 | | | 
| 22,653,225 | | |
| 
Total assets | | 
$ | 26,677,426 | | | 
$ | 30,014,952 | | |
| 
| | 
| | | | 
| | | |
| 
LIABILITIES AND STOCKHOLDERS EQUITY | | 
| | | | 
| | | |
| 
Current liabilities: | | 
| | | | 
| | | |
| 
Accounts payable and accrued liabilities | | 
$ | 2,437,167 | | | 
$ | 2,437,321 | | |
| 
Accounts payable - related party | | 
| 346,057 | | | 
| 344,099 | | |
| 
Contingent Consideration | | 
| 2,625,000 | | | 
| 2,625,000 | | |
| 
Derivative liability on notes | | 
| 703,616 | | | 
| 423,214 | | |
| 
Convertible and short-term debt, net of costs | | 
| 9,790,866 | | | 
| 8,066,957 | | |
| 
Convertible debt and short-term debt - related party, net of costs | | 
| 3,297,208 | | | 
| 2,608,356 | | |
| 
Convertible debt and short-term debt, net of costs | | 
| 3,297,208 | | | 
| 2,608,356 | | |
| 
| | 
| | | | 
| | | |
| 
Total current liabilities | | 
| 19,199,914 | | | 
| 16,504,947 | | |
| 
| | 
| | | | 
| | | |
| 
Convertible long-term debt, net of costs | | 
| - | | | 
| 1,898,468 | | |
| 
| | 
| | | | 
| | | |
| 
Total liabilities | | 
| 19,199,914 | | | 
| 18,403,415 | | |
| 
| | 
| | | | 
| | | |
| 
Commitments and contingencies (Note 13) | | 
| - | | | 
| - | | |
| 
| | 
| | | | 
| | | |
| 
Stockholders equity: | | 
| | | | 
| | | |
| 
Common stock, $.01 parvalue; 750,000,000shares authorized; 407,289,618 and 399,184,128 issued and outstanding, respectively | | 
| 4,072,899 | | | 
| 3,991,839 | | |
| 
Additional paid-in capital | | 
| 42,219,400 | | | 
| 41,655,026 | | |
| 
Accumulated deficit | | 
| (38,040,668 | ) | | 
| (33,516,736 | ) | |
| 
| | 
| | | | 
| | | |
| 
Total Oncotelic Therapeutics, Inc. stockholders equity | | 
| 8,251,631 | | | 
| 12,130,129 | | |
| 
Non-controlling interests | | 
| (774,119 | ) | | 
| (518,592 | ) | |
| 
| | 
| | | | 
| | | |
| 
Total stockholders equity | | 
| 7,477,512 | | | 
| 11,611,537 | | |
| 
Total liabilities and stockholders equity | | 
$ | 26,677,426 | | | 
$ | 30,014,952 | | |
****
The accompanying footnotes are an integral part of
these consolidated financial statements.
| F-4 | |
****
**ONCOTELIC THERAPEUTICS, INC. AND SUBSIDIARIES**
**CONSOLIDATED STATEMENTS OF OPERATIONS**
****
| 
| | 
2024 | | | 
2023 | | |
| 
| | 
For the Year Ended December 31, | | |
| 
| | 
2024 | | | 
2023 | | |
| 
| | 
| | | 
| | |
| 
Service Revenue | | 
$ | - | | | 
$ | 70,000 | | |
| 
Total Revenue | | 
| - | | | 
| 70,000 | | |
| 
| | 
| | | | 
| | | |
| 
Operating expenses: | | 
| | | | 
| | | |
| 
Research and development | | 
$ | - | | 
$ | 61,143 | | |
| 
General and administrative | | 
| 376,013 | | | 
| 573,726 | | |
| 
Goodwill impairment (See note 2 and 3) | | 
| 3,200,000 | | | 
| 6,083,146 | | |
| 
Total operating expenses | | 
| 3,576,013 | | | 
| 6,718,015 | | |
| 
| | 
| | | | 
| | | |
| 
Income/(Loss) from operations | | 
| (3,576,013 | ) | | 
| (6,648,015 | ) | |
| 
Other income (expense): | | 
| | | | 
| | | |
| 
Interest expense, net | | 
| (857,723 | ) | | 
| (1,044,786 | ) | |
| 
Reimbursement for expenses - related party | | 
| 22,937 | | | 
| 72,246 | | |
| 
Change in fair value of investment in GMP Bio | | 
| - | | | 
| 12,706 | | |
| 
Change in fair value of derivative on debt | | 
| (280,402 | ) | | 
| (225,074 | ) | |
| 
Loss on debt conversion | | 
| (88,258 | ) | | 
| (373,142 | ) | |
| 
Total other income (expense) | | 
| (1,203,446 | ) | | 
| (1,558,050 | ) | |
| 
Net income (loss) before non-controlling interests | | 
| (4,779,459 | ) | | 
| (8,206,065 | ) | |
| 
Net loss attributable to non-controlling interests | | 
| (255,527 | ) | | 
| (302,972 | ) | |
| 
Net income (loss) attributable to Oncotelic Therapeutics, Inc. | | 
$ | (4,523,932 | ) | | 
$ | (7,903,093 | ) | |
| 
| | 
| | | | 
| | | |
| 
Basic net loss per share attributable to common stock | | 
$ | (0.01 | ) | | 
$ | (0.02 | ) | |
| 
Basic weighted average common stock outstanding | | 
| 404,396,473 | | | 
| 384,075,369 | | |
The accompanying footnotes are an integral
part of these consolidated financial statements.
| F-5 | |
****
**ONCOTELIC THERAPEUTICS, INC. AND SUBSIDIARIES**
**CONSOLIDATED STATEMENT OF STOCKHOLDERS EQUITY**
**FOR THE YEAR ENDED DECEMBER 31, 2024**
****
****
| 
| | 
Shares | | | 
Amount | | | 
Shares | | | 
Amount | | | 
Capital | | | 
Deficit | | | 
Interests | | | 
Equity | | |
| 
| | 
Preferred Stock | | | 
Common Stock | | | 
Additional
Paid-in | | | 
Accumulated | | | 
Non-controlling | | | 
Stockholders | | |
| 
| | 
Shares | | | 
Amount | | | 
Shares | | | 
Amount | | | 
Capital | | | 
Deficit | | | 
Interests | | | 
Equity | | |
| 
| | 
| | | 
| | | 
| | | 
| | | 
| | | 
| | | 
| | | 
| | |
| 
Balance at January 1, 2024 | | 
| - | | | 
$ | - | | | 
| 399,184,128 | | | 
| 3,991,839 | | | 
| 41,655,026 | | | 
| (33,516,736 | ) | | 
| (518,592 | ) | | 
$ | 11,611,537 | | |
| 
Common shares issued in connection with debt conversion | | 
| - | | | 
- | | | 
| 8,105,760 | | | 
| 81,060 | | | 
| 564,374 | | | 
| - | | | 
| - | | | 
| 645,434 | | |
| 
Net Loss | | 
| | | | 
| | | | 
| - | | | 
| - | | | 
| - | | | 
| (4,523,932 | ) | | 
| (255,527 | ) | | 
| (4,779,459 | ) | |
| 
Balance as ofDecember 31, 2024 | | 
| - | | | 
$ | - | | | 
| 407,289,888 | | | 
$ | 4,072,899 | | | 
$ | 42,219,400 | | | 
$ | (38,040,668 | ) | | 
$ | (774,119 | ) | | 
$ | 7,477,512 | | |
****
The accompanying footnotes are an integral
part of these consolidated financial statements.
| F-6 | |
****
**ONCOTELIC THERAPEUTICS, INC. AND SUBSIDIARIES**
**CONSOLIDATED STATEMENT OF STOCKHOLDERS EQUITY**
**FOR THE YEAR ENDED DECEMBER 31, 2023**
| 
| | 
Preferred Stock | | | 
Common Stock | | | 
Additional Paid-in | | | 
Accumulated | | | 
Non controlling | | | 
Stockholders | | |
| 
| | 
Shares | | | 
Amount | | | 
Shares | | | 
Amount | | | 
Capital | | | 
Deficit | | | 
Interests | | | 
Equity | | |
| 
| | 
| | | 
| | | 
| | | 
| | | 
| | | 
| | | 
| | | 
| | |
| 
Balance at January 1, 2023 | | 
| - | | | 
| - | | | 
| 391,846,880 | | | 
$ | 3,918,469 | | | 
$ | 41,416,632 | | | 
$ | (25,926,069 | ) | | 
$ | (215,620 | ) | | 
$ | 19,193,412 | | |
| 
Balance | | 
| - | | | 
| - | | | 
| 391,846,880 | | | 
| 3,918,469 | | | 
| 41,416,632 | | | 
| (25,926,069 | ) | | 
| (215,620 | ) | | 
$ | 19,193,412 | | |
| 
Adoption of ASU 2020-06 | | 
| | | | 
| | | | 
| - | | | 
| - | | | 
| (521,749 | ) | | 
| 312,426 | | | 
| - | | | 
| (209,323 | ) | |
| 
Common shares issued in connection with debt conversion | | 
| - | | | 
- | | | 
| 7,337,248 | | | 
| 73,370 | | | 
| 431,559 | | | 
| - | | | 
| - | | | 
| 504,929 | | |
| 
Loss on extinguishment of PPM debt | | 
| | | | 
| | | | 
| - | | | 
| - | | | 
| - | | | 
| - | | | 
| - | | | 
| - | | |
| 
Warrants issued with convertible notes | | 
| - | | | 
| - | | | 
| - | | | 
| - | | | 
| 328,584 | | | 
| - | | | 
| - | | | 
| 328,584 | | |
| 
Net Loss | | 
| - | | | 
| - | | | 
| - | | | 
| - | | | 
| - | | | 
| (7,903,093 | ) | | 
| (302,972 | ) | | 
| (8,206,065 | ) | |
| 
Balance as ofDecember 31, 2023 | | 
| - | | | 
$ | - | | | 
| 399,184,128 | | | 
$ | 3,991,839 | | | 
$ | 41,655,026 | | | 
$ | (33,516,736 | ) | | 
$ | (518,592 | ) | | 
$ | 11,611,537 | | |
| 
Balance | | 
| - | | | 
$ | - | | | 
| 399,184,128 | | | 
$ | 3,991,839 | | | 
$ | 41,655,026 | | | 
$ | (33,516,736 | ) | | 
$ | (518,592 | ) | | 
$ | 11,611,537 | | |
****
The accompanying footnotes are an integral
part of these consolidated financial statements.
| F-7 | |
****
**ONCOTELIC THERAPEUTICS, INC. AND SUBSIDIARIES**
**CONSOLIDATED STATEMENTS OF CASH FLOWS**
****
| 
| | 
2024 | | | 
2023 | | |
| 
| | 
For the Twelve Months Ended December 31, | | |
| 
| | 
2024 | | | 
2023 | | |
| 
Cash flows from operating activities: | | 
| | | | 
| | | |
| 
Net income (loss) | | 
$ | (4,779,459 | ) | | 
$ | (8,206,065 | ) | |
| 
Adjustments to reconcile net loss to net cash provided by (used in) operating activities: | | 
| | | | 
| | | |
| 
Goodwill impairment | | 
| 3,200,000 | | | 
| 6,083,146 | | |
| 
Amortization of debt discount and deferred finance costs | | 
| 122,141 | | | 
| 301,917 | | |
| 
Change in fair value of investment in GMP Bio | | 
| - | | | 
| (12,706 | ) | |
| 
Loss on debt conversion | | 
| 88,258 | | | 
| 373,142 | | |
| 
Write off accounts receivable | | 
| - | | | 
| 772 | | |
| 
Change in fair value of derivative | | 
| 280,402 | | | 
| 225,074 | | |
| 
Changes in operating assets and liabilities: | | 
| | | | 
| | | |
| 
Prepaid expenses and other current assets | | 
| 53,249 | | 
| (40,392 | ) | |
| 
Accounts payable and accrued expenses | | 
| 293,184 | | | 
| (72,771 | ) | |
| 
Accounts payable to related party | | 
| 1,958 | | | 
| 26,836 | | |
| 
Net cash provided by (used in) operating activities | | 
| (740,267 | ) | | 
| (1,321,047 | ) | |
| 
| | 
| | | | 
| | | |
| 
Cash flows from financing activities: | | 
| | | | 
| | | |
| 
Proceeds from / (repayment to) private placement | | 
| - | | 
| (125,000 | ) | |
| 
Proceeds from short term loans, others | | 
| 656,000 | | | 
| 1,410,000 | | |
| 
Repaid to others | | 
| - | | 
| (35,000 | ) | |
| 
Net cash provided by financing activities | | 
| 656,000 | | | 
| 1,250,000 | | |
| 
| | 
| | | | 
| | | |
| 
Net increase (decrease) in cash | | 
| (84,267 | ) | | 
| (71,047 | ) | |
| 
| | 
| | | | 
| | | |
| 
Cash and restricted cash - beginning of period | | 
| 190,405 | | | 
| 261,452 | | |
| 
| | 
| | | | 
| | | |
| 
Cash and restricted cash - end of period | | 
$ | 106,128 | | | 
$ | 190,405 | | |
| 
| | 
| | | | 
| | | |
| 
Supplemental cash flow information: | | 
| | | | 
| | | |
| 
Cash paid for: | | 
| | | | 
| | | |
| 
Interest paid | | 
| 365,940 | | | 
$ | 390,561 | | |
| 
Income taxes paid | | 
| 1,600 | | | 
$ | 1,600 | | |
| 
Common shares issued upon partial conversion of debt | | 
| 645,434 | | | 
$ | 504,929 | | |
****
The accompanying footnotes are an integral
part of these consolidated financial statements.
****
| F-8 | |
****
**ONCOTELIC THERAPEUTICS, INC. AND SUBSIDIARIES**
**NOTES TO CONSOLIDATED FINANCIAL STATEMENTS**
****
**NOTE 1 DESCRIPTION OF BUSINESS AND BASIS OF PRESENTATION**
****
*Description of Business*
**
Oncotelic Therapeutics, Inc. (*Oncotelic*),
was formed in the State of New York in 1988 as OXiGENE, Inc., was reincorporated in the State of Delaware in 1992, and changed its name
to Mateon Therapeutics, Inc. in 2016, and Oncotelic Therapeutics, Inc. in November 2020. Oncotelic conducts business activities through
Oncotelic and its wholly owned subsidiaries, Oncotelic, Inc., a Delaware corporation, PointR Data, Inc. (*PointR*),
a Delaware corporation; Pet2DAO, Inc (*Pet2DAO*) and EdgePoint AI, Inc. (*Edgepoint*), a Delaware
Corporation for which there are non-controlling interests, (Oncotelic, Oncotelic Inc., PointR, Pet2DAO and Edgepoint are collectively
called the *Company* or *We*). The Company completed a reverse merger with Oncotelic Inc in April
2019, a merger with PointR in November 2019 and formed a subsidiary Edgepoint in February 2020. For more information on these mergers,
refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 14, 2024.
