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跨越细菌细胞包膜的大分子组装与分泌:II型蛋白质分泌系统

Macromolecular assembly and secretion across the bacterial cell envelope: type II protein secretion systems.

作者信息

Russel M

机构信息

Rockefeller University, New York, NY 10021, USA.

出版信息

J Mol Biol. 1998 Jun 12;279(3):485-99. doi: 10.1006/jmbi.1998.1791.

DOI:10.1006/jmbi.1998.1791
PMID:9641973
Abstract

A decade ago, Pugsley and colleagues reported the existence of a large region of Klebsiella DNA, distinct from the Klebsiella gene encoding pullulanase, which was necessary for secretion of this enzyme to the cell surface in Escherichia coli (d'Enfert et al., 1987a,b). The pul genes it contained proved to be the tip of an iceberg. The sequences reported before 1992 (d'Enfert et al., 1987a,b; d'Enfert & Pugsley, 1989; Pugsley & Reyss, 1990; Reyss & Pugsley, 1990) included only one gene (pulD) that matched any sequence in the data base; a 220 amino acid residue segment of PulD was 32% identical with a portion of the filamentous phage-encoded protein, pIV. But by the time the sequence of the 18.8 kb DNA fragment that contained the pul genes had been completed (Possot et al., 1992), reports of sets of homologous genes in several species of Gram-negative plant and animal pathogens had appeared. For the most part, these gene clusters were cloned by their ability to complement mutants that produced, but failed to secrete, proteins normally found in the extracellular milieu; when tested, the mutants showed reduced pathogenicity or were totally avirulent. The secreted proteins included hydrolytic enzymes such as cellulase and pectinase from plant pathogens, and proteases and toxins from animal pathogens. The multi-gene family necessary for secretion of these enzymes is now known as the type II system or the main terminal branch (MTB) of the general secretion pathway (GSP). As summarized by Pugsley et al. (1997), the current tally includes type II systems from Klebsiella oxytoca (pul), Erwinia chrysanthemi and carotovora (out), Xanthomonas campestris (xps), Pseudomonas aeruginosa (xcp), Aeromonas hydrophila (exe), and Vibrio cholerae (eps). A second type II system (sps) necessary for deposition of the S-layer on the cell surface in A. hydrophila is more similar to the X. campestris than A. hydrophila genes (Thomas & Trust, 1995). The biggest surprise has been the discovery of a complete set of type II secretion genes in E. coli K12. The E. coli genes are not expressed under normal growth conditions, and a search is underway to find inducing conditions and secretion substrates (Francetic & Pugsley, 1996). Impressive progress has already been made in defining components of the pathway. What remains to be understood in mechanistic detail is how this protein secretion system functions.

摘要

十年前,普格斯利及其同事报告称,存在一大段肺炎克雷伯菌DNA区域,它与编码支链淀粉酶的肺炎克雷伯菌基因不同,该区域是这种酶分泌到大肠杆菌细胞表面所必需的(登费尔特等人,1987a、b)。结果证明,它所含的pul基因只是冰山一角。1992年之前报告的序列(登费尔特等人,1987a、b;登费尔特和普格斯利,1989;普格斯利和雷伊斯,1990;雷伊斯和普格斯利,1990)中,只有一个基因(pulD)与数据库中的任何序列匹配;PulD的一段220个氨基酸残基片段与丝状噬菌体编码蛋白pIV的一部分有32%的同一性。但到包含pul基因的18.8 kb DNA片段序列完成时(波索特等人,1992),已出现了几种革兰氏阴性植物和动物病原体中同源基因集的报告。在大多数情况下,这些基因簇是通过其互补突变体的能力克隆的,这些突变体能够产生但无法分泌通常存在于细胞外环境中的蛋白质;经测试,这些突变体的致病性降低或完全无毒。分泌的蛋白质包括植物病原体的水解酶,如纤维素酶和果胶酶,以及动物病原体的蛋白酶和毒素。这些酶分泌所必需的多基因家族现在被称为II型系统或一般分泌途径(GSP)的主要末端分支(MTB)。如普格斯利等人(1997)所总结的,目前统计的包括产酸克雷伯菌(pul)、菊欧文氏菌和胡萝卜软腐欧文氏菌(out)、野油菜黄单胞菌(xps)、铜绿假单胞菌(xcp)、嗜水气单胞菌(exe)和霍乱弧菌(eps)的II型系统。嗜水气单胞菌中S层沉积到细胞表面所必需的第二种II型系统(sps)与野油菜黄单胞菌的基因比与嗜水气单胞菌的基因更相似(托马斯和特拉斯特,1995)。最大的惊喜是在大肠杆菌K12中发现了一整套II型分泌基因。大肠杆菌基因在正常生长条件下不表达,目前正在寻找诱导条件和分泌底物(弗朗塞蒂克和普格斯利,1996)。在确定该途径的组成部分方面已经取得了令人瞩目的进展。在机制细节方面仍有待理解的是这个蛋白质分泌系统是如何发挥作用的。

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