A human CD137×PD-L1 bispecific antibody promotes anti-tumor immunity via context-dependent T cell costimulation and checkpoint blockade

Author:

Geuijen Cecile,Tacken Paul,Wang Liang-Chuan,Klooster Rinse,van Loo Pieter Fokko,Zhou Jing,Mondal Arpita,Liu Yao-binORCID,Kramer Arjen,Condamine ThomasORCID,Volgina AllaORCID,Hendriks Linda J. A.,van der Maaden Hans,Rovers Eric,Engels Steef,Fransen Floris,den Blanken-Smit Renate,Zondag-van der Zande Vanessa,Basmeleh Abdul,Bartelink Willem,Kulkarni Ashwini,Marissen Wilfred,Huang Cheng-Yen,Hall Leslie,Harvey Shane,Kim Soyeon,Martinez Marina,O’Brien Shaun,Moon Edmund,Albelda Steven,Kanellopoulou Chrysi,Stewart Shaun,Nastri HoracioORCID,Bakker Alexander B. H.,Scherle Peggy,Logtenberg Ton,Hollis Gregory,de Kruif John,Huber Reid,Mayes Patrick A.ORCID,Throsby MarkORCID

Abstract

AbstractImmune checkpoint inhibitors demonstrate clinical activity in many tumor types, however, only a fraction of patients benefit. Combining CD137 agonists with these inhibitors increases anti-tumor activity preclinically, but attempts to translate these observations to the clinic have been hampered by systemic toxicity. Here we describe a human CD137xPD-L1 bispecific antibody, MCLA-145, identified through functional screening of agonist- and immune checkpoint inhibitor arm combinations. MCLA-145 potently activates T cells at sub-nanomolar concentrations, even under suppressive conditions, and enhances T cell priming, differentiation and memory recall responses. In vivo, MCLA-145 anti-tumor activity is superior to immune checkpoint inhibitor comparators and linked to recruitment and intra-tumor expansion of CD8 + T cells. No graft-versus-host-disease is observed in contrast to other antibodies inhibiting the PD-1 and PD-L1 pathway. Non-human primates treated with 100 mg/kg/week of MCLA-145 show no adverse effects. The conditional activation of CD137 signaling by MCLA-145, triggered by neighboring cells expressing >5000 copies of PD-L1, may provide both safety and potency advantages.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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