The Company is currently developing
OT-101, through its joint venture (*JV*) with Dragon Overseas Capital Limited (*Dragon*) and GMP
Biotechnology Limited (*GMP Bio*), both affiliates of Golden Mountain Partners (*GMP*), for various
cancers and COVID-19, Artemisinin for COVID-19 and AI technologies for clinical development and manufacturing. The JV is also developing
5 additional compounds, which if approved, are anticipated to be significant value contributors for the JV, as well as the Company. The
Company is also, independently, planning to develop OT-101 for certain animal health indications and contemplating using crypto currencies
for that platform. The Company has acquired apomorphine for Parkinsons Disease, erectile dysfunction and female sexual dysfunction.
In addition, the Company is evaluating the further development of its product candidates OXi4503 as a treatment for acute myeloid leukemia
and myelodysplastic syndromes and CA4P in combination with a checkpoint inhibitor for the treatment of advanced metastatic melanoma.
The Company is primarily a cancer
immunotherapy company dedicated to the development of first in class self-immunization protocol (*SIP*) candidates
for difficult to treat cancers. The Companys proprietary SIP candidates are expected to offer advantages over other immunotherapies
because they do not require extraction of the tumor or isolation of the antigens, and they have the potential for broad-spectrum applicability
for multiple cancer types. The Companys proprietary product candidates have shown promising clinical activity in phase 2 trials
for the treatment of gliomas and pancreatic cancers. The Company aims to translate its unique insights, which span more than three decades
of original work using RNA therapeutics, into the deployment of antisense as a RNA therapeutic for diseases which are caused by TGF-
overexpression, starting with cancer and expanding to Duchenne Muscular Dystrophy (*DMD*) and others. OT-101, is being
developed as a broad-spectrum anti-cancer drug that can also be used in combination with other standard cancer therapies to establish
an effective multi-modality treatment strategy for difficult-to-treat cancers. Further, The JV is also developing 5 additional compounds,
which if approved, are anticipated to be significant revenue and value contributors for the JV as well as the Company. The JV plans to
initiate phase 2 and 3 clinical trials for OT-101 in both high-grade glioma and pancreatic cancer, and any other indications that may
evolve, for human pharmaceutical needs. The JV may also be sponsoring investigator-initiated studies for OT-101 for other oncology indications.
The Company is evaluating the further development of its product candidates OXi4503, as a treatment for acute myeloid leukemia and myelodysplastic
syndromes, and CA4P, in combination with a checkpoint inhibitor for the treatment of advanced metastatic melanoma. The JV is also developing
OT-101 for the various epidemics and pandemics, similar to the corona virus (*COVID-19*) pandemic. In this connection,
the Company entered into an agreement and supplemental agreement with GMP for a total of $1.2 million to render services and was paid
for the development of OT-101. For more information on GMP and Artemisinin, refer to our 2023 Annual report on Form 10- K filed with the
SEC on April 12, 2024.
| F-9 | |
*Fundraising*
**
Private Placement 2 & JH Darbie Financing
Between July 2023 and September
2023, the Company entered into a series of subscription agreements with 15 accredited investors which resulted in a conversion of a gross
amount of $1.0 million, consisting of 40 notes, under the prior JH Darbie Financing into new debt to the Company. JH Darbie and the Company
are parties to a March 2023 placement agent agreement (Agreement) pursuant to which JH Darbie has the right to sell/convert
a minimum of 10 Units and a maximum of 200 Units on a best-efforts basis. Further, in October 2023, the Company entered into a series
of subscription agreements with 27 accredited investors which resulted in a conversion of a gross amount of $1.05 million, consisting
of 42 notes, under the prior JH Darbie Financing into new debt to the Company. Additionally, in January 2024, Company entered into a series
of subscription agreements with 4 accredited investors which resulted in a conversion of a gross amount of $0.3 million, consisting of
12 notes. The July 2023, October 2023 and January 2024 conversions fully converted JH Darbie PPM-1 notes into PPM-2 notes. For more information
on the new JH Darbie Financing, refer to Note 8 of these Notes to the Consolidated Financial Statements.
J.H. Darbie Financing Notes & Issuance of Oncotelic Warrants
In February 2022, the Company
and 99 out of 100 of the Investors agreed to extend the maturity date of the notes connected to the Units from March 31, 2022 to March
31, 2023. In addition, the Company issued approximately 33 million warrants to purchase $50,000 of shares of common stock of the Company
(Common Stock) in connection with agreeing to extend the maturity date by one year. The issuance of the additional warrants
resulted in the Company recording an expense of approximately $2.9 million in the Companys statement of operations during the year
ended December 31, 2022. The approximately 33 million warrants to purchase shares of our Common Stock expired on March 31, 2024. For more
information on the JD Darbie financing, refer to Note 7 of these unaudited Notes to the Consolidated Financial Statements.
Equity Purchase Agreement
In May 2021, the Company entered
into an Equity Purchase Agreement (the *EPL*) and Registration Rights Agreement (the *Registration Rights
Agreement*) with Peak One Opportunity Fund, L.P. (*Peak One*), pursuant to which the Company shall have the
right, but not the obligation, to direct Peak One to purchase up to $10.0 million (the *Maximum Commitment Amount*)
in shares of the common stock, par value $0.01 per share (*Common Stock*) in multiple tranches. The Company filed a
post-effective amendment for the EPL on April 12, 2024 with the SEC and the SEC has made the post-effective amendment effective on April
22, 2024. The Company filed a prospectus under rule 424b3 with the SEC on April 26, 2024. For more information on the EPL, refer to Note
10 of the Notes to the Unaudited Consolidated Financial Statements.
August 2021 Notes
In August 2021, the Company issued
Note Purchase Agreements with Autotelic Inc., the Companys Chief Financial Officer (*CFO*), and certain other
accredited investors. Under the terms of the Note Purchase Agreements, the Company issued an aggregate of $698,500 (the *Principal
Amount*) in debt in the form of unsecured convertible promissory notes (collectively, the *Notes*). The Notes
are unsecured, and provide for interest at the rate of 5% per annum. Such Notes were issued against some of the short-term debt due as
of June 30, 2021. For more information on the debt financing of the Company, refer to Note 5 of the Notes to the Consolidated Financial
Statements.
November/December 2021 and March 2022 Notes
In November / December 2021, the
Company entered into various Securities Purchase Agreements with Talos Victory Fund, LLC (the (Talos), Mast Hill Fund, LP
(Mast), FirstFire Global Opportunities Fund, LLC (FirstFire), Blue Lake Partners, LLC (Blue Lake)
and Fourth Man, LLC (Fourth Man), pursuant to which the Company issued convertible promissory notes in the aggregate principal
amount of $0.25 million each, aggregating gross $1.25 million (the Notes), and which Notes were convertible into shares
of the Companys common stock, par value $0.01 per share (Common Stock). In June 2022, Mast fully converted their
November 2021 Note, for which the company issued 4,025,000 shares of Common Stock. Further, during the year ended December 31, 2023, the
Company fully converted the balance of Fourth Man convertible note of approximately $127,000 into 1,820,395 shares of the Companys
common stock, which fully retired the convertible note as of December 31, 2024.
| F-10 | |
In March 2022, the Company entered
into a Securities Purchase Agreement with Fourth Man, pursuant to which the Company issued convertible promissory note in the aggregate
principal amount of $0.25 million, which Note is convertible into shares of the Companys Common Stock. As of December 31, 2024, this
note is in default and available for conversion into the Companys Common Stock due to cross default provision contained in November
/ December 2021 Notes. During the year ended December 31, 2024, Fourth Man converted a portion of the March 2022 debt, including interest,
and conversion fee, of approximately $35,000 for 500,000 shares of the Companys Common Stock.
For more information on the debt
financing of the Company, refer to Note 5 of the Notes to the Consolidated Financial Statements.
May 2022 Note
In May 2022, the Company entered
into a Securities Purchase Agreement with Mast, pursuant to which the Company issued convertible promissory notes in the aggregate principal
amount of $0.6 million, which note is convertible into shares of the Companys Common Stock. In May 2024, the May 2022 Note was
extended till May 2025, at a cost of 10% of the outstanding Note amount, including interest and penalty. For more information on the
debt financing of the Company, refer to Note 5 of the Notes to the Consolidated Financial Statements.
June 2022 Note
In June 2022, the Company entered
into a Securities Purchase Agreement with Blue Lake, pursuant to which the Company issued convertible promissory notes in the aggregate
principal amount of $0.34 million, which note is convertible into shares of the Companys Common Stock. During the year ended December
31, 2024, Blue Lake converted the balance of their debt, including accrued interest and penalty, of approximately $531,000 for approximately
7.6 million shares of the Companys Common Stock.
For more information on the debt
financing of the Company, refer to Note 5 of the Notes to the Consolidated Financial Statements.
Forever Prosperity (previously GMP) Note purchase agreements and unsecured
notes
Between June 2020 and January
2022, the Company entered into various purchase agreements and promissory notes with GMP, cumulatively totaling $4.5 million. Such notes
were assigned to Forever Prosperity, LLC, an affiliated entity of GMP.
For more information on the GMP
debt financing, refer to Note 5 of the Notes to the Consolidated Financial Statements.
Joint Venture with GMP Bio
In March 2022, the Company formalized
a joint venture (*JV*) with Dragon Overseas Capital Limited (*Dragon*) and GMP Biotechnology Limited
(*GMP Bio*), both affiliates of GMP. Although no assurances can be given, the Company and GMP currently intend to conduct
an initial public offering of the JV, at a future date, on either the Hong Kong Exchange or other stock exchange.
For more information on the JV,
refer to Note 6 of the Notes to the Consolidated Financial Statements.
Pet2DAO
In November 2022, the Company
formed a Decentralized autonomous organization (*DAO*) entity, Pet2DAO LLC (*Pet2DAO*), as a wholly
owned subsidiary.
For more information on Pet2DAO,
refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
| F-11 | |
Mosaic ImmunoEngineering, Inc. Term Sheet
In April 2024, the Company entered into a binding
term sheet (the Term Sheet) with Mosaic ImmunoEngineering, Inc. (*Mosaic*). For more information on the
Term Sheet, refer to the Current Report on Form 8-K filed with the SEC on April 29, 2024. In August 2024, Mosaic and the Company mutually
agreed to extend the date of the Term Sheet to expire at the earlier of (1) the signing of definitive agreements or (2) December 31, 2024.
In December 2024, he Company and Mosaic further extended the term of the term-sheet to expire at the earlier of (1) the signing of definitive
agreements or (2) June 30, 2025. This was to allow for both Companies to complete due diligence as well as agree and finalize the definitive
agreements. The Company had advanced $40 thousand to Mosaic in accordance with the terms of the Term Sheet, and Mosaic has repaid the
amount, with interest to the Company as of December 31, 2024.
**
*Licensing Agreement with Autotelic Inc.*
**
In September 2021, the Company
entered into an exclusive License Agreement (the *Agreement*) with Autotelic, Inc. (*Autotelic*).
For more information on the Agreement, refer to our 2023 10-K filed with the SEC on April 12, 2024.
*Principles of Consolidation*
**
The consolidated financial statements
include the accounts of the Company and its wholly owned subsidiaries, Oncotelic, PointR and Edgepoint for which there are non-controlling
interests. Intercompany accounts and transactions have been eliminated in consolidation.
*Basis of Presentation*
**
The accompanying consolidated
financial statements have been prepared by the Company pursuant to the rules and regulations of the Securities and Exchange Commission
including Form 10-K and Regulation S-X.
*Liquidity and Going Concern*
**
The accompanying consolidated
financial statements have been prepared assuming that the Company will continue as a going concern. The Company has incurred net losses
of approximately $38 million since inception of Oncotelic Inc. as the Companys historical financial statements before the Merger
have been replaced with the historical financial statements of Oncotelic Inc. prior to the Merger in the financial statements and filings.
The Company also has a negative working capital of approximately $19.1 million at December 31, 2024, of which approximately $2.6 million
contingent liability of issuance of common shares of the Company to PointR shareholders upon achievement of certain milestones in accordance
with the PointR Merger Agreement. The Company has negative cash flows from operations for the year ended December 31, 2024 of approximately
$0.7 million. These conditions raise substantial doubt about the Companys ability to continue as a going concern for a period of
one year from the date of this filing. Management expects to incur significantly lower costs and losses in the foreseeable future, as
a majority of the costs related with the development of OT-101 will be incurred by the JV, but the Company also recognizes the need to
raise capital to remain viable. The accompanying consolidated financial statements do not include any adjustments that might be necessary
should the Company be unable to continue as a going concern.
The Companys long-term
plans include continued development of its current pipeline of products, in addition to continue the development of OT-101 which is exclusively
out-licensed to the JV and the JV will be responsible for the funding required to support the development in entirety, to generate sufficient
revenues, through either technology transfer or product sales, or raise additional financing to cover its anticipated expenses. Until
the Company is able to generate sufficient revenues from its current pipeline, the Company plans on funding its operations through the
sale of equity and/or the issuance of debt, combined with or without warrants or other equity instruments. The Company obtained short
term loans of approximately $0.6 million from Autotelic Inc., a related party, during the year ended December 31, 2024. In addition, the
Company obtained a short-term loan of $41 thousand from Amit Shah, its CFO during year ended December 31, 2024.
Although no assurances can be
given as to the Companys ability to deliver on its revenue plans, or that unforeseen expenses may arise, management believes that
the potential equity and debt financing or other potential financing will provide the necessary funding for the Company to continue as
a going concern. Also, management cannot guarantee any potential debt or equity financing will be available on favorable terms or at all.
As such, management does not believe the Company has sufficient cash for 12 months from the date of this report. If adequate funds are
not available on acceptable terms, or at all, the Company will need to curtail operations, or cease operations completely.
| F-12 | |
**NOTE 2 - SUMMARY OF SIGNIFICANT ACCOUNTING POLICIES**
****
*Use of Estimates*
**
The preparation of financial statements
in conformity with US GAAP requires management to make estimates and assumptions that affect the reported amounts of assets, liabilities,
equity-based transactions and disclosure of contingent liabilities at the date of the financial statements and revenues and expense during
the reporting period. Actual results could materially differ from those estimates.
The Company believes the following
critical accounting policies affect its more significant judgments and estimates used in the preparation of the financial statements.
Significant estimates include the valuation of goodwill and intangible assets for impairment, deferred tax asset and valuation allowance,
and fair value of financial instruments.
*Cash*
**
As of December 31, 2024 and 2023,
respectively, the Company held all its cash in banks in the United States of America. The Company considers investments in highly liquid
instruments with a maturity of three months or less to be cash equivalents. The Company did not have any cash equivalents as of December
31, 2024 and 2023, respectively. Restricted cash consists of certificates of deposits held at banks as collateral for various purposes.
*Debt issuance Costs and Debt discount*
**
Issuance costs are specific incremental
costs that are (1) paid to third parties and (2) directly attributable to the issuance of a debt or equity instrument. The issuance costs
attributable to the initial sale of the instrument are offset against the associated proceeds in the determination of the instruments
initial net carrying amount.
Debt issuance costs and debt discounts
are being amortized over the lives of the related financings on a basis that approximates the effective interest method. Costs and discounts
are presented as a reduction of the related debt in the accompanying balance sheets if related to the issuance of debt or presented as
a reduction of additional paid in capital if related to the issuance of an equity instrument. The Company applies the relative fair value
to allocate the issuance costs among freestanding instruments that form part of the same transaction.
