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金黄色葡萄球菌对外源性硫辛酸的利用灵活性增加。

Increased flexibility in the use of exogenous lipoic acid by Staphylococcus aureus.

作者信息

Laczkovich Irina, Teoh Wei Ping, Flury Sarah, Grayczyk James P, Zorzoli Azul, Alonzo Francis

机构信息

Department of Microbiology and Immunology, Loyola University Chicago - Stritch School of Medicine, 2160 S. First Avenue, Maywood, IL, 60153, USA.

出版信息

Mol Microbiol. 2018 Jul;109(2):150-168. doi: 10.1111/mmi.13970. Epub 2018 May 3.

Abstract

Lipoic acid is a cofactor required for intermediary metabolism that is either synthesized de novo or acquired from environmental sources. The bacterial pathogen Staphylococcus aureus encodes enzymes required for de novo biosynthesis, but also encodes two ligases, LplA1 and LplA2, that are sufficient for lipoic acid salvage during infection. S. aureus also encodes two H proteins, GcvH of the glycine cleavage system and the homologous GcvH-L encoded in an operon with LplA2. GcvH is a recognized conduit for lipoyl transfer to α-ketoacid dehydrogenase E2 subunits, while the function of GcvH-L remains unclear. The potential to produce two ligases and two H proteins is an unusual characteristic of S. aureus that is unlike most other Gram positive Firmicutes and might allude to an expanded pathway of lipoic acid acquisition in this microorganism. Here, we demonstrate that LplA1 and LplA2 facilitate lipoic acid salvage by differentially targeting lipoyl domain-containing proteins; LplA1 targets H proteins and LplA2 targets α-ketoacid dehydrogenase E2 subunits. Furthermore, GcvH and GcvH-L both facilitate lipoyl relay to E2 subunits. Altogether, these studies identify an expanded mode of lipoic acid salvage used by S. aureus and more broadly underscore the importance of bacterial adaptations when faced with nutritional limitation.

摘要

硫辛酸是中间代谢所需的一种辅因子,它既可以从头合成,也可以从环境来源获取。细菌病原体金黄色葡萄球菌编码从头生物合成所需的酶,但也编码两种连接酶LplA1和LplA2,这两种酶足以在感染期间挽救硫辛酸。金黄色葡萄球菌还编码两种H蛋白,即甘氨酸裂解系统的GcvH和与LplA2在一个操纵子中编码的同源GcvH-L。GcvH是公认的将硫辛酰基转移至α-酮酸脱氢酶E2亚基的通道,而GcvH-L的功能尚不清楚。能够产生两种连接酶和两种H蛋白是金黄色葡萄球菌的一个不寻常特征,这与大多数其他革兰氏阳性厚壁菌不同,可能暗示该微生物中硫辛酸获取途径的扩展。在此,我们证明LplA1和LplA2通过差异靶向含硫辛酰结构域的蛋白促进硫辛酸的挽救;LplA1靶向H蛋白,LplA2靶向α-酮酸脱氢酶E2亚基。此外,GcvH和GcvH-L都促进硫辛酰基向E2亚基的传递。总之,这些研究确定了金黄色葡萄球菌使用的一种扩展的硫辛酸挽救模式,并更广泛地强调了细菌在面临营养限制时适应性的重要性。

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