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Precision Designed Science For Immunotherapy INVESTOR PRESENTATION NASDAQ:
2 Certain information in this presentation may include forward-looking
statements (including within the meaning of Section 21E of the United States Securities Exchange Act of 1934, as amended, and Section 27A of the United States Securities Act of 1933, as amended) concerning PDS Biotechnology Corporation (the
"Company") and other matters. These statements may discuss goals, intentions and expectations as to future plans, trends, events, results of operations or financial condition, or otherwise, based on current beliefs of the Company's
management, as well as assumptions made by, and information currently available to, management. Forward-looking statements generally include statements that are predictive in nature and depend upon or refer to future events or conditions, and
include words such as "may," "will," "should," "would," "expect," "anticipate," "plan," "likely," "believe," "estimate," "project," "intend," "forecast," "guidance", "outlook" and other similar expressions among others. Forward-looking
statements are based on current beliefs and assumptions that are subject to risks and uncertainties and are not guarantees of future performance. Actual results could differ materially from those contained in any forward-looking statement as
a result of various factors, including, without limitation: the Company's ability to protect its intellectual property rights; the Company's anticipated capital requirements, including the Company's anticipated cash runway and the Company's
current expectations regarding its plans for future equity financings; the Company's dependence on additional financing to fund its operations and complete the development and commercialization of its product candidates, and the risks that
raising such additional capital may restrict the Company's operations or require the Company to relinquish rights to the Company's technologies or product candidates; the Company's limited operating history in the Company's current line of
business, which makes it difficult to evaluate the Company's prospects, the Company's business plan or the likelihood of the Company's successful implementation of such business plan; the timing for the Company or its partners to initiate the
planned clinical trials for PDS0101, PDS0203 and other Versamune and Infectimune based product candidates; the future success of such trials; the successful implementation of the Company's research and development programs and
collaborations, including any collaboration studies concerning PDS0101, PDS0203 and other Versamune and Infectimune based product candidates and the Company's interpretation of the results and findings of such programs and collaborations
and whether such results are sufficient to support the future success of the Company's product candidates; the success, timing and cost of the Company's ongoing clinical trials and anticipated clinical trials for the Company's current product
candidates, including statements regarding the timing of initiation, pace of enrollment and completion of the trials (including the Company's ability to fully fund its disclosed clinical trials, which assumes no material changes to our
currently projected expenses), futility analyses, presentations at conferences and data reported in an abstract, and receipt of interim or preliminary results (including, without limitation, any preclinical results or data), which are not
necessarily indicative of the final results of the Company's ongoing clinical trials; any Company statements about its understanding of product candidates mechanisms of action and interpretation of preclinical and early clinical results from
its clinical development programs and any collaboration studies; the success of the Company's license agreements, including the potential for the clinical and nonclinical data available under the Company's exclusive license agreement with
Merck KGaA to aid in the development of the Versamune platform; and other factors, including legislative, regulatory, political and economic developments not within the Company's control, including unforeseen circumstances or other
disruptions to normal business operations arising from or related to COVID-19. The foregoing review of important factors that could cause actual events to differ from expectations should not be construed as exhaustive and should be read in
conjunction with statements that are included herein and elsewhere, including the risk factors included in the Company's annual and periodic reports filed with the SEC. The forward-looking statements are made only as of the date of this press
release and, except as required by applicable law, the Company undertakes no obligation to revise or update any forward-looking statement, or to make any other forward-looking statements, whether as a result of new information, future events
or otherwise. Versamune is a registered trademark, and Infectimune is a trademark of PDS Biotechnology Corporation KEYTRUDA is a registered trademark of Merck Sharp and Dohme LLC, a subsidiary of Merck & Co., Inc., Rahway, NJ, USA
Forward-Looking Statements 2
1 2 4 Company Overview Who we are: Leveraging our first-in-class T cell
activating platform and our antibody conjugated immuno-cytokine platform to develop safer, more effective and longer lasting immunotherapies to treat cancer and infectious disease Clinical Partnerships: Merck, National Cancer Institute, MD
Anderson Cancer Center, Mayo Clinic Financial: Cash as of September 30, 2022 - $71.6M cash runway to Q2 2024 with a potential registrational trial in 2023 3 3 Entering Registrational Trial for PDS0101: PDS0101 to enter Phase 3
registrational trial in 2023. PDS0101 is based on the Versamune T cell activating platform and is being developed to treat all types of HPV16-positive cancers
Designed to address limitations of current immunotherapy with potential efficacy
over immune checkpoint inhibitors (ICI) and ICIs in combination with chemotherapy Versamune Versamune + IgG1 IL-12 PDS0301 (tumor-targeting, antibody conjugated IL-12) turns "cold tumors" into "hot tumors" which are more recognized by T
cells by utilizing an antibody to deliver IL-12 into the tumor, which also limits the amount of IL-12 in the blood, making PDS0301 well tolerated by patients in a phase 1 clinical trial The combination overcomes key immune suppressive
mechanisms by inhibiting immune suppressive forces and reducing the population of myeloid derived suppressor cells (MDSC) to more effectively combat the cancer Oncology Platform Overview Induces a powerful and long-lasting anti-tumor
response by delivering tumor-specific proteins into the immune system and activates a specific signaling pathway that promotes the production of active tumor-infiltrating killer T cells within the patient's body 4 Reference phase 1 study :
The Oncologist, 2023, XX, 1-8 doi.org/10.1093/oncolo/oyac244/.