If the Company amends the terms
of its convertible notes, the Company reviews and applies the guidance per ASC 470-60 *Troubled debt restructurings*and ASC 470-50
*Debt-Modifications and Extinguishments*, evaluates and concludes whether the terms of the agreements were or were not substantially
different as of a particular reporting date and accounts the transaction as a debt modification or a troubled debt restructuring.
*Fair Value of Financial Instruments*
**
The carrying value of cash, accounts
payable and accrued expense approximate their fair values based on the short-term maturity of these instruments. As defined in ASC 820,
Fair Value Measurements and Disclosures, fair value is the price that would be received to sell an asset or paid to transfer
a liability in an orderly transaction between market participants at the measurement date (exit price). The Company utilizes market data
or assumptions that market participants would use in pricing the asset or liability, including assumptions about risk and the risks inherent
in the inputs to the valuation technique. These inputs can be readily observable, market corroborated, or generally unobservable. ASC
820 establishes a fair value hierarchy that prioritizes the inputs used to measure fair value. The hierarchy gives the highest priority
to unadjusted quoted prices in active markets for identical assets or liabilities (level 1 measurement) and the lowest priority to unobservable
inputs (level 3 measurement). This fair value measurement framework applies at both initial and subsequent measurement.
The three levels of the fair value hierarchy defined by ASC 820 are as
follows:
| 
| 
Level 1 Quoted prices are available in active markets for identical assets or liabilities as of the reporting date. Active markets are those in which transactions for the asset or liability occur in sufficient frequency and volume to provide pricing information on an ongoing basis. Level 1 primarily consists of financial instruments such as exchange-traded derivatives, marketable securities and listed equities. | |
| F-13 | |
| 
| 
Level 2 Pricing inputs are other than quoted prices in active markets included in Level 1, which are either directly or indirectly observable as of the reported date. Level 2 includes those financial instruments that are valued using models or other valuation methodologies. These models are primarily industry-standard models that consider various assumptions, including quoted forward prices for commodities, time value, volatility factors and current market and contractual prices for the underlying instruments, as well as other relevant economic measures. Substantially all of these assumptions are observable in the marketplace throughout the full term of the instrument, can be derived from observable data or are supported by observable levels at which transactions are executed in the marketplace. Instruments in this category generally include non- exchange-traded derivatives such as commodity swaps, interest rate swaps, options and collars. | |
| 
| 
| |
| 
| 
Level 3 Pricing inputs include significant inputs that are generally less observable from objective sources. These inputs may be used with internally developed methodologies that result in managements best estimate of fair value. | |
The Company did not have any Level
1 or Level 2 assets and liabilities at December 31, 2024 and 2023.
*Investment in equity securities*
**
The following table summarizes
the cumulative gross unrealized gains and losses and fair values for long- term investments accounted for at fair value under the fair
value option, with the unrealized gains and losses reported within earnings on the Condensed Consolidated Statements of Operation as of
December 31, 2024 and 2023:
SCHEDULE
OF UNREALIZED GAINS AND LOSSES
| 
| | 
Initial 
Book Value | | | 
Cumulative 
Gross Unrealized 
Gains | | | 
Cumulative 
Gross Unrealized 
Losses | | | 
Fair Value | | |
| 
December 31, 2024 | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Investment in GMP Bio (equity securities) | | 
$ | 22,653,225 | | | 
$ | - | | | 
$ | - | | | 
$ | 22,653,225 | | |
| 
Total | | 
$ | 22,653,225 | | | 
$ | - | | | 
$ | - | | | 
$ | 22,653,225 | | |
| 
| | 
Initial
Book Value | | | 
Cumulative Gross Unrealized Gains | | | 
Cumulative 
Gross Unrealized 
Losses | | | 
Fair Value | | |
| 
December 31, 2023 | | 
| | | | 
| | | | 
| | | | 
| | | |
| 
Investment in GMP Bio (equity securities) | | 
$ | 22,640,519 | | | 
$ | 12,706 | | | 
$ | - | | | 
$ | 22,653,225 | | |
| 
Total | | 
$ | 22,640,519 | | | 
$ | 12,706 | | | 
$ | - | | | 
$ | 22,653,225 | | |
The table above sets forth a summary
of the recording of the initial value of the long-term value of investment in equity securities of GMP Bio, based on a third-party valuation
report, and changes in the fair value of such equity securities, if such change occurs, as a Level 3 fair value as of December 31, 2024
and 2023. During the year ended December 31, 2024, there have been no changes in the long-term value of the investment in equity securities
of GMP Bio.
| F-14 | |
**
*Derivative Liability*
**
The Company has certain derivative
liabilities associated with its 2019 bridge financing Convertible Notes (see Note 5), consisted of conversion feature derivatives at December
31, 2024 and 2023, are Level 3 fair value measurements.
The table below sets forth a summary
of the changes in the fair value of the Companys derivative liabilities classified as Level 3 as of December 31, 2024 and 2023:
SUMMARY
OF CHANGES IN FAIR VALUE OF DERIVATIVE LIABILITIES
| 
| | 
December 31, 2024 Conversion Feature | | | 
December 31, 2023 Conversion Feature | | |
| 
Balance at January 1, 2024 and 2023 | | 
$ | 423,214 | | | 
$ | 198,140 | | |
| 
Change in fair value | | 
| 280,403 | | | 
| 225,074 | | |
| 
Balance at December 31, 2024 and 2023 | | 
$ | 703,617 | | | 
$ | 423,214 | | |
At December 31, 2024 and 2023,
respectively, the Company estimated the fair value of the conversion feature derivatives embedded in the convertible debentures based
on assumptions used in the Black-Scholes valuation model. The key valuation assumptions used consists, in part, of the price of the Companys
Common Stock, a risk-free interest rate based on the yield of a Treasury note and expected volatility of the Companys Common Stock
all as of the measurement dates. The Company used the following assumptions to estimate fair value of the derivatives as of December 31,
2024 and 2023:
SUMMARY
OF ESTIMATE FAIR VALUE OF DERIVATIVE LIABILITIES
| 
| 
| 
| 
December 31, 
2024 | 
| 
| 
December
31, 
2023 | 
| |
| 
Risk free interest | 
| 
| 
| 
3.98% - 5.09% | 
| 
| 
| 
4.64% - 5.40% | 
| |
| 
Market price of share | 
| 
| 
| 
$ 0.02 - 0.04 | 
| 
| 
| 
$ 0.03 - 0.05 | 
| |
| 
Life of instrument in years | 
| 
| 
| 
0.01 | 
| 
| 
| 
0.01 | 
| |
| 
Volatility | 
| 
| 
| 
138.38%-226.9 | 
% | 
| 
| 
142.45%-236.86 | 
% | |
| 
Dividend yield | 
| 
| 
| 
0 | 
% | 
| 
| 
0 | 
% | |
When the Company changes its valuation
inputs for measuring financial liabilities at fair value, either due to changes in current market conditions or other factors, it may
need to transfer those liabilities to another level in the hierarchy based on the new inputs used. The Company recognizes these transfers
at the end of the reporting period that the transfers occur. For the years ended December 31, 2024 and 2023, there were no transfers of
financial assets or financial liabilities between the hierarchy levels.
The $2,625,000 of contingent consideration,
of shares issuable to PointR shareholders which was recorded and associated with the PointR Merger, is also classified as Level 3 fair
value measurements. The Company initially recorded the contingency based on a valuation conducted by a third-party valuation expert. The
valuation was based on a probability of the completion of certain milestones by PointR for the shareholders to earn additional shares.
The Company evaluated the probability of the earning of the milestones and concluded that the probability of achievement of the milestones
had not changed, primarily due to the shifting of focus by the Company to develop AI technologies for the COVID-19 pandemic and other
technologies being developed. As such, the Company did not record any change to the valuation during the years ended December 31, 2024
or 2023, respectively; and as of December 31, 2024 and 2023, respectively.
| F-15 | |
**
*Net Income (Loss) Per Share*
**
Basic net income (loss) per common
share is computed by dividing the net income (loss) by the weighted- average number of common shares outstanding during the period. Diluted
net income (loss) per share includes the effect of Common Stock equivalents (notes convertible into Common Stock, stock options and warrants)
when, under either the treasury or if-converted method, such inclusion in the computation would be dilutive. During the years ended December
31, 2024 and 2023, no equivalent shares of the Common Stock were included as the Company had incurred losses during this period and addition
of such stock equivalents in the computation would have been anti-dilutive.
*Stock-Based Compensation*
**
The Company applies the provisions
of ASC 718, CompensationStock Compensation (*ASC 718*), which requires the measurement and recognition of compensation
expense for all stock-based awards made to employees and non-employees, including employee stock options, in the statements of operations.
For stock options issued, the
Company estimates the grant date fair value of each option using the Black- Scholes option pricing model. The use of the Black-Scholes
option pricing model requires management to make assumptions with respect to the expected term of the option, the expected volatility
of the Common Stock consistent with the expected life of the option, risk-free interest rates and expected dividend yields of the Common
Stock. For awards subject to service-based vesting conditions, including those with a graded vesting schedule, the Company recognizes
stock-based compensation expense equal to the grant date fair value of stock options on a straight-line basis over the requisite service
period, which is generally the vesting term. Forfeitures are recorded as they are incurred as opposed to being estimated at the time of
grant and revised.
For warrants issued in connection
with fund raising activities, the Company estimates the grant date fair value of each warrant using the Black-Scholes pricing model. The
use of the Black-Scholes option pricing model requires management to make assumptions with respect to the expected term of the warrant,
the expected volatility of the Common Stock consistent with the expected life of the warrant, risk-free interest rates and expected dividend
yields of the Common Stock. If the warrants are issued upon termination or cancellation of prior issued warrants, then the Company estimates
the grant date fair value of the new warrants using the Black-Scholes pricing model and evaluates whether the new warrants are deemed
as equity instruments or liability instruments. If the warrants are deemed to be equity instruments, the Company records stock compensation
expense and an addition to additional paid in capital. If however, the warrants are deemed to be liability instruments, then the fair
value is treated as a deemed dividend and credited to additional paid in capital.
*Impairment of Long-Lived Assets*
The Company reviews long-lived
assets, including definite-lived intangible assets, for impairment whenever events or changes in circumstances indicate that the carrying
amount of such assets may not be recoverable. Recoverability of these assets is determined by comparing the forecasted undiscounted net
cash flows of the operation to which the assets relate to the carrying amount. If the operation is determined to be unable to recover
the carrying amount of its assets, then these assets are written down first, followed by other long-lived assets of the operation to fair
value. Fair value is determined based on discounted cash flows or appraised values, depending on the nature of the assets. For the years
ended December 31, 2024 and 2023, there were no impairment losses recognized for long- lived assets.
*Intangible Assets*
**
The Company records its intangible
assets at cost in accordance with ASC 350, Intangibles Goodwill and Other. The Company reviews the intangible assets for impairment
on an annual basis or if events or changes in circumstances indicate it is more likely than not that they are impaired. These events could
include a significant change in the business climate, legal factors, a decline in operating performance, competition, sale or disposition
of a significant portion of the business, or other factors. If the review indicates the impairment, an impairment loss would be recorded
for the difference of the value recorded and the new value. For the years ended December 31, 2024 and 2023, there were no impairment losses
recognized for intangible assets. When we sell or contribute properties to unconsolidated arrangements and retain a non-controlling ownership
interest in such assets, we recognize the difference between the consideration received and the carrying amount of the asset sold or contributed.
| F-16 | |
*Goodwill*
**
Goodwill represents the excess
of the purchase price of acquired business over the estimated fair value of the identifiable net assets acquired. Goodwill is not amortized
but is tested for impairment at least once annually, at the reporting unit level or more frequently if events or changes in circumstances
indicate that the asset might be impaired. The goodwill impairment test is applied by performing a qualitative assessment before calculating
the fair value of the reporting unit. If, on the basis of qualitative factors, it is considered not more likely than not that the fair
value of the reporting unit is less than the carrying amount, further testing of goodwill for impairment would not be required. Otherwise,
goodwill impairment is tested using a two-step approach.
The first step involves
comparing the fair value of the reporting unit to its carrying amount. The Company has always operated as a single unit. If the fair
value of the reporting unit is determined to be greater than its carrying amount, there is no impairment. If the reporting
units carrying amount is determined to be greater than the fair value, the second step must be completed to measure the
amount of impairment, if any. The second step involves calculating the implied fair value of goodwill by deducting the fair value of
all tangible and intangible assets, excluding goodwill, of the reporting unit from the fair value of the reporting unit as
determined in step one. The implied fair value of the goodwill in this step is compared to the carrying value of goodwill. If the
implied fair value of the goodwill is less than the carrying value of the goodwill, an impairment loss equivalent to the difference
is recorded. When we sell or contribute properties to unconsolidated arrangements and retain a non-controlling ownership interest in
such assets, we recognize the difference between the consideration received and the carrying amount of the asset sold or
contributed. For the years ended December 31, 2024 and 2023, we recorded an impairment loss of approximately $3.2
million and $6.1
million and, respectively, on our goodwill, based on the difference between the carrying value of our goodwill as against the market
capitalization of the Company. For more information on goodwill and impairment, refer to Note 3 to these Notes to the Consolidated
Financial Statements.
*Derivative Financial Instruments Indexed to the Companys Common
Stock*
**
We have generally issued derivative
financial instruments, such as warrants, in connection with our equity offerings. We evaluate the terms of these derivative financial
instruments in order to determine their accounting treatment in our financial statements. Key considerations include whether the financial
instruments are freestanding and whether they contain conditional obligations. If the warrants are freestanding, do not contain conditional
obligations and meet other classification criteria, we account for the warrants as an equity instrument. However, if the warrants contain
conditional obligations, then we account for the warrants as a liability until the conditional obligations are met or are no longer relevant.
Because no established market prices exist for the warrants that we issue in connection with our equity offerings, we must estimate the
fair value of the warrants based on the price of our Common Stock as of December 31 each year, which is as inherently subjective as it
is for stock options, and for similar reasons as noted in the stock-based compensation section above. For financial instruments which
are accounted for as a liability, we report any changes in their estimated fair values as gains or losses in our Consolidated Statement
of Income.
*Convertible Instruments*
**
The Company evaluates and accounts
for conversion options embedded in its convertible instruments in accordance with ASC 815 Derivatives and Hedging.
ASC 815 generally provides three
criteria that, if met, require companies to bifurcate conversion options from their host instruments and account for them as free-standing
derivative financial instruments. These three criteria include circumstances in which (a) the economic characteristics and risks of the
embedded derivative instrument are not clearly and closely related to the economic characteristics and risks of the host contract, (b)
the hybrid instrument that embodies both the embedded derivative instrument and the host contract is not re-measured at fair value under
otherwise applicable generally accepted accounting principles with changes in fair value reported in earnings as they occur, and (c) a
separate instrument with the same terms as the embedded derivative instrument would be considered a derivative instrument. Professional
standards also provide an exception to this rule when the host instrument is deemed to be conventional as defined under professional standards
as The Meaning of Conventional Convertible Debt Instrument.
| F-17 | |
The Company accounts for convertible
instruments (when it has determined that the embedded conversion options should not be bifurcated from their host instruments) in accordance
with ASC 470-20 Debt Debt with Conversion and Other Options. Accordingly, the Company records, when necessary, discounts
to convertible notes for the intrinsic value of conversion options embedded in debt instruments based upon the differences between the
fair value of the underlying Common Stock at the commitment date of the note transaction and the effective conversion price embedded in
the note. Original issue discounts (*OID*) under these arrangements are amortized over the term of the related debt
to their earliest date of redemption. The Company also records, when necessary, deemed dividends for the intrinsic value of conversion
options embedded in preferred shares based upon the differences between the fair value of the underlying Common Stock at the commitment
date of the note transaction and the effective conversion price embedded in the note.
