通过其相互作用蛋白塑造BRCA2功能。
Molding BRCA2 function through its interacting partners.
作者信息
Martinez Juan S, Baldeyron Céline, Carreira Aura
机构信息
a Institut Curie; Centre de Recherche ; Orsay , France.
b CNRS UMR3348; Genotoxic Stress and Cancer; Centre Universitaire ; Orsay , France.
出版信息
Cell Cycle. 2015;14(21):3389-95. doi: 10.1080/15384101.2015.1093702.
Abstract
The role of the tumor suppressor BRCA2 has been shaped over 2 decades thanks to the discovery of its protein and nucleic acid partners, biochemical and structural studies of the protein, and the functional evaluation of germline variants identified in breast cancer patients. Yet, the pathogenic and functional effect of many germline mutations in BRCA2 remains undetermined, and the heterogeneity of BRCA2-associated tumors challenges the identification of causative variants that drive tumorigenesis. In this review, we propose an overview of the established and emerging interacting partners and functional pathways attributed to BRCA2, and we speculate on how variants altering these functions may contribute to cancer susceptibility.
摘要
得益于其蛋白质和核酸伴侣的发现、蛋白质的生化与结构研究以及对乳腺癌患者中鉴定出的种系变体的功能评估,肿瘤抑制因子BRCA2的作用在20多年间得以明确。然而,BRCA2中许多种系突变的致病和功能效应仍未确定,且BRCA2相关肿瘤的异质性对驱动肿瘤发生的致病变体的鉴定构成挑战。在本综述中,我们概述了已确定的和新出现的与BRCA2相关的相互作用伴侣和功能途径,并推测改变这些功能的变体如何可能导致癌症易感性。
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