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烷基化剂诱导嗜热栖热菌中反向回旋酶的选择性降解和DNA片段化

Selective degradation of reverse gyrase and DNA fragmentation induced by alkylating agent in the archaeon Sulfolobus solfataricus.

作者信息

Valenti Anna, Napoli Alessandra, Ferrara Maria Carmina, Nadal Marc, Rossi Mosè, Ciaramella Maria

机构信息

Institute of Protein Biochemistry, Consiglio Nazionale delle Ricerche, Via P. Castellino 111, 80131 Naples, Italy.

出版信息

Nucleic Acids Res. 2006 Apr 14;34(7):2098-108. doi: 10.1093/nar/gkl115. Print 2006.

Abstract

Reverse gyrase is a peculiar DNA topoisomerase, specific of hyperthermophilic Archaea and Bacteria, which has the unique ability of introducing positive supercoiling into DNA molecules. Although the function of the enzyme has not been established directly, it has been suggested to be involved in DNA protection and repair. We show here that the enzyme is degraded after treatment of Sulfolobus solfataricus cells with the alkylating agent MMS. MMS-induced reverse gyrase degradation is highly specific, since (i) neither hydroxyurea (HU) nor puromycin have a similar effect, and (ii) topoisomerase VI and two chromatin components are not degraded. Reverse gyrase degradation does not depend on protein synthesis. Experiments in vitro show that direct exposure of cell extracts to MMS does not induce reverse gyrase degradation; instead, extracts from MMS-treated cells contain some factor(s) able to degrade the enzyme in extracts from control cells. In vitro, degradation is blocked by incubation with divalent metal chelators, suggesting that reverse gyrase is selectively degraded by a metal-dependent protease in MMS-treated cells. In addition, we find a striking concurrence of extensive genomic DNA degradation and reverse gyrase loss in MMS-treated cells. These results support the hypothesis that reverse gyrase plays an essential role in DNA thermoprotection and repair in hyperthermophilic organisms.

摘要

反向回旋酶是一种独特的DNA拓扑异构酶,存在于嗜热古菌和细菌中,具有将正超螺旋引入DNA分子的独特能力。尽管该酶的功能尚未直接确定,但有研究表明它参与DNA的保护和修复。我们在此表明,用烷化剂MMS处理嗜热栖热放线菌细胞后,该酶会被降解。MMS诱导的反向回旋酶降解具有高度特异性,因为(i)羟基脲(HU)和嘌呤霉素均无类似作用,且(ii)拓扑异构酶VI和两种染色质成分未被降解。反向回旋酶的降解不依赖于蛋白质合成。体外实验表明,将细胞提取物直接暴露于MMS不会诱导反向回旋酶降解;相反,MMS处理细胞的提取物中含有某些能够降解对照细胞提取物中该酶的因子。在体外,与二价金属螯合剂孵育可阻止降解,这表明反向回旋酶在MMS处理的细胞中被金属依赖性蛋白酶选择性降解。此外,我们发现MMS处理的细胞中广泛的基因组DNA降解与反向回旋酶缺失同时出现。这些结果支持了反向回旋酶在嗜热生物的DNA热保护和修复中起重要作用的假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa9d/1440885/909d2c26ba78/gkl115f1.jpg

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