ASC 815-40 Derivatives
and Hedging Contracts in Entitys Own Equity provides that, among other things, generally, if an event occurs that
is not within the entitys control could or would require net cash settlement, then the contract shall be classified as an asset
or a liability.
*Variable Interest Entity (VIE) Accounting*
**
The Company evaluates its ownership,
contractual relationships and other interests in entities to determine the nature and extent of the interests, whether such interests
are variable interests and whether the entities are VIEs in accordance with ASC 810, Consolidations. These evaluations can be complex
and involve Management judgment as well as the use of estimates and assumptions based on available historical information, among other
factors. Based on these evaluations, if the Company determines that it is the primary beneficiary of a VIE, the entity is consolidated
into the financial statements. At December 31, 2024 and 2023, the Company identified EdgePoint to be the Companys sole VIE. At
December 31, 2024, and 2023, the Companys ownership percentage of EdgePoint was 29% each, respectively. The VIEs net assets
were less than approximately $0.1 million at December 31, 2024 and 2023, respectively.
*Investments - Equity Method*
**
The Company accounts for equity
method investments at cost, adjusted for the Companys share of the investees earnings or losses, which are reflected in
the consolidated statements of operations. The Company periodically reviews the investments for other than temporary declines in fair
value below cost and more frequently when events or changes in circumstances indicate that the carrying value of an asset may not be recoverable.
The Investment in GMP Bio represents the investment into equity securities for which the Company elected the fair value option pursuant
to ASC 825-10-15 and subsequent fair value changes in the GMP Bio shares shall be included in the result from other income. Refer to Note
6 to these Notes to the Consolidated Financial Statements.
*Joint Venture agreement*
**
We have equity interest in unconsolidated
arrangement that is primarily engaged in the business of drug discovery, development, and commercialization, including but not limited
to development and commercialization of TGF-beta therapeutics as well as establishing and operating contract development and manufacturing
organization (*CDMO*) facilities and capabilities. The Company first reviews the arrangement to determine if it meets
the definition of an accounting joint venture pursuant to ASC 323-10-20. In order to meet the definition of a joint venture, the arrangement
must have all of the following characteristics, (i) the arrangement is organized within a separate legal entity, (ii) the entity is under
the joint control of the venturers, (iii) the venturers must be able to exercise joint control through their equity investments, (iv)
the qualitative characteristics of the entity, including its purpose and design must be consistent with the definition of a joint venture.
We consolidate arrangements that
are considered to be VIEs where we are the primary beneficiary. We analyze our investments in joint ventures to determine if the joint
venture is considered a VIE and would require consolidation. We (i) evaluate the sufficiency of the total equity investment at risk, (ii)
review the voting rights and decision-making authority of the equity investment holders as a group and whether there are limited partners
(or similar owning entities) that lack substantive participating or kick out rights, guaranteed returns, protection against losses, or
capping of residual returns within the group and (iii) establish whether activities within the venture are on behalf of an investor with
disproportionately few voting rights in making this VIE determination.
| F-18 | |
To the extent that we own interests
in a VIE and we (i) have the power to direct the activities that most significantly impact the economic performance of the VIE and (ii)
have the obligation or rights to absorb losses or receive benefits that could potentially be significant to the VIE, then we would be
determined to be the primary beneficiary and would consolidate the VIE. To the extent that we own interests in a VIE, then at each reporting
period, we re-assess our conclusions as to which, if any, party within the VIE is considered the primary beneficiary.
To the extent that our arrangements
do not qualify as VIEs, they are consolidated if we control them through majority ownership interests or if we are the managing entity
(general partner or managing member) and our partner does not have substantive participating rights. Control is further demonstrated by
our ability to unilaterally make significant operating decisions, refinance debt, and sell the assets of the joint venture without the
consent of the non- managing entity and the inability of the non-managing entity to remove us from our role as the managing entity.
We use the equity method of accounting
for those arrangements where we exercise significant influence but do not have control. Under the equity method of accounting, our investment
in each arrangement is included on our consolidated balance sheet; however, the assets and liabilities of the joint ventures for which
we use the equity method are not included on our consolidated balance sheet. When we sell or contribute properties to unconsolidated arrangements
and retain a non-controlling ownership interest in such assets, we recognize the difference between the consideration received and the
carrying amount of the asset sold or contributed when its derecognition criteria are met. The equity method investment we retain in such
partial sale transactions is noncash consideration and is measured at fair value. As a result, the accounting for a partial sale will
result in the recognition of a full gain or loss.
When circumstances indicate there
may have been a reduction in the value of an equity investment, we evaluate whether the loss in value is other than temporary. If we conclude
it is other than temporary, we recognize an impairment charge to reflect the equity investment at fair value.
The Company elected the fair value
option under the fair value option Subsection of Section 825-10-15 to account for its equity-method investment as the Company believes
that the fair value option is most appropriate for a company in the biotechnology industry, The fair value option is more appropriate
for companies that are involved in extensive and usually very expensive research and development efforts, which are not appropriately
reflected in the market value or reflective of the true value of the development activities of the Company.
*Embedded debt costs in convertible debt instruments*
**
In August 2020, the FASB issued
ASU 2020-06, Debt with Conversion and Other Options (Subtopic 470-20) and Derivatives and HedgingContracts in Entitys
Own Equity (Subtopic 815-40) (*ASU 2020-06*) which simplifies the accounting for convertible instruments. The
guidance removes certain accounting models which separate the embedded conversion features from the host contract for convertible instruments.
Either a modified retrospective method of transition or a fully retrospective method of transition was permissible for the adoption of
this standard. Update No. 2020-06 is effective for fiscal years beginning after December 15, 2021, including interim periods within those
fiscal years. Early adoption was permitted no earlier than the fiscal year beginning after December 15, 2020. The Company adopted ASU
2020-06 effective January 1, 2023 and has removed the effects of any embedded conversion features from certain of our convertible instruments
as of that date.
*Revenue Recognition*
**
The Company recognizes revenue
in accordance with ASC Topic 606, Revenue from Contracts with Customers.
Under ASC 606, the Company recognizes
revenue when its customers obtain control of the promised good or services, in an amount that reflects the consideration which the Company
expects to receive in exchange for those goods or services. The Company applies the following five-step process: (i) identify the contract(s)
with a customer; (ii) identify the performance obligation(s) in the contract; (iii) determine the transaction price; (iv) allocate the
transaction price to the performance obligation(s) in the contract; and (v) recognize revenue when (or as) the Company satisfies a performance
obligation.
| F-19 | |
At contract inception, once the
contract is determined to be within the scope of ASC 606, the Company identifies the performance obligation(s) in the contract by assessing
whether the goods or services promised within each contract are distinct. The Company then recognizes revenue for the amount of the transaction
price that is allocated to the respective performance obligation when (or as) the performance obligation is satisfied.
The Company does not anticipate
generating revenues from rendering services to other third party customers for the development of certain drug products and/or in connection
with certain out-licensing agreements, at least in the near future. In the case of services rendered for development of the drugs, revenue
is recognized upon the achievement of the performance obligations or over time on a straight-line basis over the extended service period.
In the case of out-licensing contracts, the Company records revenues either (i) upon achievement of certain pre-defined milestones when
there is no obligation of the Company achieve any performance obligations in connection with the said pre-defined milestones, or (ii)
upon achievement of the performance obligations if the milestones require the Company to provide the performance obligations.
The Company may occasionally collect
advance payments from customers toward commitments to provide services or performance obligations, in which case the advance payment is
recorded as a liability until the obligations are fulfilled and revenue is recognized.
*Research & Development Costs*
**
In accordance with ASC 730-10-25
Research and Development, research and development costs are charged to expense as and when incurred.
*Recent Accounting Pronouncements*
**
In August 2020, the FASB issued
ASU 2020-06, Debt with Conversion and Other Options (Subtopic 470- 20) and Derivatives and HedgingContracts in Entitys
Own Equity (Subtopic 815-40) (*ASU 2020-06*) which simplifies the accounting for convertible instruments. The
guidance removes certain accounting models which separate the embedded conversion features from the host contract for convertible instruments.
Either a modified retrospective method of transition or a fully retrospective method of transition was permissible for the adoption of
this standard. Update No. 2020-06 is effective for fiscal years beginning after December 15, 2023, including interim periods within those
fiscal years. Early adoption was permitted no earlier than the fiscal year beginning after December 15, 2020.The Company adopted ASU 2020-06
effective January 1, 2023 and recorded approximately $0.5 million as a reduction to the additional paid in capital and added approximately
$0.3 million to the opening retained earnings in accordance with the authoritative guidance under ASU 2020-06.
All other newly issued but not
yet effective accounting pronouncements have been deemed to be not applicable or immaterial to the Company.
**NOTE 3 ACQUISITIONS, GOODWILL AND INTANGIBLE ASSETS**
****
*Goodwill from 2019 Reverse Merger with Oncotelic and Merger with PointR*
**
The Company completed the reverse
merger with Oncotelic Inc. (Merger) in April 2019. The Company completed the merger with PointR Data Inc (PointR
Merger) in November 2019. For more details on the two mergers, refer to our 2020 Annual Report on Form 10-K for the year ended
December 31, 2020 filed by the Company on April 15, 2021.
The Oncotelic merger gave rise
to Goodwill of approximately $4.9 million. Upon the non-financial sale of our asset as contribution to our equity method investment, we
derecognized the balance of the carrying value of our goodwill of approximately $4.9 million from the Oncotelic Merger in accordance with
our policy and authoritative accounting guidance.
Further, we added goodwill of
$16,182,456 upon the completion of the Merger with PointR.
| F-20 | |
We have one operating segment
and reporting unit. Accordingly, our review of goodwill impairment indicators was performed at the entity-wide level. In performing our
annual impairment assessment, we determined if we should qualitatively assess whether it was more likely than not the fair value of goodwill
was less than its carrying amount (the qualitative impairment test). The factors we considered in the assessment included our market capitalization,
general macroeconomic conditions, conditions specific to the industry and market and whether there had been sustained declines in our
share price. If we concluded, it was more likely than not, the fair value of the reporting unit was less than its carrying amount, or
elected not to use the qualitative impairment test, a quantitative impairment test would be performed.
We used our market capitalization
as an indicator of fair value. While we believe the fair value measurement need not be based solely on the quoted market price of an individual
share of our Common Stock, and that we also could consider the impact of a control premium in measuring the fair value of its reporting
unit. In the absence of any other valuation metrics, the Company believed using a control premium utilized would not be appropriate under
the current circumstances. We also considered some other market comparables, trends in our stock price as well as the industry over a
period of two successive quarters and prospective quarter to evaluate whether the fair value of our reporting unit was greater than our
carrying amount. As such, we performed a quantitative impairment assessment of goodwill for our single reporting unit at the end of 2024
and 2023, due to a sustained change in our market capitalization and an increase in negative economic outlook for biotech markets. We
estimated and reconciled the fair value of our reporting unit utilizing our market capitalization based on the stock price of our Common
Stock as of December 31, 2024 and 2023. Before completing our goodwill impairment test, we first tested our indefinite-lived intangible
asset then our remaining long-lived assets for impairment. We concluded our indefinite-lived intangible assets were not impaired. Based
on the market capitalization, we further concluded the fair value of our single reporting unit was less than its carrying value and therefore
recognized an impairment charge of approximately $3.2 million and approximately $6.1 million during the year ended December 31, 2024 and
2023. The calculation of the impairment charge included substantial fact-based determinations and estimates. The goodwill impairment charge
is reflected as goodwill impairment in the consolidated statements of operations for the year ended December 31, 2024.
A summary of our goodwill as of
December 31, 2024 and 2023 is shown below:
SCHEDULE OF GOODWILL
| 
| | 
December 31, 
2024 | | | 
December 31, 
2023 | | |
| 
Balance at January 1, 2024 and 2023 | | 
$ | 5,988,230 | | | 
$ | 12,071,376 | | |
| 
Less: Goodwill impairment due to market capitalization | | 
| (3,200,000 | ) | | 
| (6,083,146 | ) | |
| 
Balance at December 31, 2024 and 2023 | | 
$ | 2,788,230 | | | 
$ | 5,988,230 | | |
In general, the goodwill is tested
on an annual impairment date of December 31, unless we observe any further deterioration in our market capitalization, in which case we
may, depending on the materiality of the impairment, record an impairment at the end of other reporting periods, as we have done during
the course of the year ended December 31, 2024.
