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G2 期检查点释放后的染色体断裂。

Chromosome breakage after G2 checkpoint release.

作者信息

Deckbar Dorothee, Birraux Julie, Krempler Andrea, Tchouandong Leopoldine, Beucher Andrea, Walker Sarah, Stiff Tom, Jeggo Penny, Löbrich Markus

机构信息

Fachrichtung Biophysik, Universität des Saarlandes, 66421 Homburg/Saar, Germany.

出版信息

J Cell Biol. 2007 Mar 12;176(6):749-55. doi: 10.1083/jcb.200612047.

Abstract

DNA double-strand break (DSB) repair and checkpoint control represent distinct mechanisms to reduce chromosomal instability. Ataxia telangiectasia (A-T) cells have checkpoint arrest and DSB repair defects. We examine the efficiency and interplay of ATM's G2 checkpoint and repair functions. Artemis cells manifest a repair defect identical and epistatic to A-T but show proficient checkpoint responses. Only a few G2 cells enter mitosis within 4 h after irradiation with 1 Gy but manifest multiple chromosome breaks. Most checkpoint-proficient cells arrest at the G2/M checkpoint, with the length of arrest being dependent on the repair capacity. Strikingly, cells released from checkpoint arrest display one to two chromosome breaks. This represents a major contribution to chromosome breakage. The presence of chromosome breaks in cells released from checkpoint arrest suggests that release occurs before the completion of DSB repair. Strikingly, we show that checkpoint release occurs at a point when approximately three to four premature chromosome condensation breaks and approximately 20 gammaH2AX foci remain.

摘要

DNA双链断裂(DSB)修复和检查点控制是减少染色体不稳定性的不同机制。共济失调毛细血管扩张症(A-T)细胞存在检查点阻滞和DSB修复缺陷。我们研究了ATM的G2检查点和修复功能的效率及相互作用。艾美氏综合征细胞表现出与A-T相同且上位的修复缺陷,但显示出有效的检查点反应。在用1 Gy照射后4小时内,只有少数G2期细胞进入有丝分裂,但表现出多个染色体断裂。大多数具有检查点功能的细胞在G2/M检查点阻滞,阻滞时间取决于修复能力。引人注目的是,从检查点阻滞中释放的细胞显示出一到两个染色体断裂。这是染色体断裂的一个主要原因。从检查点阻滞中释放的细胞中存在染色体断裂表明释放发生在DSB修复完成之前。引人注目的是,我们发现检查点释放发生在大约三到四个早熟染色体凝缩断裂且大约20个γH2AX焦点仍然存在的时候。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff93/2064048/1493edee534a/jcb1760749f01.jpg

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