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Inhibiting the stringent response blocks Mycobacterium tuberculosis entry into quiescence and reduces persistence

机译:抑制严格的反应可阻止结核分枝杆菌进入静止状态并减少持久性

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摘要

The stringent response enables Mycobacterium tuberculosis (Mtb) to shut down its replication and metabolism under various stresses. Here we show that Mtb lacking the stringent response enzyme RelMtb was unable to slow its replication rate during nutrient starvation. Metabolomics analysis revealed that the nutrient-starved relMtb-deficient strain had increased metabolism similar to that of exponentially growing wild-type bacteria in nutrient-rich broth, consistent with an inability to enter quiescence. Deficiency of relMtb increased the susceptibility of mutant bacteria to killing by isoniazid during nutrient starvation and in the lungs of chronically infected mice. We screened a pharmaceutical library of over 2 million compounds for inhibitors of RelMtb and showed that the lead compound X9 was able to directly kill nutrient-starved M. tuberculosis and enhanced the killing activity of isoniazid. Inhibition of RelMtb is a promising approach to target M. tuberculosis persisters, with the potential to shorten the duration of TB treatment.
机译:严格的响应使结核分枝杆菌(Mtb)在各种压力下都能关闭其复制和代谢。在这里,我们表明缺乏严格反应酶RelMtb的Mtb在营养饥饿期间无法减慢其复制速度。代谢组学分析表明,缺乏营养的relMtb缺陷菌株与富含营养的肉汤中指数生长的野生型细菌的代谢相似,这与无法进入静止状态一致。 relMtb的缺乏增加了营养缺乏和慢性感染小鼠肺部突变细菌对异烟肼杀死的敏感性。我们筛选了超过200万种化合物作为RelMtb抑制剂的药物库,结果表明前导化合物X9能够直接杀死营养不良的结核分枝杆菌并增强异烟肼的杀伤活性。抑制RelMtb是靶向结核分枝杆菌持续者的一种有前途的方法,具有缩短结核病治疗时间的潜力。

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