Irreversible electroporation (IRE) with intratumoral CD40 antibody increases T-cell reactivity to personalized neoantigens in locally advanced pancreatic cancer
Presenter: Rebekah White, MD Session: Phase I Clinical Trials in Progress Time: 4/20/2026 9:00:00 AM → 4/20/2026 12:00:00 PM
Authors
Spencer Mirabile-Brightman 1 , Bjoern Peters 1 , Himangshu Sonowal 2 , Zachary Berman 2 , Zev Wainberg 3 , Aaron Miller 2 , Karen Messer 2 , Jiayu Chen 2 , Yago Pico de Coana 4 , Peter Ellmark 4 , Stephen Schoenberger 1 , Rebekah R. White 2 1 La Jolla Institute of Immunology, La Jolla, CA, 2 UC San Diego School of Medicine, La Jolla, CA, 3 UC Los Angeles School of Medicine, Los Angeles, CA, 4 Alligator Bioscience, Lung, Sweden
Abstract
Background: Irreversible electroporation (IRE) is a form of non-thermal tumor ablation in use for locally advanced PDAC. Our published preclinical data demonstrate that combination of IRE with local CD40 agonism induces systemic anti-tumor immune effects. Mitazalimab, a second-generation CD40 agonistic IgG1 mAb, had promising clinical activity when delivered systemically in combination with chemotherapy in metastatic PDAC. Methods: We are conducting a phase I dose-escalation study of mitazalimab injected intratumorally at the time of surgical IRE in patients with locally advanced PDAC after standard of care chemotherapy (NCT06205849). Primary endpoints are the rates of dose limiting toxicities and adverse events. Secondary endpoints are progression-free and overall survival. Candidate neoantigens (NeoAg’s) are identified by profiling nucleic acids derived from tumor biopsies obtained intraoperatively prior to IRE using our Identification-Prioritization-Validation (IPV) bioinformatic pipeline. Peptides representing prioritized mutations are synthesized. Peripheral blood mononuclear cells are collected pre- and 12-weeks post-treatment to evaluate NeoAg-specific T-cell reactivity using ELISPOT for interferon-gamma. “Hits” were peptides with spots > 2 SD above negative control peptides. Results: We have enrolled eight patients since the study opened in September 2024. Pre- and post-treatment ELISPOT assays have been completed for 6 patients, and all 6 demonstrated NeoAg-specific T-cell reactivity. For most of the validated NeoAg’s, reactivity was either newly detected or increased post-treatment, but reactivity to some NeoAg’s decreased with treatment. The total number of recognized NeoAg’s was increased in post- vs pre-treatment samples for 5/6 patients assessed. Conclusions: Unbiased, personalized IPV analysis confirms the presence of NeoAg-specific responses against multiple mutations, which are diversified after treatment with IRE and CD40 agonism. The evaluation of additional patients and correlation with clinical outcomes are ongoing. NeoAg-specific T-cell reactivity pre- and post-treatment Patient # of mutations tested Pre-treatment “hits” Post-treatment “hits” 2 25 1 4 3 24 8 12 4 25 5 14 5 25 2 2 7 28 9 10 8 22 2 6
Disclosure
S. Mirabile-Brightman, None. B. Peters, Amgen Other, Speaker, consultant. Sanofi Other, Speaker, consultant. H. Sonowal, None. Z. Berman, Aztra-Zeneca ). Boston Scientific Other, Consultant. Trisalus Life Sciences ). Guerbet Other, Consulting. Varian Other, Consultant. Z. Wainberg, Abbvie Other, Consulting. Alligator Other, Consulting. Amgen Other, Consulting. Arcus Consulting. Bayer Other, Consulting. BeOne Other, Consulting. Bristol Myers Squibb Other, Consulting. Daiichi Sankyo Other, Consulting. Gilead Other, Consulting. Ipsen Other, Consulting. Janssen Other, Consulting. Jazz Other, Consulting. Lilly Other, Consulting. Merck Other, Consulting. EMD Serono Other, Consulting. Novartis Other, Consulting. Pfizer Other, Consulting. Phanes Other, Consulting. Revolution Medicine Other, Consulting. AztraZeneca Other, Consulting. A. Miller, None.. K. Messer, None.. J. Chen, None. Y. Pico de Coana, Alligator Bioscience Employment, Stock. P. Ellmark, Alligator Bioscience Employment, Stock. S. Schoenberger, None.. R. R. White, None.
Cited in
Control: 9847 · Presentation Id: 12186 · Meeting 21436