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遗传性乳腺癌与 BRCA1 相关的 FANCJ/BACH1/BRIP1。

Hereditary breast cancer and the BRCA1-associated FANCJ/BACH1/BRIP1.

机构信息

Department of Cancer Biology, University of Massachusetts Medical School, 364 Plantation St., Worcester, MA 01605, USA.

出版信息

Future Oncol. 2011 Feb;7(2):253-61. doi: 10.2217/fon.10.191.

DOI:10.2217/fon.10.191
PMID:21345144
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3109611/
Abstract

It is clear that FANCJ, also known as BACH1 or BRIP1, is an essential tumor suppressor gene based on the identification of clinically relevant mutations not only in breast cancer, but also the childhood cancer syndrome, Fanconi anemia. This conclusion is further supported by the direct and functional interaction between FANCJ and the hereditary breast cancer-associated gene product BRCA1. In the absence of the FANCJ DNA helicase or its interaction with BRCA1, cells have defects in several aspects of the DNA damage response. In particular, the BRCA1-FANCJ interaction is essential for promoting error-free repair, checkpoint control and for limiting DNA damage tolerance. As the number of FANCJ clinical mutations and affected patients accumulate, it will be critical to understand whether the associated tumors resemble BRCA-associated tumors. If so, FANCJ patients could also benefit from new therapies that selectively sensitize DNA repair-defective tumors and spare healthy cells. In this article, we summarize the breast cancer-associated FANCJ mutations and discuss functional outcomes for DNA repair and tumor suppression.

摘要

很明显,FANCJ,也称为 BACH1 或 BRIP1,是一种必需的肿瘤抑制基因,这一结论基于对不仅在乳腺癌,而且在儿童癌症综合征——范可尼贫血症中临床相关突变的鉴定。这一结论还得到了 FANCJ 与遗传性乳腺癌相关基因产物 BRCA1 之间直接和功能相互作用的支持。在缺乏 FANCJ DNA 解旋酶或其与 BRCA1 的相互作用的情况下,细胞在 DNA 损伤反应的几个方面存在缺陷。特别是,BRCA1-FANCJ 相互作用对于促进无差错修复、检查点控制和限制 DNA 损伤耐受至关重要。随着 FANCJ 临床突变数量和受影响患者的增加,了解相关肿瘤是否类似于 BRCA 相关肿瘤将至关重要。如果是这样,FANCJ 患者也可能受益于新的治疗方法,这些方法可以选择性地使 DNA 修复缺陷型肿瘤敏感,并使健康细胞免受损伤。在本文中,我们总结了乳腺癌相关的 FANCJ 突变,并讨论了 DNA 修复和肿瘤抑制的功能结果。

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