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细菌中铜响应基因调控。

Copper-responsive gene regulation in bacteria.

机构信息

Biologie der Mikroorganismen, Fakultät für Biologie und Biotechnologie, Ruhr-Universität Bochum, 44780 Bochum, Germany.

出版信息

Microbiology (Reading). 2012 Oct;158(Pt 10):2451-2464. doi: 10.1099/mic.0.058487-0. Epub 2012 Aug 23.

Abstract

Copper is an essential cofactor of various enzymes, but free copper is highly toxic to living cells. To maintain cellular metabolism at different ambient copper concentrations, bacteria have evolved specific copper homeostasis systems that mostly act as defence mechanisms. As well as under free-living conditions, copper defence is critical for virulence in pathogenic bacteria. Most bacteria synthesize P-type copper export ATPases as principal defence determinants when copper concentrations exceed favourable levels. In addition, many bacteria utilize resistance-nodulation-cell division (RND)-type efflux systems and multicopper oxidases to cope with excess copper. This review summarizes our current knowledge on copper-sensing transcriptional regulators, which we assign to nine different classes. Widespread one-component regulators are CueR, CopY and CsoR, which were initially identified in Escherichia coli, Enterococcus hirae and Mycobacterium tuberculosis, respectively. CueR activates homeostasis gene expression at elevated copper concentrations, while CopY and CsoR repress their target genes under copper-limiting conditions. Besides these one-component systems, which sense the cytoplasmic copper status, many Gram-negative bacteria utilize two-component systems, which sense periplasmic copper concentrations. In addition to these well-studied transcriptional factors, copper control mechanisms acting at the post-transcriptional and the post-translational levels will be discussed.

摘要

铜是多种酶的必需辅因子,但游离铜对活细胞具有高度毒性。为了在不同的环境铜浓度下维持细胞代谢,细菌已经进化出特定的铜稳态系统,这些系统主要起防御机制的作用。除了在自由生活条件下,铜防御对于病原细菌的毒力至关重要。当铜浓度超过有利水平时,大多数细菌合成 P 型铜输出 ATP 酶作为主要防御决定因素。此外,许多细菌利用抗性调节细胞分裂(RND)型外排系统和多铜氧化酶来应对过量的铜。本综述总结了我们目前对铜感应转录调节剂的认识,我们将其分为九类。广泛存在的单组分调节剂是 CueR、CopY 和 CsoR,它们最初分别在大肠杆菌、屎肠球菌和结核分枝杆菌中被发现。CueR 在铜浓度升高时激活同源基因的表达,而 CopY 和 CsoR 在铜限制条件下抑制其靶基因。除了这些检测细胞质铜状态的单组分系统外,许多革兰氏阴性细菌还利用检测周质铜浓度的双组分系统。除了这些研究充分的转录因子外,还将讨论在转录后和翻译后水平发挥作用的铜调控机制。

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