BRCA1 Is Required for Common-Fragile-Site Stability via Its G2/M Checkpoint Function

机译：通过其G2 / M检查点功能需要BRCA1来实现共易碎场地稳定性

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Common fragile sites are loci that form chromosome gaps or breaks when DNA synthesis is partially inhibited. Fragile sites are prone to deletions, translocations, and other rearrangements that can cause the inactivation of associated tumor suppressor genes in cancer cells. It was previously shown that ATR is critical to fragile-site stability and that ATR-deficient cells have greatly elevated fragile-site expression (A. M. Casper, P. Nghiem, M. F. Arlt, and T. W. Glover, Cell >111:779-789, 2002). Here we demonstrate that mouse and human cells deficient for BRCA1, due to mutation or knockdown by RNA interference, also have elevated fragile-site expression. We further show that BRCA1 functions in the induction of the G2/M checkpoint after aphidicolin-induced replication stalling and that this checkpoint function is involved in fragile-site stability. These data indicate that BRCA1 is important in fragile-site stability and that fragile sites are recognized by the G2/M checkpoint pathway, in which BRCA1 plays a key role. Furthermore, they suggest that mutations in BRCA1 or interacting proteins could lead to rearrangements at fragile sites in cancer cells.

机译：常见的脆弱位点是在部分抑制DNA合成时形成染色体缺口或断裂的基因座。易碎位点易于缺失，易位和其他重排，可能导致癌细胞中相关的肿瘤抑制基因失活。先前显示，ATR对脆弱位点的稳定性至关重要，并且ATR缺陷型细胞的脆弱位点表达大大提高（AM Casper，P。Nghiem，MF Arlt和TW Glover，Cell > 111： 779-789，2002）。在这里，我们证明了由于突变或RNA干扰导致的BRCA1缺陷的小鼠和人类细胞，其脆弱位点表达也有所提高。我们进一步表明，在蚜虫素诱导的复制停滞后，BRCA1在G2 / M检查点的诱导中起作用，并且该检查点功能与脆弱的位点稳定性有关。这些数据表明，BRCA1在脆弱位点稳定性中很重要，并且脆弱位点被G2 / M检查点途径识别，其中BRCA1起着关键作用。此外，他们认为BRCA1或相互作用蛋白中的突变可能导致癌细胞脆弱部位的重排。

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期刊名称 Molecular and Cellular Biology
作者
Martin F. Arlt; Bo Xu; Sandra G. Durkin; Anne M. Casper; Michael B. Kastan; Thomas W. Glover;
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作者单位

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年(卷),期 2004(24),15
年度 2004
页码 6701–6709
总页数 9
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;
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入库时间 2022-08-17 12:23:15

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专利

1. BRCA1 Is Required for Common-Fragile-Site Stability via Its G2/M Checkpoint Function [J] . Martin F. Arlt, Bo Xu, Sandra G. Durkin, Molecular and Cellular Biology . 2004,第15期

机译：通过其G2 / M检查点功能，需要BRCA1才能实现共易碎场地稳定性
2. An ATR- and BRCA1-Mediated Fanconi Anemia Pathway Is Required for Activating the G2/M Checkpoint and DNA Damage Repair upon Rereplication [J] . Wenge Zhu, Anindya Dutta Molecular and Cellular Biology . 2006,第12期

机译：ATR和BRCA1介导的Fanconi贫血途径是激活G2 / M检查点和复制后DNA损伤修复所必需的
3. Centrosome amplification and a defective G2-M cell cycle checkpoint induce genetic instability in BRCA1 exon 11 isoform-deficient cells. [J] . Xu X, Weaver Z, Linke SP, Molecular cell . 1999,第3期

机译：中心体扩增和有缺陷的G2-M细胞周期检查点在BRCA1外显子11亚型缺陷型细胞中引起遗传不稳定。
4. Functional and Quality Requirements for Susceptibility Genetic Testing in Cancer Care: The Case of BRCA1/2 Testing in Jordan [C] . Amal Al-Tabba, Maysa Al-Hussaini, Amal Al-Omari International Conference on Cancer Care Informatics . 2018

机译：癌症护理中易感基因测试的功能和质量要求：以约旦的BRCA1 / 2测试为例
5. ATM, BRCA1, and Aurora A: Mechanisms of G2/M Checkpoint Control in Human Embryonic Stem Cells [D] . Beckta, Jason Mark. 2014

机译：ATM，BRCA1和Aurora A：人类胚胎干细胞中G2 / M检查点控制的机制。
6. An ATR- and BRCA1-Mediated Fanconi Anemia Pathway Is Required for Activating the G2/M Checkpoint and DNA Damage Repair upon Rereplication [O] . Wenge Zhu, Anindya Dutta 2006

机译：ATR和BRCA1介导的Fanconi贫血途径是激活G2 / M检查点和复制后DNA损伤修复所必需的
7. BRCA1 Is Required for Common-Fragile-Site Stability via Its G2/M Checkpoint Function [O] . Arlt, Martin F., Xu, Bo, Durkin, Sandra G., 2004

机译：通过其G2 / M检查点功能需要BRCA1来实现共易碎场地稳定性
8. Checkpoint Functions of the BRCA1/BARD1 Tumor Suppressor [R] . Modi, A. 2009

机译：BRCa1 / BaRD1肿瘤抑制因子的检查点功能

BRCA1 Is Required for Common-Fragile-Site Stability via Its G2/M Checkpoint Function

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