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Cockayne 综合征 B 组蛋白在复制应激中的作用:对癌症治疗的影响。

Role of Cockayne Syndrome Group B Protein in Replication Stress: Implications for Cancer Therapy.

机构信息

Department of Biology, McMaster University, Hamilton, ON L8S 4K1, Canada.

出版信息

Int J Mol Sci. 2022 Sep 6;23(18):10212. doi: 10.3390/ijms231810212.

Abstract

A variety of endogenous and exogenous insults are capable of impeding replication fork progression, leading to replication stress. Several SNF2 fork remodelers have been shown to play critical roles in resolving this replication stress, utilizing different pathways dependent upon the nature of the DNA lesion, location on the DNA, and the stage of the cell cycle, to complete DNA replication in a manner preserving genetic integrity. Under certain conditions, however, the attempted repair may lead to additional genetic instability. Cockayne syndrome group B (CSB) protein, a SNF2 chromatin remodeler best known for its role in transcription-coupled nucleotide excision repair, has recently been shown to catalyze fork reversal, a pathway that can provide stability of stalled forks and allow resumption of DNA synthesis without chromosome breakage. Prolonged stalling of replication forks may collapse to give rise to DNA double-strand breaks, which are preferentially repaired by homology-directed recombination. CSB plays a role in repairing collapsed forks by promoting break-induced replication in S phase and early mitosis. In this review, we discuss roles of CSB in regulating the sources of replication stress, replication stress response, as well as the implications of CSB for cancer therapy.

摘要

多种内源性和外源性损伤都可能阻碍复制叉的前进,导致复制压力。已经有研究表明,几种 SNF2 叉重塑酶在解决这种复制压力方面发挥着关键作用,它们利用不同的途径,取决于 DNA 损伤的性质、DNA 上的位置和细胞周期的阶段,以在保持遗传完整性的情况下完成 DNA 复制。然而,在某些情况下,尝试修复可能会导致额外的遗传不稳定性。CSA 综合征 B 组 (CSB) 蛋白,一种以转录偶联核苷酸切除修复作用而闻名的 SNF2 染色质重塑酶,最近被证明能够催化叉反转,这一途径可以为停滞的叉提供稳定性,并允许在不发生染色体断裂的情况下恢复 DNA 合成。复制叉的长时间停滞可能会崩溃,导致 DNA 双链断裂,这些断裂更倾向于通过同源定向重组进行修复。CSB 通过促进 S 期和早期有丝分裂中的断裂诱导复制,在修复崩溃的叉方面发挥作用。在这篇综述中,我们讨论了 CSB 在调节复制压力源、复制压力反应以及 CSB 对癌症治疗的影响方面的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/30aa/9499456/5199fab5b8cb/ijms-23-10212-g001.jpg

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