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嗜肺军团菌DotB ATP酶的遗传分析揭示了其在IV型分泌系统蛋白输出中的作用。

Genetic analysis of the Legionella pneumophila DotB ATPase reveals a role in type IV secretion system protein export.

作者信息

Sexton Jessica A, Yeo Hye-Jeong, Vogel Joseph P

机构信息

Department of Molecular Microbiology, Washington University, Campus Box 8230, 660 S. Euclid Ave., St. Louis, MO 63110, USA.

出版信息

Mol Microbiol. 2005 Jul;57(1):70-84. doi: 10.1111/j.1365-2958.2005.04667.x.

Abstract

The pulmonary pathogen Legionella pneumophila uses the Dot/Icm type IV secretion system (T4SS) to replicate inside host cells. This apparatus translocates proteins into macrophages to alter their endocytic pathway and enable bacterial growth. Although the secretion ATPase DotB is critical for T4SS function, its specific role in type IV secretion remains undefined. Due to similarity to the VirB11 and PilT ATPases, DotB has been proposed to play a role in assembly of the T4SS, retraction of pili and/or export of substrates. With the goal of understanding the protein's function(s), we isolated and characterized 30 dotB alleles using a variety of phenotypic and biochemical assays. Twenty-four of these alleles possess several dot/icm mutant phenotypes, including a complete lack of intracellular replication, plasmid mobilization and contact-dependent cytotoxicity. These 24 non-functional alleles fall into three classes: those with a known biochemical defect, those with a predicted enzymatic defect and those with an unknown defect. Six other alleles display partial activity in dot/icm phenotypic assays, thus constituting a fourth class. Two mutants in this class are unable to export a subset of T4SS substrates, providing the first evidence for a DotB function in substrate export and suggesting a possible role in substrate selection.

摘要

肺部病原体嗜肺军团菌利用Dot/Icm IV型分泌系统(T4SS)在宿主细胞内进行复制。该装置将蛋白质转运到巨噬细胞中,以改变其胞吞途径并促进细菌生长。尽管分泌型ATP酶DotB对T4SS功能至关重要,但其在IV型分泌中的具体作用仍不明确。由于与VirB11和PilT ATP酶相似,有人提出DotB在T4SS的组装、菌毛回缩和/或底物输出中发挥作用。为了了解该蛋白的功能,我们使用多种表型和生化分析方法分离并鉴定了30个dotB等位基因。其中24个等位基因具有多种dot/icm突变表型,包括完全缺乏细胞内复制、质粒转移和接触依赖性细胞毒性。这24个无功能的等位基因分为三类:具有已知生化缺陷的、具有预测酶缺陷的和具有未知缺陷的。其他六个等位基因在dot/icm表型分析中显示出部分活性,因此构成第四类。该类中的两个突变体无法输出T4SS底物的一个子集,这为DotB在底物输出中的功能提供了首个证据,并暗示其在底物选择中可能发挥作用。

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