硫肽抗生素通过影响宿主和微生物对细胞内病原体表现出双重作用模式。

Chemistry & biology Pub Date : 2015-08-20 Epub Date: 2015-07-23 DOI:10.1016/j.chembiol.2015.06.019
Qingfei Zheng, Qinglan Wang, Shoufeng Wang, Jiequn Wu, Qian Gao, Wen Liu
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引用次数: 57

摘要

硫链霉素(TSR)是一种典型的硫肽类抗生素,其侧环系统中含有一个醌酸(QA)片段。根据已知的TSR靶向细菌核糖体的机制,我们最近设计并生物合成了几种具有不同QA取代的TSR衍生物。利用这些硫肽抗生素治疗细胞内病原体海洋分枝杆菌,我们在此报道了一种新的TSRs作用模式,它诱导内质网应激介导的自噬以增强宿主细胞防御。这种对QA基团修饰敏感的细胞内反应是消除细胞内病原体的间接但不可忽视的机制。因此,据我们所知,tsr是唯一一种对寄生细菌和受感染宿主细胞具有双重作用的抗生素。新观察到的TSRs机制可能会通过考虑宿主反应来启发细胞内病原体治疗的未来变化。
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Thiopeptide Antibiotics Exhibit a Dual Mode of Action against Intracellular Pathogens by Affecting Both Host and Microbe.

Thiostrepton (TSR) is an archetypal thiopeptide antibiotic possessing a quinaldic acid (QA) moiety in the side ring system. According to the mechanism of TSR previously known to target bacterial ribosome, we recently designed and biosynthesized several TSR derivatives that varied in QA substitution. Utilizing these thiopeptide antibiotics to treat the intracellular pathogen Mycobacterium marinum, we herein report a novel mode of action of TSRs, which induce ER stress-mediated autophagy to enhance host cell defense. This intracellular response, which is sensitive to the modification of the QA group, serves as an indirect but unignorable mechanism for eliminating intracellular pathogens. TSRs are thus the only type of antibiotics, to our knowledge, with the dual action on both the parasitic bacteria and the infected host cells. The newly observed mechanism of TSRs may inspire the future change in the treatment of intracellular pathogens, by taking host response into account.

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来源期刊
Chemistry & biology
Chemistry & biology 生物-生化与分子生物学
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审稿时长
4-8 weeks
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