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PduM 蛋白是参与沙门氏菌属辅酶 B(12)依赖的 1,2-丙二醇降解的微隔间的结构组成部分。

The PduM protein is a structural component of the microcompartments involved in coenzyme B(12)-dependent 1,2-propanediol degradation by Salmonella enterica.

机构信息

Department of Biochemistry, Biophysics and Molecular Biology, Iowa State University, Ames, Iowa, USA.

出版信息

J Bacteriol. 2012 Apr;194(8):1912-8. doi: 10.1128/JB.06529-11. Epub 2012 Feb 17.

Abstract

Diverse bacteria use proteinaceous microcompartments (MCPs) to optimize metabolic pathways that have toxic or volatile intermediates. MCPs consist of metabolic enzymes encased within a protein shell that provides a defined environment. In Salmonella enterica, a MCP is involved in B(12)-dependent 1,2-propanediol utilization (Pdu MCP). In this report, we show that the protein PduM is required for the assembly and function of the Pdu MCP. The results of tandem mass spectrometry and Western blot analyses show that PduM is a component of the Pdu MCP. Electron microscopy shows that a pduM deletion mutant forms MCPs with abnormal morphology. Growth tests and metabolite measurements establish that a pduM deletion mutant is unable to form functional MCPs. PduM is unrelated in sequence to proteins of known function and hence may represent a new class of MCP structural proteins. We also report a modified protocol for the purification of Pdu MCP from Salmonella which allows isolation of milligram amounts of MCPs in about 4 h. We believe that this protocol can be extended or modified for the purification of MCPs from diverse bacteria.

摘要

多种细菌利用蛋白质微室(MCPs)来优化代谢途径,这些代谢途径的中间产物具有毒性或挥发性。MCPs 由包裹代谢酶的蛋白质外壳组成,为其提供了一个确定的环境。在沙门氏菌中,一种 MCP 参与 B(12)依赖性 1,2-丙二醇利用(Pdu MCP)。在本报告中,我们表明 PduM 蛋白是 Pdu MCP 组装和功能所必需的。串联质谱和 Western blot 分析的结果表明,PduM 是 Pdu MCP 的一个组成部分。电子显微镜显示,pduM 缺失突变体形成的 MCP 具有异常形态。生长试验和代谢物测量表明,pduM 缺失突变体无法形成功能性 MCPs。PduM 在序列上与已知功能的蛋白质没有关系,因此可能代表一类新的 MCP 结构蛋白。我们还报告了一种改良的从沙门氏菌中纯化 Pdu MCP 的方案,该方案允许在大约 4 小时内分离毫克量的 MCPs。我们相信,该方案可以扩展或修改,用于从不同细菌中纯化 MCPs。

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