*In-Process Research & Development (IPR&D) Summary*
**
The IPR&D assets were acquired
in the PointR Merger during the year ended December 31, 2019. Since January 2021, the Company has determined that the IPR&D should
be reported as an indefinitely lived asset and therefore will evaluate, on an annual basis, for any impairment on the IPR&D and will
record an impairment if identified. The balance of IPR&D as of December 31, 2024 and December 31, 2023 was $1,101,760. For more information
on the IPR&D, please refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
| F-21 | |
****
**NOTE 4 ACCOUNTS PAYABLE AND ACCRUED EXPENSES**
Accounts payable and accrued expense consists of the following amounts:
SCHEDULE
OF ACCOUNTS PAYABLE AND ACCRUED EXPENSES
| 
| | 
December 31,
2024 | | | 
December 31,
2023 | | |
| 
Accounts payable | | 
$ | 1,691,725 | | | 
$ | 1,656,613 | | |
| 
Accrued expenses | | 
| 745,442 | | | 
| 780,708 | | |
| 
Accounts payable and
accrued liabilities | | 
$ | 2,437,167 | | | 
$ | 2,437,321 | | |
| 
| | 
December 31, 
2024 | | | 
December 31, 
2023 | | |
| 
Accounts payable related party | | 
$ | 346,057 | | | 
$ | 344,099 | | |
****
**NOTE 5 CONVERTIBLE DEBENTURES, NOTES AND OTHER DEBT**
****
As of December 31, 2024, special
purchase agreements (SPAs) with convertible debentures and notes, net of debt discount and including accrued interest, if any, consist
of the following amounts:
SCHEDULE
OF CONVERTIBLE DEBENTURES AND NOTES, NET OF DISCOUNT
| 
| | 
December 31, 
2024 | | | 
December 31, 
2023 | | |
| 
Current Debt | | 
| | | | 
| | | |
| 
Convertible debentures | | 
| | | | 
| | | |
| 
10% Convertible note payable, due April 23, 2022 Bridge Investor | | 
$ | 35,556 | | | 
$ | 35,556 | | |
| 
10% Convertible note payable, due April 23, 2022 Related Party | | 
| 164,444 | | | 
| 164,444 | | |
| 
10% Convertible note payable, due August 6, 2022 Bridge Investor | | 
| 200,000 | | | 
| 200,000 | | |
| 
Convertible note payable | | 
| 400,000 | | | 
| 400,000 | | |
| 
Fall 2019 Notes | | 
| | | | 
| | | |
| 
5% Convertible note payable Stephen Boesch | | 
| 133,958 | | | 
| 128,958 | | |
| 
5% Convertible note payable Related Party | | 
| 313,733 | | | 
| 301,233 | | |
| 
5% Convertible note payable Dr. Sanjay Jha (Through his family trust) | | 
| 313,253 | | | 
| 300,753 | | |
| 
5% Convertible note payable CEO & CFO Related Parties | | 
| 102,659 | | | 
| 98,559 | | |
| 
5% Convertible note payable Bridge Investors | | 
| 210,322 | | | 
| 201,922 | | |
| 
Convertible note payable | | 
| 1,073,925 | | | 
| 1,031,425 | | |
| 
August 2021 Convertible Notes | | 
| | | | 
| | | |
| 
5% Convertible note Autotelic Inc Related Party | | 
| 292,552 | | | 
| 280,052 | | |
| 
5% Convertible note Bridge investors | | 
| 437,075 | | | 
| 418,399 | | |
| 
5% Convertible note CFO Related Party | | 
| 87,770 | | | 
| 84,018 | | |
| 
Convertible note payable | | 
| 817,397 | | | 
| 782,469 | | |
| 
JH Darbie PPM Debt | | 
| | | | 
| | | |
| 
16% Convertible Notes Non-related parties | | 
| - | | | 
| 311,693 | | |
| 
Convertible note payable | | 
| - | | | 
| 311,693 | | |
| 
| | 
| | | | 
| | | |
| 
November/December 2021 & March 2022 Notes | | 
| | | | 
| | | |
| 
16% Convertible Notes Accredited Investors | | 
| 233,687 | | | 
| 233,392 | | |
| 
| | 
| | | | 
| | | |
| 
Debt for Clinical Trials Forever Prosperity ( Formerly GMP) | | 
| | | | 
| | | |
| 
2% Convertible Notes Forever Prosperity | | 
| 4,840,247 | | | 
| 4,750,000 | | |
| 
| | 
| | | | 
| | | |
| 
May and June 2022 Note | | 
| | | | 
| | | |
| 
16% Convertible Notes Accredited Investors | | 
| 993,130 | | | 
| 1,401,284 | | |
| 
| | 
| | | | 
| | | |
| 
JH Darbie PPM 2 Debt | 
| 
| 
| 
| 
| 
| 
| 
| |
| 
16% Convertible Notes - Non-related parties | 
| 
| 
2,183,638 | 
| 
| 
| 
- | 
| |
| 
16% Convertible Notes CEO Related Party | 
| 
| 
125,000 | 
| 
| 
| 
- | 
| |
| 
Convertible
note payable | 
| 
| 
2,308,638 | 
| 
| 
| 
- | 
| |
| 
Other Debt | | 
| | | | 
| | | |
| 
Short term debt Bridge investors | | 
| 210,000 | | | 
| 210,000 | | |
| 
Short term debt from CFO Related Party | | 
| 76,050 | | | 
| 35,050 | | |
| 
Short term debt Autotelic Inc. Related Party | | 
| 2,085,000 | | | 
| 1,470,000 | | |
| 
Short Term Debt from CEO Related Party | | 
| 50,000 | | | 
| 50,000 | | |
| 
Short term debt | | 
| 2,421,050 | | | 
| 1,765,050 | | |
| 
Total of short term convertible debentures & notes and other debt | | 
$ | 13,088,074 | | | 
| 10,675,313 | | |
| F-22 | |
| 
| | 
December 31, 
2024 | | | 
December 31, 
2023 | | |
| 
| | 
| | 
| |
| 
Long Term Debt | | 
| | | | 
| | | |
| 
JH Darbie PPM 2 Debt | | 
| | | | 
| | | |
| 
16% Convertible Notes - Non-related parties | | 
| - | | | 
| 1,773,468 | | |
| 
16% Convertible Notes CEO Related Party | | 
| - | | | 
| 125,000 | | |
| 
Convertible note payable | | 
| - | | | 
| 1,898,468 | | |
*Convertible Debentures*
**
As of December 31, 2024, the Company
had a derivative liability of approximately $704,000 and recorded a change in fair value of approximately $280,000 during the year ended
December 31, 2024, on the Convertible Debentures issued in 2019 to our CEO and a bridge investor.
*Bridge Financing*
**
**Notes with Officer and Bridge Investor**
****
In April 2019, the Company entered
into a Securities Purchase Agreement (the *Bridge SPA*) with our CEO (the *Trieu Note*) and a Bridge
Investor with a commitment to purchase convertible notes in the aggregate of $400,000. For more information on the Bridge SPA, refer to
our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
The issuance of the Trieu Note
resulted in a discount from the beneficial conversion feature totaling $131,555 related to the conversion feature. Total amortization
of the OID and the discount totaled $0 and approximately for the years ended December 31, 2024, and 2023, respectively. Total unamortized
discount on this note was approximately $0 as of December 31, 2024, and 2023, respectively.
In April 2019, pursuant to the
Bridge SPA the Company entered into Convertible Note Tranche #1 (*Tranche #1*) with the Bridge Investor. For more information
on Tranche #1, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
The issuance of the note resulted
in a discount from the beneficial conversion feature totaling $28,445. Total amortization of the OID and discount totaled approximately
$0 for the year ended December 31, 2024, and 2023, respectively. Total unamortized discount on this note was approximately $0
as of December 31, 2024, and December 31, 2023.
In August 2019, pursuant to the
Bridge SPA the Company entered into Convertible Note Tranche #2 (*Tranche #2*) with the Bridge Investor. For more information
on Tranche #2, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
The issuance of the note resulted
in a discount from the beneficial conversion feature totaling $175,000. Total amortization of the OID and discount totaled approximately
$0 for the years ended December 31, 2024, and 2023, respectively. Total unamortized discount on this note was $0 as of December 31, 2024,
and 2023.
| F-23 | |
*Fall 2019 Debt Financing*
**
In December 2019, the Company
closed its Fall 2019 Debt Financing, raising an additional $500,000 bringing the gross proceeds of all debt financings under the Fall
2019 Debt Financing to $1,000,000. The Company entered into those certain Note Purchase Agreements (the *Fall 2019 Note Purchase
Agreements*) with certain accredited investors and the officers of the Company for the sale of convertible promissory notes
(the *Fall 2019 Notes*). The Company completed the initial closing under the Fall 2019 Note Purchase Agreements in
November 2019. The Company issued Fall 2019 Notes in the principal amount of $250,000 to each of Dr. Vuong Trieu, the Companys
Chief Executive Officer, and Stephen Boesch, in exchange for gross proceeds of $500,000. In connection with the second and final closing
of the Fall 2019 Debt Financing, the Company issued Fall 2019 Notes to additional investors including $250,000 to Dr. Sanjay Jha, through
his family trust, the former CEO of Motorola and COO/President of Qualcomm. The Company also offset certain amounts due to Dr. Vuong Trieu,
the Companys Chief Executive Officer, Chulho Park, the Companys then Chief Technology Officer, and Amit Shah, the Companys
Chief Financial Officer, all related parties as Officers of the Company, and converted such amounts due into the Fall 2019 Notes. $35,000
due to Dr. Vuong Trieu, $27,000 due to Chulho Park and $20,000 due to Amit Shah were converted into convertible debt under the Fall 2019
Notes. The Company also issued the Fall 2019 Notes of $168,000 to two accredited investors.
All the Fall 2019 Notes provided
for interest at the rate of 5% per annum and are unsecured. For more information on the Fall 2019 Debt Financing, refer to our 2023 Annual
Report on Form 10-K filed with the SEC on April 12, 2024.
There was no activity during the
year ended December 31, 2024 and 2023.The total unamortized principal amount of the Fall 2019 Notes was $850,000 as of December 31, 2024,
and 2023.
Further, the Company recorded interest expense of
approximately $42,500 on these Fall 2019 Notes for the years ended December 31, 2024, and 2023. The total amount outstanding under the
Fall 2019 Notes, net of discounts and including accrued interest thereon, as of December 31, 2024, and 2023 was approximately $1,073,900
and $1,031,400 respectively.
*Forever Prosperity (Formerly GMP) Notes*
**
In June 2020, the Company secured
$2 million in debt financing, evidenced by a one-year convertible note (the *GMP Note*) from GMP, to conduct a clinical
trial evaluating OT-101 against COVID-19 bearing 2% annual interest, and is personally guaranteed by Dr. Vuong Trieu, the Chief Executive
Officer of the Company. The GMP Note is convertible into the Companys Common Stock upon the GMP Notes maturity of the GMP
Note, at the Companys Common Stock price on the date of conversion with no discount. GMP has waived the default in the maturity
of the GMP Note and as such there is no event of default and also agreed to extend the date of maturity of the GMP Note to December 31,
2024. GMP does not have the option to convert prior to the GMP Notes maturity. Such financing will be utilized solely to fund the
clinical trial. The Companys liability under GMP Note commenced to accrue when GMP first began to pay for services related to the
clinical trial to our third-party clinical research organization, up to a maximum of $2 million. GMP has been invoiced by the clinical
research organization for the full $2 million as of December 31, 2024, and as such the Company has recognized the liability as a convertible
debt.
In September 2021, the Company
secured a further $1.5
million in debt financing, evidenced by a one-year convertible note (the *GMP Note 2*) from GMP, to fund the same
clinical trial evaluating OT-101 against COVID- 19 bearing 2%
annual interest. The GMP Note is convertible into the Companys Common Stock upon the GMP Note 2s maturity one year from
the date of the GMP Note 2, at the Companys Common Stock price on the date of conversion with no discount. GMP has waived the
default in the maturity of the GMP Note and as such there is no event of default and also agreed to extend the date of maturity of the
GMP Note to December 31, 2024. GMP does not have the option to convert prior to the GMP Note 2s maturity at the end of one year.
Such financing was to be utilized solely to fund the clinical trial. GMP was invoiced by the clinical research organization for $1.5
million.
| F-24 | |
In October 2021, the Company entered
into an Unsecured Convertible Note Purchase Agreement (the *October Purchase Agreement*) with GMP, pursuant to which
the Company issued a convertible promissory note in the aggregate principal amount of $0.5 million (the *October 2021 Note*),
which October 2021 Note is convertible into shares of the Companys Common Stock. GMP has waived the default in the maturity of
the GMP Note and as such there is no event of default and also agreed to extend the date of maturity of the GMP Note to December 31, 2024.
In January 2022, the Company entered
into an Unsecured Convertible Note Purchase Agreement (the *January Purchase Agreement*) with GMP, pursuant to which
the Company issued a convertible promissory note in the aggregate principal amount of $0.5 million (the *January 2022 Note*),
which January 2022 Note is convertible into shares of the Companys Common Stock. GMP agreed to extend the date of maturity of the
January 2022 Note to December 31, 2024.
Cumulatively,
the GMP Note, GMP Note 2, October 2021 Note and the January 2022 Notes are referred to as the *GMP Notes*. The GMP
Notes carry an interest rate of 2%
per annum and mature on the earlier of (a) the one- year anniversary of the date of the Purchase Agreement, or (b) the acceleration of
the maturity by GMP upon occurrence of an Event of Default (as defined below). All Notes contain a voluntary conversion mechanism whereby
GMP may convert the outstanding principal and accrued interest under the terms of all the GMP Notes into shares of Common Stock (the
*Conversion Shares*), at the consolidated closing bid price of the Companys Common Stock on the applicable
OTC Market as of the date the Company receives a Notice of Conversion from GMP. Prepayment of the GMP Notes may be made at any time by
payment of the outstanding principal amount plus accrued and unpaid interest. The October Note contained customary events of default
(each an *Event of Default*). If an Event of Default occurred, at GMPs election, the outstanding principal amount
of the GMP Notes, plus accrued but unpaid interest, would become immediately due and payable in cash. The October Purchase Agreement
required the Company to use of the proceeds received under the October 2021 Note to support the clinical development of OT-101, including
payroll and had been made in continuation of the relationship between the Company and GMP. All the GMP notes were assigned to Forever
Prosperity, LLC, an affiliated entity of GMP. As of January 1, 2025, the GMP Notes are in default. The total principal outstanding on
all the GMP notes, inclusive of accrued interest, was approximately $4.8
million as of December 31, 2024 and 2023, respectively.
During the years ended December
31, 2024 and 2023, the Company incurred approximately $90,000 of interest expense.
*August 2021 Notes*
**
In August 2021, the Company entered
into Note Purchase Agreements with Autotelic - a related party, our CFO a related party, and certain accredited investors (the
August 2021 investors), whereby the Company issued four convertible notes in the aggregate principal amount of $698,500
convertible into shares of common stock of the Company for net proceeds of approximately $691,000. The convertible notes carry a five
(5%) percent coupon and mature one year from issuance. The majority of the August 2021 investors have the right, but not the obligation,
not more than five days following the maturity date, to convert all, but not less than all, the outstanding and unpaid principal plus
accrued interest into the Companys common stock, at a conversion price of $0.18. The August 2021 Note Holders has waived the default
in the maturity of the August 2021 Notes and as such there is no event of default and also agreed to extend the date of maturity of the
August 2021 Notes to December 31, 2025. The Company determined that the economic characteristics and risks of the embedded conversion
option are not clearly and closely related to the economic characteristics and risks of the debt host instrument. Further, the Company
determined that the embedded conversion feature meets the definition of a derivative but met the scope exception to the derivative accounting
required under ASC 815 for certain contracts involving a reporting entitys own equity.
As of December 31, 2024 and 2023,
the August 2021 convertible notes, net of debt discount, consist of the following amounts:
SCHEDULE
OF CONVERTIBLE NOTES, NET OF DISCOUNT
| 
| | 
December 31, | | | 
December 31, | | |
| 
| | 
2024 | | | 
2023 | | |
| 
Autotelic Related party convertible note, 5% coupon December 2024 | | 
$ | 292,552 | | | 
$ | 280,052 | | |
| 
CFO Related party convertible note, 5% coupon December 2024 | | 
| 87,770 | | | 
| 84,018 | | |
| 
Accredited investors convertible note, 5% coupon December 2024 | | 
| 437,075 | | | 
| 418,399 | | |
| 
Convertible notes | | 
$ | 817,397 | | | 
$ | 782,469 | | |
| F-25 | |
During the years ended December
31, 2024 and 2023 the Company recognized approximately $35,000 of interest expense on the August 2021 Investors notes of which approximately
$16,000 are attributable to related parties.
At December 31, 2024, and 2023,
accrued interests on these convertible notes totaled approximately $119,000 and $84,000, respectively.
The outstanding balance on the
note for the year ended December 31, 2024 was approximately $817,000 including related party balance of approximately $380,000. The outstanding
balance on the note for the year ended December 31, 2023 was approximately $782,000 including related party balance of $364,000.
