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嗜肺军团菌的PilT同源物DotB具有ATP酶活性,这对其细胞内生长至关重要。

The Legionella pneumophila PilT homologue DotB exhibits ATPase activity that is critical for intracellular growth.

作者信息

Sexton Jessica A, Pinkner Jerome S, Roth Robyn, Heuser John E, Hultgren Scott J, Vogel Joseph P

机构信息

Department of Molecular Microbiology, Washington University, St. Louis, Missouri 63110, USA.

出版信息

J Bacteriol. 2004 Mar;186(6):1658-66. doi: 10.1128/JB.186.6.1658-1666.2004.

Abstract

The ability of Legionella pneumophila to grow and cause disease in the host is completely dependent on a type IV secretion system known as the Dot/Icm complex. This membrane-spanning apparatus translocates effector molecules into host cells in a process that is poorly understood but that is known to require the putative ATPase DotB. One possible role for DotB is suggested by its similarity to the PilT family of proteins, which mediate pilus retraction. To better understand the molecular behavior of DotB, we have purified the protein and shown that it forms stable homohexameric rings and hydrolyzes ATP with a specific activity of 6.4 nmol of ATP/min/mg of protein. ATPase activity is critical to the function of DotB, as alteration of the conserved Walker box lysine residue resulted in a mutant protein, DotB K162Q, which failed to bind or hydrolyze ATP and which could not complement a DeltadotB strain for intracellular growth in macrophages. Consistent with the ability of DotB to interact with itself, the dotBK162Q allele exhibited transdominance over wild-type dotB, providing the first example of such a mutation in L. pneumophila. Finally, the DotB K162Q mutant protein had a significantly enhanced membrane localization in L. pneumophila compared to wild-type DotB, suggesting a relationship between nucleotide binding and membrane association. These results are consistent with a model in which DotB cycles between the cytoplasm and the Dot/Icm complex at the membrane, where it hydrolyzes nucleotides to provide energy to the complex.

摘要

嗜肺军团菌在宿主体内生长并致病的能力完全依赖于一种名为Dot/Icm复合体的IV型分泌系统。这种跨膜装置将效应分子转运到宿主细胞中,这一过程目前了解甚少,但已知需要假定的ATP酶DotB。DotB与介导菌毛回缩的PilT蛋白家族相似,这提示了DotB的一种可能作用。为了更好地理解DotB的分子行为,我们纯化了该蛋白,结果表明它形成稳定的同六聚体环,并以6.4 nmol ATP/分钟/毫克蛋白的比活性水解ATP。ATP酶活性对DotB的功能至关重要,因为保守的沃克盒赖氨酸残基的改变产生了一种突变蛋白DotB K162Q,它无法结合或水解ATP,并且不能在巨噬细胞的细胞内生长中互补缺失DotB的菌株。与DotB自身相互作用的能力一致,dotBK162Q等位基因对野生型dotB表现出反式显性,这是嗜肺军团菌中此类突变的首个例子。最后,与野生型DotB相比,DotB K162Q突变蛋白在嗜肺军团菌中的膜定位显著增强,这表明核苷酸结合与膜结合之间存在关联。这些结果与一个模型一致,即DotB在细胞质和膜上的Dot/Icm复合体之间循环,在那里它水解核苷酸为复合体提供能量。

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