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

人源CD137×PD-L1双特异性抗体通过依赖于特定情境的T细胞共刺激和检查点阻断促进抗肿瘤免疫。

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

Abstract

Immune 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.

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