DT40细胞DNA交联修复过程中维持磷酸化Chk1和G2/M期阻滞需要BRCA1。

BRCA1 Is Required for Maintenance of Phospho-Chk1 and G2/M Arrest during DNA Cross-Link Repair in DT40 Cells.

作者信息

Draga Margarethe, Madgett Elizabeth B, Vandenberg Cassandra J, du Plessis David, Kaufmann Aisling, Werler Petra, Chakraborty Prasun, Lowndes Noel F, Hiom Kevin

机构信息

Division of Cancer Research, Medical Research Institute, Jacqui Wood Cancer Centre, Ninewells Hospital and Medical School, Dundee, Scotland Institute of Anatomy II, Department of Vertebrate Embryology, University of Cologne, Cologne, Germany.

MRC Laboratory of Molecular Biology, Cambridge Biomedical Campus, Cambridge, United Kingdom.

出版信息

Mol Cell Biol. 2015 Nov;35(22):3829-40. doi: 10.1128/MCB.01497-14. Epub 2015 Aug 31.

DOI:10.1128/MCB.01497-14

PMID:26324327

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4609749/

Abstract

The Fanconi anemia DNA repair pathway is pivotal for the efficient repair of DNA interstrand cross-links. Here, we show that FA-defective (Fancc(-)) DT40 cells arrest in G2 phase following cross-link damage and trigger apoptosis. Strikingly, cell death was reduced in Fancc(-) cells by additional deletion of the BRCA1 tumor suppressor, resulting in elevated clonogenic survival. Increased resistance to cross-link damage was not due to loss of toxic BRCA1-mediated homologous recombination but rather through the loss of a G2 checkpoint. This proapoptotic role also required the BRCA1-A complex member ABRAXAS (FAM175A). Finally, we show that BRCA1 promotes G2 arrest and cell death by prolonging phosphorylation of Chk1 on serine 345 after DNA damage to sustain arrest. Our data imply that DNA-induced cross-link death in cells defective in the FA pathway is dependent on the ability of BRCA1 to prolong cell cycle arrest in G2 phase.

摘要

范可尼贫血DNA修复途径对于高效修复DNA链间交联至关重要。在此，我们表明，FA缺陷型（Fancc(-)）DT40细胞在交联损伤后停滞于G2期并触发凋亡。引人注目的是，通过额外缺失BRCA1肿瘤抑制因子，Fancc(-)细胞中的细胞死亡减少，导致克隆形成存活率升高。对交联损伤的抗性增加并非由于有毒的BRCA1介导的同源重组丧失，而是由于G2期检查点的丧失。这种促凋亡作用也需要BRCA1-A复合物成员ABRAXAS（FAM175A）。最后，我们表明，BRCA1通过延长DNA损伤后Chk1丝氨酸345位点的磷酸化以维持停滞，从而促进G2期停滞和细胞死亡。我们的数据表明，FA途径缺陷的细胞中DNA诱导的交联死亡取决于BRCA1在G2期延长细胞周期停滞的能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1862/4609749/e0e2a5d46494/zmb9991010060001.jpg

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DT40细胞DNA交联修复过程中维持磷酸化Chk1和G2/M期阻滞需要BRCA1。

BRCA1 Is Required for Maintenance of Phospho-Chk1 and G2/M Arrest during DNA Cross-Link Repair in DT40 Cells.

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