*November / December 2021 and March 2022 Financing*
**
In November / December 2021, the
Company entered into securities purchase agreement with five institutional investors, whereby the Company issued five convertible notes
in the aggregate principal amount of $1,250,000 convertible into shares of common stock of the Company. The convertible notes carry a
twelve (12%) percent coupon and a default coupon of 16% and mature at the earliest of one year from issuance or upon event of default.
Investors has the right at any time following issuance date to convert all or any part of the outstanding and unpaid amount of the note
into the Companys common stock at a conversion price established at a fixed rate of $0.07. The Company granted a total number of
9,615,385 warrants convertible into an equivalent number of the Company Common Stock at a strike price of $0.13 up to five years after
issuance. The Placement agent was also granted a total of 961,540 warrants convertible into an equivalent number of the Company Common
Stock at a strike price of $0.13 up to five years after issuance, as part of a finders fee agreement.
Further, in March 2022, the Company
entered into a Securities Purchase Agreement with Fourth Man, pursuant to which the Company issued convertible promissory note in the
aggregate principal amount of $0.25 million, convertible into shares of common stock of the Company. The convertible notes carry a twelve
(12%) percent coupon and a default coupon of 16% and mature at the earliest of one year from issuance or upon event of default. As of
December 31, 2022, this note is in Investors have the right at any time following issuance date to convert all or any part of the outstanding
and unpaid amount of the note into the Companys Common Stock at a conversion price established at a fixed rate of $0.10. The Company
granted a total number of 1,250,000 warrants convertible into an equivalent number of the Company common shares at a strike price of $0.20
up to five years after issuance. The Placement agent was also granted a total of 125,000 warrants convertible into an equivalent number
of the Company Common Stock at a strike price of $0.20 up to five years after issuance, as part of a finders fee agreement.
During the year ended December
31, 2023, the Company converted the balance of approximately $243,000 of Blue Lake convertible note, inclusive of accrued interest, into
3,466,583 shares of the Companys Common Stock, which fully retired the convertible note as of December 31, 2023. Further, during
the year ended December 31, 2023, the Company fully converted the balance of Fourth Man convertible note of approximately $127,000 into
1,820,395 shares of the Companys common stock, which fully retired the convertible note as of December 31, 2023.
As of December 31, 2024, all
of the November- December 2021 notes and any accrued interest, are fully converted.
As of December 31, 2024, and
December 31, 2023, the Fourth Man convertible note, net of debt discount, consist of the following amounts:
| 
| | 
December 31,
2024 | | | 
December 31,
2023 | | |
| 
Fourth Man Convertible note, 16% coupon March 2023 inclusive of accrued interest and default provision | | 
$ | 233,687 | | | 
$ | 233,392 | | |
| 
Unamortized debt discount | | 
| - | | | 
| - | | |
| 
Convertible notes, net | | 
$ | 233,687 | | | 
| 233,392 | | |
| F-26 | |
The March 2022 Fourth Man Financing
principal balance was approximately $142,000 and $162,000 as of December 31, 2024, and December 31, 2023, respectively.
During the year ended December
31, 2024, the Company converted approximately $35,000 in principal, accrued interest and legal fees into 500,000 shares of common stock.
The note includes a default amount calculated at 125% of the unpaid principal and accrued interest. As the Company failed to repay the
note at the original maturity date, The Company has recorded an estimated default penalty of approximately $70,000.
As of December 31, 2024, the balance
includes the remaining principal of $142,000 and $70,000 of accrued default penalty pursuant to the terms of the underlying agreement.
The Company recognized approximately
$34,000 and $25,000 of interest during the years ended December 31, 2024 and 2023.
As of December 31, 2024 and 2023,
the balance of the unamortized debt discount was $0. The Company adopted ASU 2020-06 on January
1, 2023, which resulted in the reversal of the original BCF amount to additional paid in capital for $109,349, reversal of the unamortized
debt discount related to the BCF for $25,489with the balance being recorded through retained earnings for $78,460.
*May 2022 Mast Financing*
**
In May 2022, the Company entered
into a securities purchase agreement with one institutional investor, whereby the Company issued one convertible note in the aggregate
principal amount of $605,000 convertible into shares of common stock of the Company (May 2022 Mast Note). The convertible
notes carry a twelve (12%) percent coupon and a default coupon of 16% and mature at the earliest of one year from issuance or upon event
of default. Investor has the right at any time following issuance date to convert all or any part of the outstanding and unpaid amount
of the note into the Companys common stock at a conversion price established at a fixed rate of $0.10. The Company granted a total
number of 3,025,000 warrants convertible into an equivalent number of Company common shares at a strike price of $0.20 up to five years
after issuance. The Placement agent was also granted a total of 302,500 warrants convertible into an equivalent number of the Company
Common Stock at a strike price of $0.20 up to five years after issuance, as part of a finders fee agreement. A portion of the proceeds
were used to retire some of the November/December 2021 notes.
As of December 31, 2024, and December
31, 2023, convertible note under the May 2022 Mast Financing, net of debt discount, consist of the following amounts:
| 
| | 
December 31,
2024 | | | 
December 31,
2023 | | |
| 
Mast Hill Convertible note, 12% coupon May 2025, inclusive of accrued interest and penalty | | 
$ | 993,130 | | | 
$ | 905,484 | | |
| 
Convertible notes, net | | 
$ | 993,130 | | | 
$ | 905,484 | | |
The Mast Hill Note of $993,130
as of December 31, 2024 includes $605,000 of principal, $169,400 in default penalty, and approximately $219,000 in accrued interest.
Accrued interest was approximately
$219,000 and $131,000 as of December 31, 2024 and 2023, respectively. The May 2022 Mast Note was extended through May 2025 at a cost
of approximately $82 thousand, and which is included in the amount outstanding and payable to Mast as of December 31, 2024.
The Company recognized approximately
$0 and approximately $146,000 of interest expense attributable to the amortization of the debt discount from the original debt discount,
deferred financing costs, fair value allocated to the warrants during the years ended December 31, 2024 and 2023, respectively.
Effective January 1, 2023, the
Company adopted ASU 2020-06, which resulted in the reversal of the original BCF amount to additional paid in capital for approximately
$0.2million, a reversal of the unamortized debt discount related to the BCF for approximately $0.1million, with the balance
of approximately $0.1million being recorded through retained earnings.
| F-27 | |
*June 2022 Blue Lake Financing*
**
In June 2022, the Company entered
into a securities purchase agreement with one institutional investor, whereby the Company issued one convertible note in the aggregate
principal amount of $335,000 convertible into shares of common stock of the Company (June 2022 Blue Lake Note). The convertible
notes carry a twelve (12%) percent coupon and a default coupon of 16% and mature at the earliest of one year from issuance or upon event
of default. The investor has the right at any time following issuance date to convert all or any part of the outstanding and unpaid amount
of the note into the Companys common stock at a conversion price established at a fixed rate of $0.10. The Company granted a total
number of 837,500 warrants convertible into an equivalent number of the Company common shares at a strike price of $0.20 up to five years
after issuance. The Placement agent was also granted a total of 83,750 warrants convertible into an equivalent number of the Company Common
Stock at a strike price of $0.20 up to five years after issuance, as part of a finders fee agreement. A portion of the proceeds
were used to retire some of the November/December 2021 notes.
In May 2024, Blue Lake converted
the balance of their note of approximately $531,000 including principal, accrued interest and default penalty, into 7,605,760 common shares
of the Company
As of December 31, 2024 and 2023,
convertible note under the June 2022 Blue Lake Financing, net of debt discount, consist of the following amounts:
| 
| | 
December 31, 
2024 | | | 
December 31, 2023 | | |
| 
| | 
| | | 
| | |
| 
Blue Lake Convertible note, 16% coupon June 2023, inclusive of accrued interest | | 
$ | - | | | 
$ | 495,800 | | |
| 
Convertible notes, net | | 
$ | - | | | 
$ | 495,800 | | |
The Company
recognized approximately $35,000 and $88,400 of interest expense attributable to interest, amortization of the debt discount from the
original debt discount, deferred financing costs, fair value allocated to the warrants and the beneficial conversion feature during the
years ended December 31, 2024 and 2023, respectively. The Company recognized approximately $0 and approximately $62,000 of interest expense
attributable to the amortization of the debt discount from the original debt discount, deferred financing costs, fair value allocated
to the warrants and BCF during the years ended December 31, 2024 and 2023.
The Company recognized $35,000 and
approximately $40,200 of interest expense related to the guaranteed coupon for the years ended December 31, 2024 and 2023, respectively.
The Company adopted ASU 2020-06
effective January 1, 2023, which resulted in the reversal of the original BCF amount to additional paid in capital of approximately $0.2
million, reversal of the unamortized debt discount of approximately $0.1 million related to the BCF and the balance of $0.1 million being
recorded through retained earnings.
*Other short-term advances*
**
As of December 31, 2024, other
short-term advances consist of the following amounts obtained from various employees and related parties:
SCHEDULE
OF SHORT-TERM LOANS
| 
Other Advances | | 
December 31, 2024 | | | 
December 31, 2023 | | |
| 
Short term advance from CFO Related Party | | 
$ | 76,050 | | | 
$ | 35,050 | | |
| 
Short term advance from CEO Related Party | | 
| 50,000 | | | 
| 50,000 | | |
| 
Short term advances bridge investors & others | | 
| 210,000 | | | 
| 210,000 | | |
| 
Short term advances Autotelic Inc. Related Party | | 
| 2,085,000 | | | 
| 1,470,000 | | |
| 
Short term advance | | 
$ | 2,421,050 | | | 
$ | 1,765,050 | | |
| F-28 | |
In May 2021, Autotelic provided
an additional short-term funding of approximately $0.3 million to the Company, which was converted into the August 2021 Notes. Autotelic
provided an additional $0.1 million short term loan to the Company during the year ended December 31, 2022. During the year ended December
31, 2023, Autotelic provided $1.4 million in various short-term loans to the Company. During the year ended December 31, 2024 Autotelic
Inc. provided additional short-term funding of $614,000 to the Company. As such, approximately $2.1 million was outstanding and payable
to Autotelic at December 31, 2024.
The Companys CFO was
owed approximately $25 thousand at December 31, 2022. During the year ended December 31, 2023, the companys CFO provided additional
short-term advance of $10 thousand. During the year ended December 31, 2024, the CFO provided additional short-term funding of $41 thousand.
As such, approximately $76 thousand was outstanding from the Companys CFO at December 31, 2024.
In December 2023, the Company
received $50 thousand from the companys CEO. As such, $50 thousand was outstanding to the Companys CEO at December 31, 2024.
As of December 31, 2024 and December
31, 2023, respectively, approximately $210,000 was outstanding as short-term advances from certain bridge investors.
**NOTE 6 - JOINT VENTURE WITH GMP BIO AND AFFILIATES,
EQUITY METHOD INVESTMENT**
****
On March 31, 2022, the Company
entered into (i) a joint venture (the *JV*) agreement with Dragon and GMP Bio, both affiliates of GMP, (and the Company,
Dragon and GMP Bio are collectively called the *Parties*) (the *JVA*), (ii) a license agreement
for rights to OT-101 (the *US License Agreement*) for the territory within the United States of America (the *US*)
with Sapu Holdings, LLC, a subsidiary of GMP Bio and (iii) a license agreement for rights to OT-101 for the rest of the world with GMP
Bio (the *Ex-US Rights Agreement*, and the US License Agreement and the Ex-US License Agreement are collectively called
the *Agreements*). For more information on the JV, JVA, and Agreements, refer to our 2022 Annual Report on Form 10-K/A
filed with the SEC on April 19, 2023.
As of the effective date of the
formation of the JV, the combined enterprise value of GMP Bio was approximately $50.4 million, comprising of the fair value of the Companys
investment in GMP Bio of approximately $22.7 million and the total original capital contributions by Dragon Overseas of approximately
$27.7 million. As of December 31, 2024, the JV had approximately $24.4 million in assets, recorded approximately $1.2 million in liabilities
and incurred approximately $9.2 million and $6.5 million in operational expenses for the years ended December 31, 2024 and 2023, respectively.
While GMPs fiscal year commences on April 1 and ends on March 31, the Company has reported the operational expenses for the same
fiscal period as the Company. The JV has determined to changing the fiscal year to an annual year and plans to do it soon.
In late 2023, the JV initiated
a plan to start evaluating various nanoparticles that could treat various cancers. In this regard, the JV identified a total of 4 compounds,
in addition to OT-101, which had the potential of significant revenue generation for the JV. In the same year, the JV signed a lease
agreement to set up a GMP manufacturing facility in San Diego (*SD*), California. The main purpose of this facility
was to initially commence an aggressive formulation development of newly planned nanoparticle platform (*Nano Platform*).
The GMP manufacturing facility was initiated in January 2024. Upon the initiation of this facility by the JV, the JV commenced the development
work on two of the four identified compounds, as well as other activities, in tandem with the development of OT-101. The JV has since
completed the formulation development of one of the products and is moving to complete the formulation development for the three additional
products. The JV is also working on improved formulations for OT-101 with new nanoparticle sizes. The JV also has started clinical development
for OT-101 for pancreatic cancer. Significant progress has been made in the development of the products and the JV anticipates to complete
the formulation development work in 2025 and pushing to initiate clinical trials for the various compounds. In late 2024, the GMP facility
in San Diego was issued a Drug Manufacturing License by the State of California Department of Public Health and Food and Drug Branch.
Further, in late 2024, the JV identified a sixth candidate as a compound for development for the JV and has already started to work on
the formulation development of that compound as well. All manufacturing including Phase 1 clinical trial materials will be performed
at the SD site.
Further, in late 2024, the
JV identified a sixth candidate as a compound for development for the JV and has already started to work on the formulation
development of that compound as well. In early 2025, the Company announced that it had entered into a strategic partnership with
Shanghai Medicilon, Inc. (*Medicilon*) to access its industry-leading rapid investigational new drug
(*IND*) development platform to support up to 20 IND projects, which the JV can also utilize to support their
INDS. All six of our compounds the JV is developing are planned to be these INDs and are focused on becoming next-generation
anticancer agents. The JV anticipates that all these six anticancer agents have the potential to become significant growth
contributors to the JV, which in turn would add substantial value to the Company. The Company successfully completed a Phase 1
clinical trial evaluating OT-101, in combination with IL-2 for advanced or metastatic solid tumors. These results set the stage for
new studies that combine OT-101, an antisense therapeutic targeting Transforming Growth Factor Beta 2 (TGF2), with checkpoint
inhibitors (CKIs) and recombinant IL-2 (aldesleukin) (IL-2). The Phase 1 trial (ClinicalTrials.gov ID:
NCT04862767) investigated the safety and tolerability of OT-101 in combination with recombinant IL-2 in patients with advanced or
metastatic solid tumors. The combination showed a tolerable safety profile at the planned dosing schedule, with no unexpected safety
signals identified. Based on the favorable safety data, Oncotelic plans to advance OT-101 plus IL-2 into further clinical studies,
exploring synergies with CKIs such as PD-1 blockers. The Company elected the fair value option under subsection of Section 825-10-15
to account for its equity-method investment as the Company believes that it the most appropriate method to properly value the
Company and record a change in value when and upon conducting a fair value assessment. During the year ended December 31, 2023, and
based on the results of the valuation study and the 45%
ownership of the Company in GMP Bio, the Company had reported a change in fair value of the Companys investment in the JV of
approximately $13,000
for the year December 31, 2023. As of December 31, 2024, as the operations of the JV are proceeding as planned, the Company assessed
the fair value of its investment in the JV and determined that no change in the fair value is required until a triggering event has
occurred, similar to, but not limited to, any fund raising event, entering into an IPO or any other major event enabling the Company
to reassess the fair value of its investment in the JV.
| F-29 | |
A summary of the change in fair
value of our investment in GMP Bio, as of December 31, 2024 and 2023 is shown below:
SCHEDULE
OF CHANGE IN FAIR VALUE OF OUR INVESTMENT
| 
| | 
December 31, 2024 | | | 
December 31, 2023 | | |
| 
Balance at January 1, 2024 and 2023 | | 
$ | 22,653,225 | | | 
$ | 22,640,519 | | |
| 
Add: change in fair value of investment in GMP Bio | | 
| - | | | 
| 12,706 | | |
| 
| | 
| | | | 
| | | |
| 
Balance at December 31, 2024 and 2023 | | 
$ | 22,653,225 | | | 
$ | 22,653,225 | | |
For information on the various
notes from GMP, refer to Note 5 *GMP Notes*of the Notes to the Consolidated Financial Statements above.
