Journal Article10.1158/1078-0432.CCR-20-4001
Fibroblast Activation Protein α-Targeted CD40 Agonism Abrogates Systemic Toxicity and Enables Administration of High Doses to Induce Effective Antitumor Immunity.
Eva Sum,Moritz Rapp,Philipp Fröbel,Marine Le Clech,Harald Dürr,Anna Maria Giusti,Mario Perro,Dario Speziale,Leo Kunz,Elena Menietti,Peter Brünker,Ulrike Hopfer,Martin Lechmann,Andrzej Sobieniecki,Birte Appelt,Roberto Adelfio,Nicolini Valeria G,Anne Freimoser-Grundschober,Whitney Shannon Jordaan,Sara Labiano,Felix C. Weber,Thomas Emrich,Francois Christen,Birgit Essig,Pedro Romero,Christine Trumpfheller,Pablo Umana +26 more
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TL;DR: In this article, a bispecific FAP-CD40 antibody was developed, which induces CD40 stimulation solely in presence of fibroblast activation protein α (FAP), a protease specifically expressed in the tumor stroma.
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Abstract: Purpose: CD40 agonists hold great promise for cancer immunotherapy (CIT) as they enhance dendritic cell (DC) activation and concomitant tumor-specific T-cell priming. However, the broad expression of CD40 accounts for sink and side effects, hampering the efficacy of anti-CD40 antibodies. We hypothesized that these limitations can be overcome by selectively targeting CD40 agonism to the tumor. Therefore, we developed a bispecific FAP-CD40 antibody, which induces CD40 stimulation solely in presence of fibroblast activation protein α (FAP), a protease specifically expressed in the tumor stroma. Experimental Design: FAP-CD409s in vitro activity and FAP specificity were validated by antigen-presenting cell (APC) activation and T-cell priming assays. In addition, FAP-CD40 was tested in subcutaneous MC38-FAP and KPC-4662-huCEA murine tumor models. Results: FAP-CD40 triggered a potent, strictly FAP-dependent CD40 stimulation in vitro. In vivo, FAP-CD40 strongly enhanced T-cell inflammation and growth inhibition of KPC-4662-huCEA tumors. Unlike nontargeted CD40 agonists, FAP-CD40 mediated complete regression of MC38-FAP tumors, entailing long-term protection. A high dose of FAP-CD40 was indispensable for these effects. While nontargeted CD40 agonists induced substantial side effects, highly dosed FAP-CD40 was well tolerated. FAP-CD40 preferentially accumulated in the tumor, inducing predominantly intratumoral immune activation, whereas nontargeted CD40 agonists displayed strong systemic but limited intratumoral effects. Conclusions: FAP-CD40 abrogates the systemic toxicity associated with nontargeted CD40 agonists. This enables administration of high doses, essential for overcoming CD40 sink effects and inducing antitumor immunity. Consequently, FAP-targeted CD40 agonism represents a promising strategy to exploit the full potential of CD40 signaling for CIT.
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References
Role of Crosslinking for Agonistic CD40 Monoclonal Antibodies as Immune Therapy of Cancer
TL;DR: Fc crosslinking is not an essential requirement for agonistic antihuman CD40 mAbs, in which potency is more dependent on the CD40 epitope recognized and the strength of the signal achieved.
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Toxicity of an Fc-engineered anti-CD40 antibody is abrogated by intratumoral injection and results in durable antitumor immunity.
TL;DR: It is shown that toxicity can be circumvented and durable systemic antitumor immunity achieved by intratumoral delivery of an Fc-engineered anti-CD40 agonistic antibody.
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Preclinical pharmacokinetics, pharmacodynamics, and activity of a humanized anti-CD40 antibody (SGN-40) in rodents and non-human primates
Sean K. Kelley,Thomas Gelzleichter,Dong Xie,Wyne P. Lee,Walter C. Darbonne,Ferhan Qureshi,Kim M. Kissler,Ezogelin Oflazoglu,Iqbal S. Grewal,Iqbal S. Grewal +9 more
TL;DR: It is necessary to select patients suitable for vaginal or laparoscopic mesh placement for intranasal administration based on prior history and once they provide informed consent for surgery to treat central nervous system disorders.
Abstract CT004: A Phase Ib study of CD40 agonistic monoclonal antibody APX005M together with gemcitabine (Gem) and nab-paclitaxel (NP) with or without nivolumab (Nivo) in untreated metastatic ductal pancreatic adenocarcinoma (PDAC) patients
Mark H. O'Hara,Eileen M. O'Reilly,Mick Rosemarie,Gauri R. Varadhachary,Zev A. Wainberg,Andrew H. Ko,George A. Fisher,Osama E. Rahma,Jaclyn P. Lyman,Christopher R. Cabanski,Erica L. Carpenter,Travis J. Hollmann,Pier Federico Gherardini,Lacey J. Kitch,Cheryl Selinsky,Theresa LaVallee,Ovid C. Trifan,Ute Dugan,Vanessa M. Hubbard-Lucey,Robert H. Vonderheide +19 more
TL;DR: Gem/NP/APX005M ± nivo demonstrated manageable safety profiles and promising antitumor activity in untreated metastatic PDAC pts and was selected as the dose for a randomized Phase II study in which the primary endpoint is 1-year overall survival.
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Preclinical pharmacokinetics, pharmacodynamics, and activity of a humanized anti-CD40 antibody (SGN-40) in rodents and non-human primates: Preclinical pharmacology of anti-CD40 in rodents and primates
Sean K. Kelley,Thomas Gelzleichter,Dong Xie,Wyne P. Lee,Walter C. Darbonne,Ferhan Qureshi,Kim Kissler,Ezogelin Oflazoglu,Iqbal S. Grewal +8 more
TL;DR: The data suggest that SGN‐40 has appropriate pharmacokinetic properties that support its clinical use, and based upon interspecies scaling, S GN‐40 clearance in humans is predicted to be similar to observed SGN•40 clearanceIn monkeys, clearance of SGN40 was also much faster at low dose, suggesting nonlinear pharmacokinetics in these species.
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