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构建细菌世界的奇迹:复杂酶的生物合成

Constructing the wonders of the bacterial world: biosynthesis of complex enzymes.

作者信息

Sargent Frank

机构信息

Centre for Metalloprotein Spectroscopy and Biology, School of Biological Sciences, University of East Anglia, Norwich NR4 7TJ, UK.

出版信息

Microbiology (Reading). 2007 Mar;153(Pt 3):633-651. doi: 10.1099/mic.0.2006/004762-0.

Abstract

The prokaryotic cytoplasmic membrane not only maintains cell integrity and forms a barrier between the cell and its outside environment, but is also the location for essential biochemical processes. Microbial model systems provide excellent bases for the study of fundamental problems in membrane biology including signal transduction, chemotaxis, solute transport and, as will be the topic of this review, energy metabolism. Bacterial respiration requires a diverse array of complex, multi-subunit, cofactor-containing redox enzymes, many of which are embedded within, or located on the extracellular side of, the membrane. The biosynthesis of these enzymes therefore requires carefully controlled expression, assembly, targeting and transport processes. Here, focusing on the molybdenum-containing respiratory enzymes central to anaerobic respiration in Escherichia coli, recent descriptions of a chaperone-mediated 'proofreading' system involved in coordinating assembly and export of complex extracellular enzymes will be discussed. The paradigm proofreading chaperones are members of a large group of proteins known as the TorD family, and recent research in this area highlights common principles that underpin biosynthesis of both exported and non-exported respiratory enzymes.

摘要

原核生物的细胞质膜不仅维持细胞完整性,在细胞与其外部环境之间形成一道屏障,还是重要生化过程发生的场所。微生物模型系统为研究膜生物学的基本问题提供了绝佳基础,这些问题包括信号转导、趋化作用、溶质运输,以及(作为本综述的主题)能量代谢。细菌呼吸作用需要一系列多样的、复杂的、含多亚基和辅因子的氧化还原酶,其中许多酶嵌入膜内或位于膜的胞外侧。因此,这些酶的生物合成需要受到严格控制的表达、组装、靶向和运输过程。在此,聚焦于大肠杆菌厌氧呼吸核心的含钼呼吸酶,将讨论最近关于一种伴侣介导的“校对”系统的描述,该系统参与协调复杂胞外酶的组装和输出。典型的校对伴侣蛋白是一大类被称为TorD家族的蛋白质成员,该领域的最新研究突出了支撑输出型和非输出型呼吸酶生物合成的共同原则。

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