Preclinical Development of the Anti-LAG-3 Antibody REGN3767: Characterization and Activity in Combination with the Anti-PD-1 Antibody Cemiplimab in Human -Knockin Mice

Overview

Journal Mol Cancer Ther

Date 2019 Aug 10

PMID 31395688

Citations 45

Authors

Elena Burova

Aynur Hermann

Jie Dai

Erica Ullman

Gabor Halasz

Terra Potocky

Seongwon Hong

Matt Liu

Omaira Allbritton

Amy Woodruff

Jerry Pei

Ashique Rafique

William Poueymirou

Joel Martin

Douglas Macdonald

William C Olson

Andrew Murphy

Ella Ioffe

Gavin Thurston

Markus Mohrs

Affiliations

Soon will be listed here.

Abstract

In the tumor microenvironment, multiple inhibitory checkpoint receptors can suppress T-cell function, thereby enabling tumor immune evasion. Blockade of one of these checkpoint receptors, PD-1, with therapeutic antibodies has produced positive clinical responses in various cancers; however, the efficacy of this approach can be further improved. Simultaneously targeting multiple inhibitory checkpoint receptors has emerged as a promising therapeutic strategy. Here, we report the development and characterization of REGN3767, a fully human IgG4 antibody targeting LAG-3, another inhibitory receptor on T cells. REGN3767 binds human and monkey LAG-3 with high affinity and specificity and blocks the interaction of LAG-3 with its ligand, MHC class II. In an engineered T-cell/antigen-presenting cell bioassay, REGN3767 alone, or in combination with cemiplimab (REGN2810, human anti-PD-1 antibody), blocked inhibitory signaling to T cells mediated by hLAG-3/MHCII in the presence of PD-1/PD-L1. To test the activity of REGN3767 alone or in combination with cemiplimab, we generated human knockin mice, in which the extracellular domains of mouse and were replaced with their human counterparts. In these humanized mice, treatment with cemiplimab and REGN3767 showed increased efficacy in a mouse tumor model and enhanced the secretion of proinflammatory cytokines by tumor-specific T cells. The favorable pharmacokinetics and toxicology of REGN3767 in nonhuman primates, together with enhancement of antitumor efficacy of anti-PD-1 antibody in preclinical tumor models, support its clinical development.

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