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评估 BACH1/FANCJ 与 MLH1 之间在 DNA 交联修复中的关联。

Assessing the link between BACH1/FANCJ and MLH1 in DNA crosslink repair.

机构信息

Department of Cancer Biology, University of Massachusetts Medical School, Worcester, Massachusetts 01605, USA.

出版信息

Environ Mol Mutagen. 2010 Jul;51(6):500-7. doi: 10.1002/em.20568.

Abstract

FANCJ (also known as BRIP1 or BACH1) is a DNA helicase that was originally identified by its direct interaction with the hereditary breast cancer protein, BRCA1. Similar to BRCA1, FANCJ function is essential for DNA repair and breast cancer suppression. FANCJ is also mutated in the cancer prone syndrome Fanconi anemia, for which patient cells are characterized by extreme sensitivity to agents that generate DNA interstand crosslinks. Unexpectedly, correction of the interstrand crosslink sensitivity of FANCJ-null patient cells did not require the FANCJ/BRCA1 interaction. Instead, FANCJ binding to the mismatch repair protein, MLH1 was required. Given this finding, we address the role of FANCJ and MLH1 in DNA crosslink processing and how their functions could be linked in checkpoint and/or recombination pathways. We speculate that after DNA crosslink processing and repair, the FANCJ/MLH1 interaction is critical for recovery and restart of replication. These ideas are considered and summarized in this review.

摘要

FANCJ(也称为 BRIP1 或 BACH1)是一种 DNA 解旋酶,最初是通过其与遗传性乳腺癌蛋白 BRCA1 的直接相互作用而被鉴定出来的。与 BRCA1 相似,FANCJ 的功能对于 DNA 修复和乳腺癌抑制至关重要。FANCJ 也在易患癌症的综合征范可尼贫血症中发生突变,患者细胞的特征是对产生 DNA 链间交联的试剂极其敏感。出乎意料的是,纠正 FANCJ 缺失患者细胞的链间交联敏感性并不需要 FANCJ/BRCA1 相互作用。相反,需要 FANCJ 与错配修复蛋白 MLH1 结合。鉴于这一发现,我们研究了 FANCJ 和 MLH1 在 DNA 交联处理中的作用,以及它们的功能如何在检查点和/或重组途径中联系起来。我们推测,在 DNA 交联处理和修复之后,FANCJ/MLH1 相互作用对于复制的恢复和重新启动至关重要。这些想法在本综述中进行了考虑和总结。

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