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II型脂肪酸合成的机制多样性与调控

Mechanistic diversity and regulation of Type II fatty acid synthesis.

作者信息

Marrakchi H, Zhang Y M, Rock C O

机构信息

Department of Infectious Diseases, Protein Science Division, St Jude Children's Research Hospital, Memphis, TN 38105, USA.

出版信息

Biochem Soc Trans. 2002 Nov;30(Pt 6):1050-5. doi: 10.1042/bst0301050.

DOI:10.1042/bst0301050
PMID:12440970
Abstract

Fatty acid biosynthesis is catalysed in most bacteria by a group of highly conserved proteins known as the Type II fatty acid synthase (FAS) system. The Type II system organization is distinct from its mammalian counterpart and offers several unique sites for selective inhibition by antibacterial agents. There has been remarkable progress in the understanding of the genetics, biochemistry and regulation of Type II FASs. One important advance is the discovery of the interaction between the fatty acid degradation regulator, FadR, and the fatty acid biosynthesis regulator, FabR, in the transcriptional control of unsaturated fatty acid synthesis in Escherichia coli. The availability of genomic sequences and high-resolution protein crystal structures has expanded our understanding of Type II FASs beyond the E. coli model system to a number of pathogens. The molecular diversity among the pathway enzymes is illustrated by the discovery of a new type of enoyl-reductase in Streptococcus pneumoniae [enoyl-acyl carrier protein (ACP) reductase II, FabK], the presence of two enoyl-reductases in Bacillus subtilis (enoyl-ACP reductases I and III, FabI and FabL), and the use of a new mechanism for unsaturated fatty acid formation in S. pneumoniae ( trans -2- cis -3-enoyl-ACP isomerase, FabM). The solution structure of ACP from Mycobacterium tuberculosis revealed features common to all ACPs, but its extended C-terminal domain may reflect a specific interaction with very-long-chain intermediates.

摘要

在大多数细菌中,脂肪酸生物合成由一组高度保守的蛋白质催化,这些蛋白质被称为II型脂肪酸合酶(FAS)系统。II型系统的组织形式与其哺乳动物对应物不同,为抗菌剂的选择性抑制提供了几个独特的位点。在对II型FAS的遗传学、生物化学和调控的理解方面取得了显著进展。一个重要的进展是发现了脂肪酸降解调节因子FadR与脂肪酸生物合成调节因子FabR之间在大肠杆菌不饱和脂肪酸合成转录控制中的相互作用。基因组序列和高分辨率蛋白质晶体结构的可得性将我们对II型FAS的理解从大肠杆菌模型系统扩展到了许多病原体。肺炎链球菌中新型烯酰还原酶[烯酰 - 酰基载体蛋白(ACP)还原酶II,FabK]的发现、枯草芽孢杆菌中两种烯酰还原酶(烯酰 - ACP还原酶I和III,FabI和FabL)的存在以及肺炎链球菌中不饱和脂肪酸形成的新机制(反式 - 2 - 顺式 - 3 - 烯酰 - ACP异构酶,FabM)说明了该途径酶之间的分子多样性。结核分枝杆菌ACP的溶液结构揭示了所有ACP共有的特征,但其延伸的C末端结构域可能反映了与超长链中间体的特定相互作用。

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