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蛋白酶解 YB-1 片段与 DNA 修复机制相互作用,并在 DNA 损伤应激时增强存活。

The proteolytic YB-1 fragment interacts with DNA repair machinery and enhances survival during DNA damaging stress.

机构信息

Institute of Protein Research; Russian Academy of Sciences; Pushchino, Moscow Region, Russian Federation.

Institute of Protein Research; Russian Academy of Sciences; Pushchino, Moscow Region, Russian Federation; University of Tartu; Institute of Technology; Tartu, Estonia.

出版信息

Cell Cycle. 2013 Dec 15;12(24):3791-803. doi: 10.4161/cc.26670. Epub 2013 Oct 7.

Abstract

The Y-box binding protein 1 (YB-1) is a DNA/RNA-binding nucleocytoplasmic shuttling protein whose regulatory effect on many DNA and RNA-dependent events is determined by its localization in the cell. We have shown previously that YB-1 is cleaved by 20S proteasome between E219 and G220, and the truncated N-terminal YB-1 fragment accumulates in the nuclei of cells treated with DNA damaging drugs. We proposed that appearance of truncated YB-1 in the nucleus may predict multiple drug resistance. Here, we compared functional activities of the full-length and truncated YB-1 proteins and showed that the truncated form was more efficient in protecting cells against doxorubicin treatment. Both forms of YB-1 induced changes in expression of various genes without affecting those responsible for drug resistance. Interestingly, although YB-1 cleavage did not significantly affect its DNA binding properties, truncated YB-1 was detected in complexes with Mre11 and Rad50 under genotoxic stress conditions. We conclude that both full-length and truncated YB-1 are capable of protecting cells against DNA damaging agents, and the truncated form may have an additional function in DNA repair.

摘要

Y 盒结合蛋白 1(YB-1)是一种 DNA/RNA 结合的核质穿梭蛋白,其对许多 DNA 和 RNA 依赖性事件的调节作用取决于其在细胞中的定位。我们之前已经表明,YB-1 可被 20S 蛋白酶体在 E219 和 G220 之间切割,并且在用 DNA 损伤药物处理的细胞中,截断的 N 端 YB-1 片段在核内积累。我们提出,截断的 YB-1 出现在核内可能预示着多种药物耐药性。在这里,我们比较了全长和截断的 YB-1 蛋白的功能活性,并表明截断形式在保护细胞免受阿霉素处理方面更有效。两种形式的 YB-1 诱导各种基因表达的变化,而不影响那些负责耐药性的基因。有趣的是,尽管 YB-1 切割并没有显著影响其 DNA 结合特性,但在遗传毒性应激条件下,截断的 YB-1 与 Mre11 和 Rad50 形成复合物。我们得出结论,全长和截断的 YB-1 都能够保护细胞免受 DNA 损伤剂的侵害,而截断形式可能在 DNA 修复中具有额外的功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e7f/3905071/db78d6b795ce/cc-12-3791-g1.jpg

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