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Piericidin A1 Blocks Yersinia Ysc Type III Secretion System Needle Assembly

机译:Piericidin A1阻止耶尔森氏菌Ysc III型分泌系统针头组装

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The type III secretion system (T3SS) is a bacterial virulence factor expressed by dozens of Gram-negative pathogens but largely absent from commensals. The T3SS is an attractive target for antimicrobial agents that may disarm pathogenic bacteria while leaving commensal populations intact. We previously identified piericidin A1 as an inhibitor of the Ysc T3SS in Yersinia pseudotuberculosis . Piericidins were first discovered as inhibitors of complex I of the electron transport chain in mitochondria and some bacteria. However, we found that piericidin A1 did not alter Yersinia membrane potential or inhibit flagellar motility powered by the proton motive force, indicating that the piericidin mode of action against Yersinia type III secretion is independent of complex I. Instead, piericidin A1 reduced the number of T3SS needle complexes visible by fluorescence microscopy at the bacterial surface, preventing T3SS translocator and effector protein secretion. Furthermore, piericidin A1 decreased the abundance of higher-order YscF needle subunit complexes, suggesting that piericidin A1 blocks YscF needle assembly. While expression of T3SS components in Yersinia are positively regulated by active type III secretion, the block in secretion by piericidin A1 was not accompanied by a decrease in T3SS gene expression, indicating that piericidin A1 may target a T3SS regulatory circuit. However, piericidin A1 still inhibited effector protein secretion in the absence of the T3SS regulator YopK, YopD, or YopN. Surprisingly, while piericidin A1 also inhibited the Y.?enterocolitica Ysc T3SS, it did not inhibit the SPI-1 family Ysa T3SS in Y.?enterocolitica or the Ysc family T3SS in Pseudomonas aeruginosa . Together, these data indicate that piericidin A1 specifically inhibits Yersinia Ysc T3SS needle assembly. IMPORTANCE The bacterial type III secretion system (T3SS) is widely used by both human and animal pathogens to cause disease yet remains incompletely understood. Deciphering how some natural products, such as the microbial metabolite piericidin, inhibit type III secretion can provide important insight into how the T3SS functions or is regulated. Taking this approach, we investigated the ability of piericidin to block T3SS function in several human pathogens. Surprisingly, piericidin selectively inhibited the Ysc family T3SS in enteropathogenic Yersinia but did not affect the function of a different T3SS within the same species. Furthermore, piericidin specifically blocked the formation of T3SS needles on the bacterial surface without altering the localization of several other T3SS components or regulation of T3SS gene expression. These data show that piericidin targets a mechanism important for needle assembly that is unique to the Yersinia Ysc T3SS.
机译:III型分泌系统(T3SS)是一种细菌毒力因子,由数十种革兰氏阴性病原体表达,但在共患病中却很缺乏。 T3SS是抗微生物剂的诱人靶标,这些抗微生物剂可解除病原细菌的武装,同时保持完整种群。我们以前确定了Piericidin A1是假质耶尔森氏菌Ysc T3SS的抑制剂。最早发现Piericidins是线粒体和某些细菌中电子传输链的复合物I的抑制剂。然而,我们发现piericidin A1不会改变质膜耶尔森菌的膜电位或抑制由质子动力驱动的鞭毛运动,这表明piericidin A1对耶尔森氏菌III型分泌的作用方式独立于复合物I。 T3SS针状复合物可在细菌表面通过荧光显微镜观察到,从而阻止了T3SS易位子和效应蛋白的分泌。此外,piericidin A1降低了高阶YscF针亚基复合物的丰度,表明Piericidin A1阻止了YscF针的组装。虽然耶尔森氏菌中T3SS成分的表达受到活性III型分泌的正向调控,但Piericidin A1的分泌阻滞并未伴随T3SS基因表达的降低,这表明Piericidin A1可能靶向于T3SS调控回路。但是,在缺乏T3SS调节剂YopK,YopD或YopN的情况下,piericidin A1仍然抑制效应蛋白的分泌。出人意料的是,尽管piericidin A1也抑制了肠炎耶尔森氏菌Ysc T3SS,但它并没有抑制铜绿假单胞菌中的SPI-1家族Ysa T3SS或铜绿假单胞菌的Ysc家族T3SS。这些数据一起表明,piericidin A1特异性抑制耶尔森氏菌Ysc T3SS针头组装。重要信息细菌III型分泌系统(T3SS)已被人类和动物病原体广泛用于引起疾病,但尚未完全了解。了解某些天然产物(例如微生物代谢物Piericidin)如何抑制III型分泌可以为T3SS的功能或调节方式提供重要的见解。采用这种方法,我们研究了piericidin阻断几种人类病原体中T3SS功能的能力。出人意料的是,piericidin在肠道致病性耶尔森氏菌中选择性抑制Ysc家族T3SS,但不影响同一物种中不同T3SS的功能。此外,piericidin特异地阻止了细菌表面上T3SS针的形成,而没有改变其他几种T3SS组件的定位或T3SS基因表达的调节。这些数据表明,piericidin靶向了一种针对耶尔森氏菌Ysc T3SS独特的针头组装重要机制。

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