**NOTE 7 - PRIVATE PLACEMENT (PPM-1) AND JH DARBIE
FINANCING**
****
During the period from July 2020
to March 2021, the Company entered into subscription agreements with certain accredited investors pursuant to the JH Darbie Financing,
whereby the Company issued and sold a total of 100 Units, for total gross proceeds of approximately $5 million, pursuant to the JH Darbie
Placement Agreement, with each Unit consisting of:
| 
| 
| 
25,000 shares of Edgepoint Common Stock for a price of $1.00 per share of Edgepoint Common Stock. | |
| 
| 
| 
One convertible promissory note, convertible into up to 25,000 shares of Edgepoint Common Stock, at a conversion price of $1.00 per share or up to 138,889 shares of the Companys Common Stock, at a conversion price of $0.18 per share. | |
| 
| 
| 
50,000 warrants to purchase an equivalent number of shares of Edgepoint Common Stock at $1.00 per share or an equivalent number of shares of the Companys Common Stock at $0.20 per share with a three-year expiration date. Either the Edgepoint or the Companys warrants would be exercised. | |
During the period between July
2023 and January 2024, the Company converted the debt of forty six accredited investors from the JH Darbie Financing (now referred to
as *PPM-1*) into the new subscription agreements under the new financing (*PPM-2*- See Note 8 below),
which resulted in conversion of $2.35 million of old debt into new debt to the Company.
| F-30 | |
As of December 31, 2024, and 2023,
funds received under the JH Darbie Financing, net of debt discounts, consist of the following amounts:
SCHEDULE
OF FUNDS RECEIVED UNDER THE SUBSCRIPTION AGREEMENT
| 
| | 
December 31, 2024 | | | 
December 31, 2023 | | |
| 
| | 
| | | 
| | |
| 
Convertible promissory notes | | 
| | | | 
| | | |
| 
Subscription agreements - accredited investors | | 
$ | - | | | 
$ | 311,693 | | |
| 
Subscription agreements related party | | 
| - | | | 
| - | | |
| 
Total convertible promissory notes | | 
$ | - | | | 
$ | 311,693 | | |
The Company incurred approximately
$0.64 million of issuance costs, including legal costs of approximately $39,000, that are incremental costs directly related to the issuance
of the various instruments bundled in the offering. As of the date of this Report, the PPM notes are in default.
Concurrently with the sale of
the Units, JH Darbie was granted, for nominal consideration, a warrant, exercisable over a five-year period, to purchase 10% of the number
of Units sold in the JH Darbie Financing. As such, the Company granted 10 Units to JH Darbie pursuant to the JH Darbie Placement Agreement.
The terms of convertible notes
are summarized as follows:
| 
| 
| 
Term: Through March 31, 2023. | |
| 
| 
| 
Coupon: 16%. | |
| 
| 
| 
Convertible at the option of the holder at any time in the Companys Common Stock or Edgepoint Common Stock. | |
| 
| 
| 
The conversion price is initially set at $0.18 per share for the Companys Common Stock or $1.00 for Edgepoint Common Stock, subject to adjustment. | |
In February 2022, the Company
and all except one of the Investors agreed to extend the maturity date of the Notes from March 31, 2022, to March 31, 2023. In consideration
for the extension of the Notes, the Company issued to the Investors an aggregate of 33,000,066 Oncotelic Warrants at a price of $0.15
per share of Companys Common Stock. Each Investor will be entitled to receive 333,334 Oncotelic Warrants for each Unit purchased.
Upon the amendment of the terms of the convertible notes under the private placement memorandum. As incentive to extend the maturity date,
approximately 33 million warrants were issued to the Unit Holders who participated in the amendment, the Company repaid the 1-unit holder
who did not participate in the amendment shortly after March 31, 2022. Further, during the year ended December 31, 2023, the Company repaid
two of the unit holders, who held 5 units and opted not to participate in the new JH Darbie financing. While the Company had been in default
under the PPM-1 since April 2023, as of the date of this Annual Report, with the conversion of the rest of the Note Holders under the
PPM-1, the event of default has been addressed.
The Company recognized amortization
expense related to the debt discount and debt issuance costs of approximately $0 and 8,400 for the years ended December 31, 2024 and 2023,
respectively, which is included in interest expense in the statements of operations.
| F-31 | |
**NOTE 8 PRIVATE PLACEMENT -2 (PPM-2) AND
JH DARBIE FUNDING**
****
During the period between July
2023 to January 2024, the Company entered into a series of subscription agreements with forty six accredited investors (the Financing)
whereby the Company issued and converted a total of 94 Units from the previous PPM (*PPM -1*- See Note 7 above) into
the current subscription agreements under the PPM-2, which resulted in conversion of $2.35 million of old debt into new debt to the Company;
and the Company did not receive any cash proceeds through the July 2023 through January 2024 conversions., with each Unit consisting of:
| 
| 
| 
One 16% convertible unsecured promissory note (the Note) of $25,000, convertible into up to 250,000 shares of the Companys common stock (par value of $0.01) based on a conversion price of $0.10 per share. | |
| 
| 
| 
250,000 warrants to purchase an equivalent number of shares of the Companys common stock at a strike price of $0.12 per share (Oncotelic warrant). | |
JH Darbie and the Company are parties to a March 2023
placement agent agreement (Agreement) pursuant to which DH Darbie had the right to sell a minimum of 10 Units and a maximum
of 200 Units on a best-efforts basis. For the 4 tranches of conversion related to PPM 2, placement agent fees of $377,500 were paid to
JH Darbie. Based on the placement agent agreement, JH Darbie was entitled to a non-refundable $25,000 fee to start the due diligence process
and 2% due diligence fees and 13% commissions on all subsequent conversions or new funding. In addition, the Company provided warrant
coverage equal to 13 % of all of the units sold to JH Darbie. As the Company converted an aggregate of 94 units, JH Darbie was entitled
to earn a total of 3,055,000 warrants. A total of 5 unit holders under the PPM-1 opted not to participate in the PPM-2.
In connection with the consummation
of Tranche 1, 2 and 3 and 4 of the July 2023 PPM, the Company entered into a Registration Rights Agreement granting certain registration
rights with respect to the shares of the Companys Common Stock issued in connection with the financing, as well as the shares of
the Companys Common Stock issuable upon exercise of the Warrants. The issuance of the Units is exempt from the registration requirements
of the Securities Act of 1933, as amended (Securities Act), in reliance on the exemptions provided by Section 4(a)(2) of
the Securities Act as provided in Rule 506 of Regulation D promulgated thereunder. The shares of common stock and warrants and any shares
of common stock issuable upon exercise of the warrants, have not been registered under the Securities Act or any other applicable securities
laws, and unless so registered, may not be offered or sold in the United States except pursuant to an exemption from the registration
requirements of the Securities Act.
As of December 31, 2024, and December
31, 2023, debt recorded under PPM-2, net of debt discounts and including accrued interest, consist of the following amounts:
SCHEDULE OF FUNDS RECEIVED
UNDER THE SUBSCRIPTION AGREEMENT
| 
| | 
December 31, 2024 | | | 
December 31, 2023 | | |
| 
Convertible promissory notes | | 
| | | | 
| | | |
| 
Subscription agreements - accredited investors | | 
$ | 2,308,638 | | | 
$ | 1,898,468 | | |
| 
Total convertible promissory, net of discounts | | 
$ | 2,308,638 | | | 
$ | 1,898,468 | | |
The Company incurred approximately
$0.4 million of issuance costs under the PPM-2 and are incremental costs directly related to the issuance of the various instruments bundled
in the offering. Concurrently with the PPM- 2, JH Darbie was granted a total of 3,055,000 stock warrants, exercisable over a two-year
period.
The terms of convertible notes
are summarized as follows:
| 
| 
| 
Term: through December 31, 2025 | |
| 
| 
| 
Coupon: 16% | |
| 
| 
| 
Convertible at the option of the holder at any time into the Companys common stock | |
| 
| 
| 
Conversion price is set at $0.10 per share subject to standard anti-dilution provision. | |
| F-32 | |
Management reviewed the guidance
per ASC 470-60 *Troubled debt restructurings*and ASC 470-50 *Debt- Modifications and Extinguishments*and concluded that the
terms of the agreements were substantially different and, accounted for the transaction as a debt extinguishment. The transaction related
to T4 during the year ended December 31, 2024 resulted in a loss from debt extinguishment of approximately $88,000, which is presented
in other expense in the consolidated statements of operations for the year ended December 31, 2024. The estimated volume weighted grant
date fair value of approximately $0.026 per share associated with the warrants to purchase up to 3,390,000 shares of common stock issued
in this offering, or a total of approximately $88,000, was recorded to additional paid-in capital. All warrants sold in this offering
have an exercise price of $0.12 per share of the Company stock, subject to adjustment, are exercisable immediately and expire two years
from the date of issuance. The fair value of the warrants was estimated using a Black Scholes valuation models using the following input
values:
SCHEDULE
OF FAIR VALUE WARRANTS
| 
Expected Term | | 
| 2 years | | |
| 
Expected volatility | | 
| 173 | % | |
| 
Risk-free interest rates | | 
| 4.29 | % | |
| 
Dividend | | 
| 0.00 | % | |
The Company recorded approximately
$318,000 as an initial debt discount related to the four tranches of PPM 2. The Company recognized amortization expense related to the
debt discount and debt issuance costs of approximately $157,000 and $50,000 for the years ended December 31, 2024 and 2023, respectively,
which is included in interest expense in the statements of operations
During the years ended December
31, 2024 and 2023, the Company incurred approximately $363,000 and $122,000 of interest expense related to the convertible notes.
**NOTE 9 - RELATED PARTY TRANSACTIONS**
****
*Master Service Agreement with Autotelic Inc.*
**
In October 2015, Oncotelic Inc.
entered into a Master Service Agreement (the *MSA*) with Autotelic Inc. (*Autotelic*), a related
party that is partly owned by Dr. Trieu. Dr. Trieu, a related party, is a control person in Autotelic. Autotelic currently owns less than
10% of the Company. The MSA stated that Autotelic will provide business functions and services to the Company and allowed Autotelic to
charge the Company for these expenses paid on its behalf. The MSA includes personnel costs allocated based on amount of time incurred
and other services such as consultant fees, clinical studies, conferences and other operating expenses incurred on behalf of the Company.
The MSA requires a 90-day written termination notice in the event either party requires to terminate such services.
Expenses related to the MSA were
$2,000 and approximately $12,000 for the years ended December 31, 2024 and 2023, respectively. The Company owed Autotelic, Inc. approximately
$0.3 million at December 31, 2024 and December 31, 2023 respectively.
*License Agreement with Autotelic Inc.*
**
In September 2021, the Company
entered into an exclusive License Agreement with Autotelic. For more information on the exclusive license Agreement with Autotelic, refer
to our 2023 Annual Report on Form 10-K filed with SEC on April 12, 2024.
*Notes Payable and Short-Term Loan Related Party*
**
In April 2019, the Company
issued a convertible note to Dr. Trieu totaling $164,444,
including OID of $16,444,
receiving net proceeds of $148,000,
which was used by the Company for working capital and general corporate purposes. The Company issued a Fall 2019 Note to Dr. Trieu
in the principal amount of $250,000.
Dr. Trieu also offset certain amounts due to him in the amount of $35,000
and was converted into the Fall 2019 debt. During the year ended December 31, 2020, Dr. Trieu purchased a total of 5
Units under the private placement for a gross total of $250,000.
During the year ended December 31, 2023, Dr Trieu provided short term loan of $50
thousand to the Company. The balance due and payable to Dr. Trieu, as of December 31, 2024 and 2023, respectively, was $50,000.
In May 2021, Autotelic provided
an additional short-term funding of $250,000 to the Company, which was converted into the August 2021 Notes. Autotelic provided an additional
$120,000 short-term loan to the Company during the year ended December 31, 2022. During the year ended December 31, 2023, Autotelic provided
$1.4 million in short term advances to the Company. During the year ended December 31, 2024, Autotelic provided and additional $0.7 million.
As such, approximately $2.1 million was outstanding and payable to Autotelic at December 31, 2024.
| F-33 | |
*Artius Consulting Agreement*
**
In March 2020, the Company
and Artius Bioconsulting, LLC (*Artius*), for which Mr. King is the Managing Member, entered into an amendment to the
Consulting Agreement dated December 1, 2018, under which Artius agreed to serve as a consultant to the Company for services related to
the Companys business from time to time, effective December 1, 2019 (the *Effective Date*) (the *Artius
Agreement*). For more information on this Agreement, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April
12, 2024.
No expense was recorded during
the year ended December 31, 2024, or 2023, respectively, related to this Agreement.
*Mosaic Consulting Agreement*
**
In July 2024, the Company and
Mosaic, for which Mr. King is the Chief Executive Officer, entered into an consulting agreement (*Mosaic Agreement*),
under which Mosaic agreed to serve as a consultant to the Company for services related to the JVs chemistry, manufacturing and
controls for the San Diego site on a month to month basis at a rate of $7,000 per month. This cost was entirely borne by the JV.
No expense was recorded during
the year ended December 31, 2024, related to the Mosaic Agreement.
*Maida Consulting Agreement*
**
Effective May 5, 2020, the Company
and Dr. Maida entered into an independent consulting agreement, commencing April 1, 2020 (the Maida Agreement), under which
Dr. Maida will assist the Company in providing medical expertise and advice from time to time in the design, conduct and oversight of
the Companys existing and future clinical trials. For more information on this Agreement, refer to our 2021 Annual Report on Form
10-K filed with the SEC on April 15, 2022.
The Company recorded an expense
of $0 during the years ended December 31, 2024 and 2023, respectively, related to this Agreement. Effective April 1, 2022, Dr Maidas
compensation is being borne by the JVA with GMP Bio.