Versamune Oncology Platform
3 6 PDS0101 and Mechanism of Action Comprised of cationic lipids (R-DOTAP)
co-administered with proprietary HPV16-specific tumor antigens, delivered via subcutaneous injection R-DOTAP spontaneously assembles into virus-like nanoparticles promoting efficient uptake by immune system Delivers antigen to CD4+ and CD8+
T cells. Activates the Type I Interferon pathway, leading to superior, multifunctional T cell responses References: Gandhapudi SK, et al. 2019. Antigen priming with enantiospecific cationic lipid nanoparticles induces potent antitumor CTL
responses through novel induction of a Type I IFN response. J Immunol. 202 (12): 3524-3536. Smalley Rumfield C et al. 2020. Immunomodulation to enhance the efficacy of an HPV therapeutic vaccine. J. for ImmunoTherapy of Cancer
8:e000612. Generates right type, potency and quantity of killer T cells
Combination PDS Biotech Funded Partner Co-Funded PDS0104 (TRP2) TBD Arm 1:
ICI na ve 1st line treatment Arm 2: ICI refractory 2nd or 3rd line treatment PDS0101 (HPV16) VERSATILE-002 Fast Track Designation PDS0101 (HPV16) IMMUNOCERV PDS0102 (TARP) PDS0103
(MUC1) Candidate Indication PC P1 P2 P3 R Partner(s) Recurrent/metastatic HPV16-positive head and neck cancer KEYTRUDA( (standard of care) HPV-positive anal, cervical, head and neck, penile, vaginal, vulvar cancers Arm 1: ICI
naive 2nd line treatment Arm 2: ICI refractory 3rd line treatment ICI 1st line treatment of locally advanced (IB3-IVA) cervical cancer TARP-associated AML, prostate and breast cancers MUC-1 associated breast, colon, lung, ovarian and
other cancers Chemo-radiation (standard of care) TBD TBD Reference: Data on file. 7 PDS0101 (HPV16) Mayo Clinic Pre-metastatic HPV-associated oropharyngeal cancer (OPSCC) Arm 1: PDS0101 monotherapy Arm 2: PDS0101 +
KEYTRUDA KEYTRUDA (standard of care) PDS0101/PDS0301 (HPV16) NCI-led Triple Combination Melanoma Oncology Pipeline Developed in partnership with leaders in immune oncology
More than 46,0002 patients were estimated to have been diagnosed last year with
HPV-associated cancers in the US1,2 HPV vaccination is not expected to impact the rate of HPV-related cancer incidence for decades3 Existing immunotherapies cost $150,000+ annually per patient1 US HPV-associated cancer incidence2 1Company
estimates based on CDC data. Assessments have not been adjusted to reflect HPV16-expression 2CDC website 3 Projected Association of Human Papillomavirus Vaccination with Oropharynx Cancer in the US 2020-2045, JAMA Oncology, September
2021 PDS0101 Market Opportunity Designed to treat human papillomavirus (HPV16)-positive cancers $6B Market Opportunity1 Reference: Data on file. 8
CIN lesion regression at 1-3 months (retrospective) 60% 20% 20% 9 PDS0101
HPV16-Targeted Immunotherapy * When treated with selected human clinical trial dosage (1mg and 3mg Versamune ) References: L. Wood et al. A Novel Enantio-Specific Cationic Lipid R-DOTAP + HPV16 E6 & E7 Antigens Induces Potent
Antigen-Specific CD8+ T Cell Responses In-Vivo in Subjects with CIN and High-Risk Human Papillomavirus Infection. Nov 8, 2019. SITC. Presentation O17. Most patients infected with multiple high risk strains of HPV that are more resistant to
spontaneous regression Potentially overcomes key limitation of immuno-oncology: > 20-fold increase in circulating dual INF- & Granzyme-B inducing killer T-cells vs. pre-treatment at Day 14* Phase 1 trial results showed no serious or
dose-limiting toxicities PDS0101 Phase 1 Clinical Trial In vivo CD8+ T cell responses appear to correlate with regression of CIN cervical lesions supporting preclinical studies
1Yoshida-Court et al,, IMMUNOCERV, an ongoing Phase II trial combining PDS0101,
an HPV-specific T cell immunotherapy, with chemotherapy and radiation for treatment of locally advanced cervical cancers (NCT04580771); SITC 2022 10 PDS0101 activates the immune system to generate killer T cells (CD8+ T cells that induce
