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The Regulation of Sulfur Metabolism in Mycobacterium tuberculosis

机译:结核分枝杆菌中硫代谢的调控

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摘要

Mycobacterium tuberculosis (Mtb) has evolved into a highly successful human pathogen. It deftly subverts the bactericidal mechanisms of alveolar macrophages, ultimately inducing granuloma formation and establishing long-term residence in the host. These hallmarks of Mtb infection are facilitated by the metabolic adaptation of the pathogen to its surrounding environment and the biosynthesis of molecules that mediate its interactions with host immune cells. The sulfate assimilation pathway of Mtb produces a number of sulfur-containing metabolites with important contributions to pathogenesis and survival. This pathway is regulated by diverse environmental cues and regulatory proteins that mediate sulfur transactions in the cell. Here, we discuss the transcriptional and biochemical mechanisms of sulfur metabolism regulation in Mtb and potential small molecule regulators of the sulfate assimilation pathway that are collectively poised to aid this intracellular pathogen in its expert manipulation of the host. From this global analysis, we have identified a subset of sulfur-metabolizing enzymes that are sensitive to multiple regulatory cues and may be strong candidates for therapeutic intervention.
机译:结核分枝杆菌(Mtb)已进化为高度成功的人类病原体。它巧妙地破坏了肺泡巨噬细胞的杀菌机制,最终诱导肉芽肿形成并在宿主中建立了长期居留权。病原体对周围环境的代谢适应以及介导其与宿主免疫细胞相互作用的分子的生物合成,促进了Mtb感染的这些标志。 Mtb的硫酸盐同化途径会产生许多含硫代谢物,这些代谢物对发病机理和生存都具有重要作用。该途径由介导细胞中硫交易的各种环境提示和调节蛋白调节。在这里,我们讨论了Mtb中硫代谢调节的转录和生化机制以及硫酸盐同化途径的潜在小分子调节剂,这些调节剂共同准备帮助该细胞内病原体对宿主进行专业操作。从这一全球分析中,我们已经确定了一个硫代谢酶子集,它对多种调节信号敏感,并且可能是治疗干预的强力候选者。

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