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Facilitation of base excision repair by chromatin remodeling

机译:通过染色质重塑促进碱基切除修复

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Base Excision Repair (BER) is a conserved, intracellular DNA repair system that recognizes and removes chemically modified bases to insure genomic integrity and prevent mutagenesis. Aberrant BER has been tightly linked with abroad spectrum of human pathologies, such as several types of cancer, neurological degeneration, developmental abnormalities, immune dysfunction-and aging. In the cell, BER must recognize and remove DNA lesions from the tightly condensed, protein-coated chromatin. Because chromatin is necessarily refractory to DNA metabolic processes, like transcription and replication, the compaction of the genomic material is also inhibitory to the repair systems necessary for its upkeep. Multiple ATP-dependent chromatin remodelling (ACR) complexes play essential roles in modulating the protein-DNA interactions within chromatin, regulating transcription and promoting activities of some DNA repair systems, including double-strand break repair and nucleotide excision repair. However, it remains unclear how BER operates in the context of chromatin, and if the chromatin remodelling processes that govern transcription and replication also actively regulate the efficiency of BER. In this review we highlight the emerging role of ACR in regulation of BER. (c) 2015 Elsevier B.V. All rights reserved.
机译:碱基切除修复(BER)是一种保守的细胞内DNA修复系统,可识别并去除经过化学修饰的碱基,以确保基因组完整性并防止诱变。 BER异常与国外人类疾病谱密切相关,例如多种类型的癌症,神经系统变性,发育异常,免疫功能障碍和衰老。在细胞中,BER必须识别并去除紧密凝结的蛋白涂层染色质中的DNA损伤。由于染色质必须对DNA代谢过程(例如转录和复制)具有抵抗力,因此基因组材料的压实也抑制了其维持所需的修复系统。多种ATP依赖的染色质重塑(ACR)复合物在调节染色质内的蛋白质-DNA相互作用,调节转录和促进某些DNA修复系统(包括双链断裂修复和核苷酸切除修复)的活性中起着至关重要的作用。然而,目前尚不清楚BER如何在染色质的背景下运作,以及控制转录和复制的染色质重塑过程是否也积极调节BER的效率。在本文中,我们重点介绍了ACR在BER调节中的新兴作用。 (c)2015 Elsevier B.V.保留所有权利。

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