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细菌中的磷脂酸合成

Phosphatidic acid synthesis in bacteria.

作者信息

Yao Jiangwei, Rock Charles O

机构信息

Department of Infectious Diseases, St. Jude Children's Research Hospital, Memphis, USA.

出版信息

Biochim Biophys Acta. 2013 Mar;1831(3):495-502. doi: 10.1016/j.bbalip.2012.08.018. Epub 2012 Aug 30.

DOI:10.1016/j.bbalip.2012.08.018
PMID:22981714
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3548993/
Abstract

Membrane phospholipid synthesis is a vital facet of bacterial physiology. Although the spectrum of phospholipid headgroup structures produced by bacteria is large, the key precursor to all of these molecules is phosphatidic acid (PtdOH). Glycerol-3-phosphate derived from the glycolysis via glycerol-phosphate synthase is the universal source for the glycerol backbone of PtdOH. There are two distinct families of enzymes responsible for the acylation of the 1-position of glycerol-3-phosphate. The PlsB acyltransferase was discovered in Escherichia coli, and homologs are present in many eukaryotes. This protein family primarily uses acyl-acyl carrier protein (ACP) endproducts of fatty acid synthesis as acyl donors, but may also use acyl-CoA derived from exogenous fatty acids. The second protein family, PlsY, is more widely distributed in bacteria and utilizes the unique acyl donor, acyl-phosphate, which is produced from acyl-ACP by the enzyme PlsX. The acylation of the 2-position is carried out by members of the PlsC protein family. All PlsCs use acyl-ACP as the acyl donor, although the PlsCs of the γ-proteobacteria also may use acyl-CoA. Phospholipid headgroups are precursors in the biosynthesis of other membrane-associated molecules and the diacylglycerol product of these reactions is converted to PtdOH by one of two distinct families of lipid kinases. The central importance of the de novo and recycling pathways to PtdOH in cell physiology suggest that these enzymes are suitable targets for the development of antibacterial therapeutics in Gram-positive pathogens. This article is part of a Special Issue entitled Phospholipids and Phospholipid Metabolism.

摘要

膜磷脂合成是细菌生理学的一个重要方面。尽管细菌产生的磷脂头部基团结构种类繁多,但所有这些分子的关键前体都是磷脂酸(PtdOH)。通过甘油 - 3 - 磷酸合酶从糖酵解衍生而来的甘油 - 3 - 磷酸是PtdOH甘油骨架的普遍来源。有两个不同的酶家族负责甘油 - 3 - 磷酸1位的酰化。PlsB酰基转移酶在大肠杆菌中被发现,其同源物存在于许多真核生物中。这个蛋白质家族主要使用脂肪酸合成的酰基 - 酰基载体蛋白(ACP)终产物作为酰基供体,但也可能使用源自外源脂肪酸的酰基辅酶A。第二个蛋白质家族PlsY在细菌中分布更广泛,利用独特的酰基供体酰基 - 磷酸,它由PlsX酶从酰基 - ACP产生。2位的酰化由PlsC蛋白质家族的成员进行。所有的PlsC都使用酰基 - ACP作为酰基供体,尽管γ - 变形菌的PlsC也可能使用酰基辅酶A。磷脂头部基团是其他膜相关分子生物合成的前体,这些反应的二酰甘油产物通过两个不同的脂质激酶家族之一转化为PtdOH。从头合成和循环途径对细胞生理学中PtdOH的核心重要性表明,这些酶是革兰氏阳性病原体抗菌治疗药物开发的合适靶点。本文是名为“磷脂与磷脂代谢”的特刊的一部分。

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