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A Biparatopic Antibody That Modulates MET Trafficking Exhibits Enhanced Efficacy Compared with Parental Antibodies in MET-Driven Tumor Models

抗体 表位 酪氨酸激酶 表型 阻断抗体 单克隆抗体 封锁 癌症 基因 免疫学 信号转导 癌症研究 生物 受体 细胞生物学 遗传学
作者
John O. DaSilva,Katie Yang,Andrés E. Perez Bay,Julian Andreev,Peter Ngoi,Erica Pyles,Matthew C. Franklin,Drew Dudgeon,Ashique Rafique,Anthony Doré,Frank J. Delfino,Terra Potocky,Robert Babb,Gang Chen,Douglas MacDonald,William C. Olson,Gavin Thurston,Christopher Daly
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:26 (6): 1408-1419 被引量:27
标识
DOI:10.1158/1078-0432.ccr-19-2428
摘要

Abstract Purpose: Recent clinical data demonstrate that tumors harboring MET genetic alterations (exon 14 skip mutations and/or gene amplification) respond to small-molecule tyrosine kinase inhibitors, validating MET as a therapeutic target. Although antibody-mediated blockade of the MET pathway has not been successful in the clinic, the failures are likely the result of inadequate patient selection strategies as well as suboptimal antibody design. Thus, our goal was to generate a novel MET blocking antibody with enhanced efficacy. Experimental Design: Here, we describe the activity of a biparatopic MET×MET antibody that recognizes two distinct epitopes in the MET Sema domain. We use a combination of in vitro assays and tumor models to characterize the effect of our antibody on MET signaling, MET intracellular trafficking, and the growth of MET-dependent cells/tumors. Results: In MET-driven tumor models, our biparatopic antibody exhibits significantly better activity than either of the parental antibodies or the mixture of the two parental antibodies and outperforms several clinical-stage MET antibodies. Mechanistically, the biparatopic antibody inhibits MET recycling, thereby promoting lysosomal trafficking and degradation of MET. In contrast to the parental antibodies, the biparatopic antibody fails to activate MET-dependent biological responses, consistent with the observation that it recycles inefficiently and induces very transient downstream signaling. Conclusions: Our results provide strong support for the notion that biparatopic antibodies are a promising therapeutic modality, potentially having greater efficacy than that predicted from the properties of the parental antibodies.
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