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(p)ppGpp 合酶 RSH 作为 RelA/SpoT 同源物在金黄色葡萄球菌严格反应和毒力中的作用。

Role of the (p)ppGpp synthase RSH, a RelA/SpoT homolog, in stringent response and virulence of Staphylococcus aureus.

机构信息

Interfaculty Institute of Microbiology and Infection Medicine, Universität Tübingen, Elfriede-Aulhorn-Strasse 6, 72076 Tübingen, Germany.

出版信息

Infect Immun. 2010 May;78(5):1873-83. doi: 10.1128/IAI.01439-09. Epub 2010 Mar 8.

Abstract

In most bacteria, nutrient limitations provoke the stringent control through the rapid synthesis of the alarmones pppGpp and ppGpp. Little is known about the stringent control in the human pathogen Staphylococcus aureus, partly due to the essentiality of the major (p)ppGpp synthase/hydrolase enzyme RSH (RelA/SpoT homolog). Here, we show that mutants defective only in the synthase domain of RSH (rsh(syn)) are not impaired in growth under nutrient-rich conditions. However, these mutants were more sensitive toward mupirocin and were impaired in survival when essential amino acids were depleted from the medium. RSH is the major enzyme responsible for (p)ppGpp synthesis in response to amino acid deprivation (lack of Leu/Val) or mupirocin treatment. Transcriptional analysis showed that the RSH-dependent stringent control in S. aureus is characterized by repression of genes whose products are predicted to be involved in the translation machinery and by upregulation of genes coding for enzymes involved in amino acid metabolism and transport which are controlled by the repressor CodY. Amino acid starvation also provoked stabilization of the RNAs coding for major virulence regulators, such as SaeRS and SarA, independently of RSH. In an animal model, the rsh(syn) mutant was shown to be less virulent than the wild type. Virulence could be restored by the introduction of a codY mutation into the rsh(syn) mutant. These results indicate that stringent conditions are present during infection and that RSH-dependent derepression of CodY-regulated genes is essential for virulence in S. aureus.

摘要

在大多数细菌中,营养限制会通过快速合成警报素 pppGpp 和 ppGpp 引发严格控制。关于人类病原体金黄色葡萄球菌中的严格控制,人们知之甚少,部分原因是主要(p)ppGpp 合酶/水解酶酶 RSH(RelA/SpoT 同源物)的必需性。在这里,我们表明,仅在 RSH 的合成酶结构域中存在缺陷的突变体(rsh(syn)) 在富营养条件下的生长不受影响。然而,这些突变体对 mupirocin 更敏感,并且当培养基中耗尽必需氨基酸时,它们的存活能力受到损害。RSH 是响应氨基酸饥饿(缺乏 Leu/Val)或 mupirocin 处理而合成(p)ppGpp 的主要酶。转录分析表明,金黄色葡萄球菌中 RSH 依赖性严格控制的特征是抑制其产物被预测参与翻译机制的基因,并上调编码参与氨基酸代谢和转运的酶的基因,这些基因受抑制物 CodY 控制。氨基酸饥饿还引发编码主要毒力调节剂(如 SaeRS 和 SarA)的 RNA 稳定,而与 RSH 无关。在动物模型中,rsh(syn)突变体比野生型的毒力要小。通过将 codY 突变引入 rsh(syn)突变体,可以恢复毒力。这些结果表明,在感染过程中存在严格条件,并且 RSH 依赖性 CodY 调节基因的去抑制对于金黄色葡萄球菌的毒力至关重要。

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