A PSMA-Targeting CD3 Bispecific Antibody Induces Antitumor Responses that Are Enhanced by 4-1BB Costimulation

癌症研究 双特异性抗体 T细胞 CD3型 抗体 医学 免疫疗法 抗原 癌症免疫疗法 免疫系统 免疫学 CD8型 单克隆抗体
作者
Danica Chiu,Richard Tavaré,Lauric Haber,Olulanu H. Aina,Kristin Vazzana,Priyanka Ram,Makenzie Danton,Jennifer Finney,Sumreen Jalal,Pamela Krueger,Jason T. Giurleo,Dangshe Ma,Eric Smith,Gavin Thurston,Jessica R. Kirshner,Alison Crawford
出处
期刊:Cancer immunology research [American Association for Cancer Research]
卷期号:8 (5): 596-608 被引量:45
标识
DOI:10.1158/2326-6066.cir-19-0518
摘要

Abstract Patients with hematologic cancers have improved outcomes after treatment with bispecific antibodies that bind to CD3 on T cells and that redirect T cells toward cancer cells. However, clinical benefit against solid tumors remains to be shown. We made a bispecific antibody that targets both the common prostate tumor–specific antigen PSMA and CD3 (PMSAxCD3) and provide evidence for tumor inhibition in several preclinical solid tumor models. Mice expressing the human extracellular regions of CD3 and PSMA were generated to examine antitumor efficacy in the presence of an intact immune system and PSMA expression in normal tissues. PSMAxCD3 accumulated in PSMA-expressing tissues and tumors as detected by immuno-PET imaging. Although PSMAxCD3 induced T-cell activation and showed antitumor efficacy in mice with low tumor burden, PSMAxCD3 lost efficacy against larger solid tumors, mirroring the difficulty of treating solid tumors in the clinic. Costimulatory receptors can enhance T-cell responses. We show here that costimulation can enhance the antitumor efficacy of PSMAxCD3. In particular, 4-1BB stimulation in combination with PSMAxCD3 enhanced T-cell activation and proliferation, boosted efficacy against larger tumors, and induced T-cell memory, leading to durable antitumor responses. The combination of CD3 bispecific antibodies and anti-4-1BB costimulation represents a therapeutic approach for the treatment of solid tumors.
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