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首页> 外文期刊>Environmental and molecular mutagenesis. >Chromodomain helicase DNA-binding protein 2 affects the repair of X-ray and UV-induced DNA damage.
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Chromodomain helicase DNA-binding protein 2 affects the repair of X-ray and UV-induced DNA damage.

机译:染色体域解旋酶DNA结合蛋白2影响X射线和UV诱导的DNA损伤的修复。

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摘要

Eukaryotic cells have evolved a variety of parallel and redundant DNA damage response pathways that function in a coordinated fashion to prevent the fixation of DNA damage as mutations. Despite the wealth of knowledge on DNA damage signaling on downstream cellular events, the mechanisms of DNA damage recognition, DNA repair as well as DNA damage signaling in the context of chromatin is poorly understood. Chromodomain helicase DNA-binding proteins (CHD) belong to a group of highly conserved chromatin remodeling proteins that are implicated in regulation of transcription. In an effort to understand the physiological role of one of the CHD members in a mammalian model system, we developed a mutant mouse model for the Chd2 gene. The Chd2 mutant mice are highly susceptible to spontaneous lymphoid tumor formation. In this study, we present evidence that the Chd2 mutant cells are defective in their ability to repair DNA damage induced by ionizing and ultraviolet radiation. Consistent with the role of Chd2 in regulating DNA damage responses, the Chd2 mutant cells are also sensitive to DNA damaging agents in clonogenic assays. In summary, our data suggest that the Chd2 protein is involved in regulating the DNA damage responses at the chromatin level.
机译:真核细胞已经进化出多种平行和冗余的DNA损伤反应途径,这些途径以协调的方式起作用,以防止DNA损伤作为突变被固定。尽管对下游细胞事件中的DNA损伤信号传递有丰富的知识,但对于染色质背景下的DNA损伤识别,DNA修复以及DNA损伤信号传递的机制知之甚少。染色体域解旋酶DNA结合蛋白(CHD)属于一组高度保守的染色质重塑蛋白,与转录调控有关。为了努力了解CHD成员之一在哺乳动物模型系统中的生理作用,我们开发了Chd2基因的突变小鼠模型。 Chd2突变小鼠高度易发自发性淋巴样肿瘤。在这项研究中,我们提供的证据表明Chd2突变细胞在修复由电离和紫外线辐射诱导的DNA损伤方面存在缺陷。与Chd2在调节DNA损伤反应中的作用一致,在克隆形成测定中,Chd2突变细胞对DNA损伤剂也很敏感。总而言之,我们的数据表明Chd2蛋白参与了染色质水平的DNA损伤反应的调控。

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