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转录调节因子PhoP中的突变导致结核分枝杆菌H37Ra菌株的无毒力。

Mutation in the transcriptional regulator PhoP contributes to avirulence of Mycobacterium tuberculosis H37Ra strain.

作者信息

Lee Jong Seok, Krause Roland, Schreiber Jörg, Mollenkopf Hans-Joachim, Kowall Jane, Stein Robert, Jeon Bo-Young, Kwak Jeong-Yeon, Song Min-Kyong, Patron Juan Pablo, Jorg Sabine, Roh Kyoungmin, Cho Sang-Nae, Kaufmann Stefan H E

机构信息

Department of Immunology, Max Planck Institute for Infection Biology, Charitéplatz 1, 10117 Berlin, Germany.

出版信息

Cell Host Microbe. 2008 Feb 14;3(2):97-103. doi: 10.1016/j.chom.2008.01.002.

Abstract

Attenuated strains of mycobacteria can be exploited to determine genes essential for their pathogenesis and persistence. To this goal, we sequenced the genome of H37Ra, an attenuated variant of Mycobacterium tuberculosis H37Rv strain. Comparison with H37Rv revealed three unique coding region polymorphisms. One polymorphism was located in the DNA-binding domain of the transcriptional regulator PhoP, causing the protein's diminished DNA-binding capacity. Temporal gene expression profiles showed that several genes with reduced expression in H37Ra were also repressed in an H37Rv phoP knockout strain. At later time points, genes of the dormancy regulon, typically expressed in a state of nonreplicating persistence, were upregulated in H37Ra. Complementation of H37Ra with H37Rv phoP partially restored its persistence in a murine macrophage infection model. Our approach demonstrates the feasibility of identifying minute but distinct differences between isogenic strains and illustrates the consequences of single point mutations on the survival stratagem of M. tuberculosis.

摘要

减毒分枝杆菌菌株可用于确定其致病和持续存在所必需的基因。为实现这一目标,我们对结核分枝杆菌H37Rv菌株的减毒变体H37Ra的基因组进行了测序。与H37Rv的比较揭示了三个独特的编码区多态性。其中一个多态性位于转录调节因子PhoP的DNA结合结构域,导致该蛋白的DNA结合能力减弱。时间基因表达谱显示,在H37Ra中表达降低的几个基因在H37Rv phoP基因敲除菌株中也受到抑制。在后期时间点,通常在非复制性持续存在状态下表达的休眠调节子基因在H37Ra中上调。用H37Rv phoP对H37Ra进行互补在小鼠巨噬细胞感染模型中部分恢复了其持续性。我们的方法证明了识别同基因菌株之间微小但明显差异的可行性,并说明了单点突变对结核分枝杆菌生存策略的影响。

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