granzyme-B) Killer T cells target, infiltrate and eliminate the cervical cancer tumors HPV16 tumor DNA in the blood circulation declines by day 170 (T5) 100% (9/9) Objective Response Rate & 89% (8/9) Complete Response No recurrences
in Complete Responders at 1 year Quantity of tumor cells circulating in the blood at start of treatment Killer T cells that infiltrated the tumors PDS0101 Appears to Induce Clinically Beneficial T Cells Induction of activated CD8+
killer T cells correlates with elimination of circulating tumor DNA1 Representative Subject
119% objective response rate with KEYTRUDA monotherapy reported in KEYNOTE-048
study 212-month overall survival of 49% with KEYTRUDA monotherapy reported in KEYNOTE-048 study 317% of patients had treatment related grade 3 and higher adverse events with KEYTRUDA monotherapy reported in KEYNOTE-048
study 11 Partner: FDA approved standard of care: KEYTRUDA (Pembrolizumab) owned by Merck1,2 Preliminary Results PDS0101+KEYTRUDA Fast Track Designation awarded by FDA Preparing to progress to registrational trial based on successful
FDA meeting Preliminary efficacy data (American Society of Clinical Oncology (ASCO) Conference, June 2022): Objective response (% of patients with 30% tumor shrinkage) - 7/17 (41.1%)1 Clinical benefit (stable disease + objective
response) - 13/17 (76.5%) 9-month overall survival rate - 87.2%2 Safety In first 43 patients, no treatment related grade 3 and higher (serious) adverse events - 0/43 (0%)3 VERSATILE-002 Phase 2 Clinical Trial: PDS0101 + KEYTRUDA
Potential treatment for recurrent or metastatic HPV16-positive head and neck cancer
Phase 2: PDS0101 + KEYTRUDA Company-sponsored trial for the potential
treatment of HPV16-positive metastatic/recurrent head and neck cancer (VERSATILE-002) 12 Complete Response (CR) Partial Response (PR) Stable Disease (SD) Progressive Disease (PD) N=17 Subjects w/Imaging Data OR (2 CR + 5PR) 7
(41.2%) SD (reduction in 4/6) 6 (35.3%) PD 4 (23.5%) CR+PR+SD 13 (76.5%) *Reference: Weiss J. et al. Phase II study VERSATILE-002 evaluation of PDS0101 and KEYTRUDA in treatment of CPI na ve and ICI refractory patients with recurrent
or metastatic HPV16-related HNSCC. Presented at: American Society of Clinical Oncology 2022 Annual Meeting; June 3-7, 2022; Virtual. Abstract: 6041. In first 43 patients treated had zero grade 3 or higher treatment related adverse events
Versamune + IgG1 IL-12 Oncology Platform
14 PDS0101 HPV16-Targeted Immunotherapy 60% 20% 20% Tumor sections revealed
that IgG1 IL-12 binds to exposed cell nuclei within necrotic regions of murine tumors. PDS0301 (IgG1 IL-12) is a first-in-class immuno-cytokine fusion protein composed of two molecules of IL-12 fused to each of the heavy chains of the human
IgG1 antibody IGg1 antibody targets DNA/histones exposed in necrotic areas of solid tumors, delivering IL-12 into the tumor and limiting its systemic accumulation PDS0301: A Novel Investigational Tumor-Targeted IgG1 IL-12
15 PDS0101 HPV16-Targeted Immunotherapy 20% Safety Results - PDS0301 Most
adverse events were low grade self-limiting (Grade 1 & 2 toxicities) Grade 3 toxicities included aspartate transaminase/alanine transaminase [AST/ALT] elevation (1/13), flu-like symptoms (1/13), decreased white blood cell count
(1/13) Efficacy Results - PDS0301 upregulates PD-L1 expression including soluble PD-L1 Analysis at baseline and early after PDS0301 treatment showed association with clinical response. 50% (6/12) experienced stable disease and 42% (5/12)
developed progressive disease Phase 1 PDS0301 (IgG1 IL1-2) Monotherapy Trial in Advanced Cancer Patients with Metastatic Solid Tumors PDS0301 monotherapy promotes therapeutically relevant immune responses Stronger immune activation is