**NOTE 10 - EQUITY PURCHASE AGREEMENT AND REGISTRATION RIGHTS AGREEMENT**
****
On May 3, 2021, the Company entered
into an Equity Purchase Agreement (EPL) and Registration Rights Agreement with Peak One Opportunity Fund LP (Peak
One or the Investor). For further information on EPL, refer to our 2023 Annual Report on Form 10-K filed with the
SEC on April 12, 2024. The Company also filed a post-effective amendment Registration Statement on Form S-1 with the Commission on April
12, 2024, and the Form S-1 was declared effective on April 22, 2024. The Company filed the prospectus under rule 424b3 with the SEC on
April 26, 2024.
During year ended December 31,
2024 and 2023, the Company did not sell any shares of Common Stock under the EPL.
**NOTE 11 STOCKHOLDERS EQUITY**
****
The following transactions affected the Companys
Stockholders Equity:
Issuance of Common Stock during
the year ended December 31, 2024
In February 2024, Fourth Man partially
converted $35,000 of their debt. In connection with the partial Note conversion, the Company issued 500,000 shares of Common Stock to
Fourth Man.
In May 2024, Blue Lake converted
the balance of their $531,000 debt, inclusive of accrued interest and penalty, into 7,605,760 shares of Common Stock of the Company.
Issuance of Common Stock during
the year ended December 31, 2023
In February 2023, Fourth Man partially
converted $71,750 of their debt. In connection with the partial Note conversion, the Company issued 1,025,000 shares of Common Stock to
Fourth Man.
In June 2023, Blue Lake converted
the full remainder of their $181,750 debt, accrued interest and penalty. In connection with this Note conversion, the Company issued 3,466,853
shares of Common Stock to Blue Lake.
In May and June 2023, Fourth Man
converted $50,000 in principal and $30,000 in accrued interest into 1,192,857 shares of Common Stock.
| F-34 | |
In July 2023, Fourth Man converted
approximately $43,000 balance in principal and accrued interest into 627,538 shares of Common Stock.
In October 2023, Fourth Man converted
approximately $72,000 in principal, accrued interest and legal fees into 1,025,000 shares of Common Stock.
For further information on Common
Stock issuance, refer to our 2023 Annual Report on Form 10-K filed with the SEC on April 12, 2024.
**NOTE 12 STOCK-BASED COMPENSATION**
****
*Options*
Pursuant to the Merger, the Companys
Common Stock and corresponding outstanding options survived. The below information details the Companys associated option activity.
As of December 31, 2024, the Company
had options to purchase Common Stock that were outstanding under three stock option plans the 2017 Equity Incentive Plan (the
*2017 Plan*), the 2015 Equity Incentive Plan (the *2015 Plan*) and the 2005 Stock Plan (the *2005
Plan*). Under the 2017 Plan, up to 2,000,000 shares of the Companys Common Stock may be issued pursuant to awards granted
in the form of nonqualified stock options, restricted and unrestricted stock awards, and other stock-based awards. Under the 2015 and
2005 Plans, taken together, up to 27,250,000 shares of the Companys Common Stock may be issued pursuant to awards granted in the
form of incentive stock options, nonqualified stock options, restricted and unrestricted stock awards, and other stock-based awards.
Employees, consultants, and directors
are eligible for awards granted under the 2017 and 2015 Plans. Since the adoption of the 2015 Plan, no further awards may be granted under
the 2005 Plan, although options previously granted remain outstanding in accordance with their terms.
Compensation based stock option
activity for qualified and unqualified stock options are summarized as follows:
SCHEDULE
OF COMPENSATION BASED STOCK OPTION ACTIVITY
| 
| | 
| | | 
Weighted | | |
| 
| | 
| | | 
Average | | |
| 
For the year ended December 31, 2024 | | 
Shares | | | 
Exercise Price | | |
| 
Outstanding at January 1, 2024 | | 
| 24,177,761 | | | 
$ | 0.21 | | |
| 
Expired or cancelled | | 
| - | | | 
| - | | |
| 
Outstanding at December 31, 2024 | | 
| 24,177,761 | | | 
| 0.21 | | |
| 
Options exercisable at December 31, 2024 | | 
| 13,985,261 | | | 
| | | |
| 
| | 
| | | 
Weighted | | |
| 
| | 
| | | 
Average | | |
| 
For the year ended December 31, 2023 | | 
Shares | | | 
Exercise Price | | |
| 
Outstanding at January 1, 2023 | | 
| 25,690,261 | | | 
$ | 0.23 | | |
| 
Expired or cancelled | | 
| (1,512,500 | ) | | 
| 0.46 | | |
| 
Outstanding at December 31, 2023 | | 
| 24,177,761 | | | 
| 0.21 | | |
| 
Options exercisable at December 31, 2023 | | 
| 13,985,261 | | | 
| | | |
| F-35 | |
The following table summarizes
information about options to purchase shares of the Companys Common Stock outstanding and exercisable at December 31, 2024:
SCHEDULE
OF OPTIONS TO PURCHASE SHARES OF COMMON STOCK OUTSTANDING AND EXERCISABLE
| 
Exercise prices | 
| 
| 
Outstanding 
Options | 
| 
| 
Weighted- 
Average 
Remaining Life 
In Years | 
| 
| 
Weighted- 
Average
Exercise 
Price | 
| 
| 
Number 
Exercisable | 
| |
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| 
| |
| 
$ | 
0.1 to $0.15 | 
| 
| 
| 
16,250,000 | 
| 
| 
| 
7.2 | 
| 
| 
$ | 
0.12 | 
| 
| 
| 
6,057,500 | 
| |
| 
| 
0.16 to $0.21 | 
| 
| 
| 
5,502,761 | 
| 
| 
| 
6.5 | 
| 
| 
| 
0.16 | 
| 
| 
| 
5,502,761 | 
| |
| 
| 
0.22 to $0.37 | 
| 
| 
| 
1,550,000 | 
| 
| 
| 
3.0 | 
| 
| 
| 
0.28 | 
| 
| 
| 
1,550,000 | 
| |
| 
| 
0.38 to $0.72 | 
| 
| 
| 
500,000 | 
| 
| 
| 
1.2 | 
| 
| 
| 
0.73 | 
| 
| 
| 
500,000 | 
| |
| 
| 
0.73 to $15.0 | 
| 
| 
| 
375,000 | 
| 
| 
| 
0.4 | 
| 
| 
| 
4.14 | 
| 
| 
| 
375,000 | 
| |
| 
| 
| 
| 
| 
| 
24,177,761 | 
| 
| 
| 
6.5 | 
| 
| 
$ | 
0.21 | 
| 
| 
| 
13,985,261 | 
| |
The compensation expense attributed
to the issuance of the options is recognized as they are vested. The employee stock option plan stock options are generally exercisable
for ten years from the grant date and vest over various terms from the grant date to three years.
As of December 31, 2024, there
was no unamortized stock compensation cost related to the stock options granted during the year ended December 31, 2022. Of the approximately
10 million unvested stock options, the vesting criteria for 7.3 million options is still being evaluated as on the date of this Report,
as those options are subject to individual milestone achievements. For more information on the stock options, refer to our 2023 Annual
Report on Form 10-K filed with the SEC on April 12, 2024.
The Company amortized $0 stock
compensation expense during the years ended December 31, 2024 and 2023, respectively on the 2021 and 2022 grants.
*Warrants*
**
The Company has issued warrants
in connection with the various financings conducted by the Company. For more information on the warrant issuances, refer to our 2023 Annual
Report on Form 10-K filed with the SEC on April 12, 2024.
The issuance of warrants to purchase
shares of the Companys Common Stock, including those attributed to debt issuances, for the years ended December 31, 2024 and 2023,
respectively are summarized as follows:
SCHEDULE
OF WARRANTS ACTIVITY
| 
For the year ended December 31, 2024 | | 
Shares | | | 
Average Exercise Price | | |
| 
Outstanding at January 1, 2024 | | 
| 61,500,355 | | | 
$ | 0.15 | | |
| 
Issued during the year ended December 31, 2024 | | 
| 3,390,000 | | | 
| 0.12 | | |
| 
Exercised / cancelled during the year ended December 31, 2024 | | 
| (33,000,066 | ) | | 
| 0.15 | | |
| 
Outstanding at December 31, 2024 | | 
| 31,890,289 | | | 
$ | 0.13 | | |
| 
For the year ended December 31, 2023 | | 
Shares | | | 
Average Exercise Price | | |
| 
Outstanding at January 1, 2023 | | 
| 81,072,855 | | | 
$ | 0.18 | | |
| 
Issued during the year ended December 31, 2023 | | 
| 23,165,000 | | | 
| 0.12 | | |
| 
Exercised / cancelled during the year ended December 31, 2023 | | 
| (42,737,500 | ) | | 
| 0.20 | | |
| 
Outstanding at December 31, 2023 | | 
| 61,500,355 | | | 
$ | 0.15 | | |
| F-36 | |
The following table summarizes
information about warrants outstanding and exercisable at December 31, 2024:
SCHEDULE
OF WARRANTS OUTSTANDING AND EXERCISABLE
| 
| 
| 
| 
Outstanding and exercisable | 
| |
| 
Exercise Price | 
| 
| 
Number 
Outstanding | 
| 
| 
Weighted- 
Average 
Remaining Life 
in Years | 
| 
| 
Weighted- 
Average 
Exercise 
Price | 
| 
| 
Number 
Exercisable | 
| |
| 
$ | 
0.13 | 
| 
| 
| 
961,539 | 
| 
| 
| 
2.00 | 
| 
| 
| 
0.13 | 
| 
| 
| 
961,539 | 
| |
| 
| 
0.20 | 
| 
| 
| 
4,373,750 | 
| 
| 
| 
2.26-2.47 | 
| 
| 
| 
0.20 | 
| 
| 
| 
4,373,750 | 
| |
| 
| 
0.12 | 
| 
| 
| 
11,300,000 | 
| 
| 
| 
0.51 | 
| 
| 
| 
0.12 | 
| 
| 
| 
11,300,000 | 
| |
| 
| 
0.12 | 
| 
| 
| 
11,865,000 | 
| 
| 
| 
0.81 | 
| 
| 
| 
0.12 | 
| 
| 
| 
11,865,000 | 
| |
| 
| 
0.12 | 
| 
| 
| 
3,390,000 | 
| 
| 
| 
1.08 | 
| 
| 
| 
0.12 | 
| 
| 
| 
3,390,000 | 
| |
| 
| 
| 
| 
| 
| 
31,890,289 | 
| 
| 
| 
0.99 | 
| 
| 
$ | 
0.13 | 
| 
| 
| 
31,890,289 | 
| |
**NOTE 13 INCOME TAXES**
****
Significant components of the
Companys deferred tax assets and liabilities for federal and state income taxes as of December 31, 2024 and 2023 are as follows
in thousands:
SCHEDULE
OF COMPONENTS OF NET DEFERRED TAX ASSETS AND LIABILITIES
| 
| | 
December 31, | | | 
December 31, | | |
| 
| | 
2024 | | | 
2023 | | |
| 
Deferred tax assets: | | 
| | | | 
| | | |
| 
Stock-based compensation | | 
$ | 1,438 | | | 
$ | 1,438 | | |
| 
Assets | | 
| 1,174 | | | 
| 1,304 | | |
| 
Liability accruals | | 
| 311 | | | 
| 324 | | |
| 
R&D Credit | | 
| 1,372 | | | 
| 1,372 | | |
| 
Capital Loss | | 
| 528 | | | 
| 528 | | |
| 
Deferred state tax | | 
| (2,087 | ) | | 
| (2,065 | ) | |
| 
Net operating loss carry forward | | 
| 10,024 | | | 
| 10,489 | | |
| 
Total gross deferred tax assets | | 
| 12,760 | | | 
| 13,390 | | |
| 
Less - valuation allowance | | 
| (12,760 | ) | | 
| (13,390 | ) | |
| 
Net deferred tax assets | | 
$ | - | | | 
$ | - | | |
The Company had gross deferred
tax assets, which primarily relate to net operating loss carryforwards. As of December 31, 2024, the Company had gross federal and state
net operating loss carryforwards, which are available to offset future taxable income, if any. The Company recorded a valuation allowance
in the full amount of its net deferred tax assets since realization of such tax benefits has been determined by our management to be less
likely than not.
Portions of these carryforwards
will expire through 2038, if not otherwise utilized. The Companys utilization of net operating loss carryforwards could be subject
to an annual limitation. as a result of certain past or future events, such as stock sales or other equity events constituting a change
in ownership under the provisions of Sections 382 and 383 of the Internal Revenue Code of 1986, as amended, and similar state provisions.
The annual limitations could result in the expiration of net operating loss carryforwards and tax credits before they can be utilized.
We have not performed a formal analysis, but we believe our ability to use such net operating losses and tax credit carryforwards will
be subject to annual limitations, due to change of ownership control provisions under Section 382 and 383 of the Internal Revenue Code,
which would significantly impact our ability to realize these deferred tax assets.
| F-37 | |
**NOTE 14 COMMITMENTS AND CONTINGENCIES**
****
*Leases*
**
Currently, the Company is leasing
an office located at 29397 Agoura Road, Suite 107, Agoura Hills, CA 91301 on a month-to-month basis until such time a new office is identified.
The Company believes the office is sufficient for its current operations.
*PointR Merger Consideration*
**
The total purchase price in the
PointR Merger of $17,831,427 included $2,625,000 of contingent consideration of shares issuable to PointR shareholders, upon achievement
of certain milestones. For more information on the PointR Merger Contingent Consideration, refer to our 2021 Annual Report on Form 10-K
filed with the SEC on April 12, 2024.
*Third Party Service Provider Claim*
**
The Company had disputed a judgement
of $20,000 for a non-payment to a third service provider. The Company considered the claim to be immaterial to the financial position
of the Company. The Company had filed a counter claim on the third-party service provider as the Company believed the claim to be false
and malicious to the interests of the Company. In March 2024, The Honorable Court overruled the previous judgement and ruled in favor
of the Company.
*Other claims*
**
From time to time, the Company
may become involved in certain claims arising in the ordinary course of business. One of the Companys ex-employees has made a breach
of employment contract claim against the Company. The Company and its legal counsel are evaluating the validity of the claim, as the Company
believes that such claim has limited merits and is hopeful to attain a positive outcome for such claim. Since the Company and its legal
counsel are still evaluating the claim, we are unable to quantify the amount such claim would be settled at, if at all settled.
**NOTE 15 SUBSEQUENT EVENTS**
****
In March 2025, the Company
announced of successfully completing a Phase 1 clinical trial evaluating OT-101, in combination with IL-2 for advanced or metastatic
solid tumors, on behalf of the JV. These results set the stage for new studies that combine OT-101, an antisense therapeutic
targeting Transforming Growth Factor Beta 2 (TGF2), with checkpoint inhibitors (CKIs) and recombinant IL-2
(aldesleukin) (IL-2). The Phase 1 trial (ClinicalTrials.gov ID: NCT04862767) investigated the safety and tolerability
of OT-101 in combination with recombinant IL-2 in patients with advanced or metastatic solid tumors. The combination showed a
tolerable safety profile at the planned dosing schedule, with no unexpected safety signals identified. Based on the favorable safety
data, the JV, through the Company, plans to advance OT-101 plus IL-2 into further clinical studies, exploring synergies with CKIs such as PD-1
blockers.
| F-38 | |