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三磷酸柠檬酸裂解酶的结构和克雷布斯循环中柠檬酸合酶的起源。

Structure of ATP citrate lyase and the origin of citrate synthase in the Krebs cycle.

机构信息

Unit for Structural Biology, VIB Center for Inflammation Research, Ghent, Belgium.

Unit for Structural Biology, Department of Biochemistry and Microbiology, Ghent University, Ghent, Belgium.

出版信息

Nature. 2019 Apr;568(7753):571-575. doi: 10.1038/s41586-019-1095-5. Epub 2019 Apr 3.

DOI:10.1038/s41586-019-1095-5
PMID:30944476
Abstract

Across different kingdoms of life, ATP citrate lyase (ACLY, also known as ACL) catalyses the ATP-dependent and coenzyme A (CoA)-dependent conversion of citrate, a metabolic product of the Krebs cycle, to oxaloacetate and the high-energy biosynthetic precursor acetyl-CoA. The latter fuels pivotal biochemical reactions such as the synthesis of fatty acids, cholesterol and acetylcholine, and the acetylation of histones and proteins. In autotrophic prokaryotes, ACLY is a hallmark enzyme of the reverse Krebs cycle (also known as the reductive tricarboxylic acid cycle), which fixates two molecules of carbon dioxide in acetyl-CoA. In humans, ACLY links carbohydrate and lipid metabolism and is strongly expressed in liver and adipose tissue and in cholinergic neurons. The structural basis of the function of ACLY remains unknown. Here we report high-resolution crystal structures of bacterial, archaeal and human ACLY, and use distinct substrate-bound states to link the conformational plasticity of ACLY to its multistep catalytic itinerary. Such detailed insights will provide the framework for targeting human ACLY in cancer and hyperlipidaemia. Our structural studies also unmask a fundamental evolutionary relationship that links citrate synthase, the first enzyme of the oxidative Krebs cycle, to an ancestral tetrameric citryl-CoA lyase module that operates in the reverse Krebs cycle. This molecular transition marked a key step in the evolution of metabolism on Earth.

摘要

在不同的生命王国中,三磷酸腺苷柠檬酸裂解酶 (ACLY,也称为 ACL) 催化三磷酸腺苷依赖性和辅酶 A (CoA) 依赖性柠檬酸转化为草酰乙酸和高能生物合成前体乙酰辅酶 A。后者为关键的生化反应提供燃料,如脂肪酸、胆固醇和乙酰胆碱的合成,以及组蛋白和蛋白质的乙酰化。在自养原核生物中,ACLY 是逆向克雷布斯循环(也称为还原三羧酸循环)的标志性酶,该循环将两个二氧化碳分子固定在乙酰辅酶 A 中。在人类中,ACLY 连接碳水化合物和脂质代谢,在肝脏和脂肪组织以及胆碱能神经元中强烈表达。ACLY 功能的结构基础仍然未知。在这里,我们报告了细菌、古细菌和人类 ACLY 的高分辨率晶体结构,并使用不同的底物结合状态将 ACLY 的构象可塑性与其多步催化途径联系起来。这些详细的见解将为靶向人类 ACLY 治疗癌症和高脂血症提供框架。我们的结构研究还揭示了一种基本的进化关系,将柠檬酸合酶,即氧化克雷布斯循环的第一酶,与在逆向克雷布斯循环中起作用的原始四聚体柠檬酸-CoA 裂解酶模块联系起来。这种分子转变标志着地球代谢进化的关键一步。

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