observed at higher doses of PDS0301 Analysis of patients at baseline and after PDS0301 treatment showed association with clinical response Interferon-gamma (IFN- ) is associated with induction of T cells and Granzyme B is associated with
induction of active killer (CD8) T cells 20% Immune Correlates Strauss 2019 Clin Canc Res: doi: 10.1158/1078-0432.CCR-18-1512 Toney 2023 International Immunopharmacology. doi.org/10.1016/j.intimp.2023.109736
*73% grade 3 and higher adverse events reported in KEYNOTE-048 Burtness 2019
https://doi.org/10.1016/S0140-6736(19)32591-7 Goswami 2022 http://dx.doi.org/10.1136/jitc-2022-SITC2022.0695 16 Immunology/immune correlates, (SITC), November 2022: Greater than two-fold increase in HPV16-specific T cells in the blood of
11/14 (79% ) of the evaluated patients Induction of multifunctional killer (CD8) T cells Increases in granzyme B (associated with active killer T cells), IFN- , TNF- , etc., signal a pro-inflammatory response and role in overcoming tumor
immune suppression PDS0101 HPV16-Targeted Immunotherapy Partner: Types of cancer included in the trial: Anal, cervical, head and neck, penile, vaginal, vulvar FDA approved standard of care: None Triple Combination: PDS0101 + PDS0301 +
Checkpoint Inhibitor Advanced HPV16-positive cancer patients who are checkpoint inhibitor refractory Safety results (Arms 1 & 2)* 24/50 (48%) of patients experienced grade 3 and higher adverse events 2/50 (4%) experienced grade 4
17 Phase 2 Results in Recurrent Metastatic ICI Refractory HPV-Positive Cancer
(PD-L1 agnostic) Compared to Published Data Triple Combination: PDS0101 + PDS0301 + Checkpoint Inhibitor Advanced HPV16-positive cancer patients who are checkpoint inhibitor refractory N=29 Objective Response (ORR) in high dose PDS0301
Group = 63% (5/8) *Strauss J, et al. J Immunother Cancer 2020;8:e001395. doi:10.1136/jitc-2020-001395Strauss 2021 J Clin Oncol 39, 2021 (suppl 15; abstr 2501).DOI10.1200/JCO.2021.39.15_suppl.2501 **ASCO 2022: Strauss 2022 DOI:
10.1200/JCO.2022.40.16_suppl.2518 Journal of Clinical Oncology 40, no. 16_suppl (June 01, 2022) 2518-2518. tumor shrinkage in HPV16-negative subjects (ASCO 2021) - Suggests critical role of PDS0101-induced HPV16-specific CD8+ T cells No
tumor shrinkage in HPV16-negative subjects (ASCO 2021) - Suggests critical role of PDS0101-induced HPV16-specific CD8+ T cells
18 PDS0101 HPV16-Targeted Immunotherapy Phase 2 Results in Recurrent
Metastatic ICI Na ve Head and Neck Cancer (CPS>0; PD-L1 agnostic) Compared to Published Data Triple Combination: PDS0101 + PDS0301 + Checkpoint Inhibitor Advanced HPV16-positive cancer patients who are checkpoint inhibitor naive *Data
from KEYNOTE-048 STUDY Median OS not yet reached N=8
Projected Milestones Through 3Q 2023* *Based on current enrollment and forecast
modeling as of December 2022. Subject to change. 19 2Q22 3Q22 4Q22 1Q23 2Q23 PDS0101 Preliminary data from IMMUNOCERV (MD Anderson) Estimated IND filing in MUC1-related cancers PDS0103 Anticipate preliminary efficacy data from Mayo
Clinic IIT 3Q23 Updated preliminary safety and updated efficacy data from NCI trial presented at ASCO Preliminary safety and efficacy data (KEYTRUDA combo) presented at ASCO - FAST TRACK DESIGNATION GRANTED Completed Type B meeting with
FDA for combination therapy of PFS0101, PDS0301 and ICI Discussions with the FDA on Pivotal Trial (VERSATILE-002) Initiate registrational trial for PDS0101 Anticipate updated data (VERSATILE-002)
1 2 4 Company Overview Who we are: Leveraging our first-in-class T cell
activating platform and our antibody conjugated immuno-cytokine platform to develop safer, more effective and longer lasting immunotherapies to treat cancer and infectious disease Clinical Partnerships: Merck, National Cancer Institute, MD
Anderson Cancer Center, Mayo Clinic Financial: Cash as of September 30, 2022 - $71.6M cash runway to Q2 2024 with a potential registrational trial in 2023 3 20 Entering Registrational Trial for PDS0101: PDS0101 to enter Phase 3