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(p)ppGpp与严谨反应:对抗生素治疗的新威胁

(p)ppGpp and the Stringent Response: An Emerging Threat to Antibiotic Therapy.

作者信息

Hobbs Joanne K, Boraston Alisdair B

机构信息

Department of Biochemistry and Microbiology , University of Victoria , 3800 Finnerty Road , Victoria , BC V8P 5C2 , Canada.

出版信息

ACS Infect Dis. 2019 Sep 13;5(9):1505-1517. doi: 10.1021/acsinfecdis.9b00204. Epub 2019 Jul 22.

Abstract

In 1969, Cashel and Gallant first observed the presence of (p)ppGpp-the signaling molecule of the stringent response-in starved bacterial cells. Fifty years later, (p)ppGpp and the stringent response have emerged as essential master regulators of not only the bacterial response to stress but also almost all aspects of bacterial physiology, virulence, and immune evasion. More worryingly, a wealth of data now indicate that (p)ppGpp and stringent response activation pose a serious threat to the efficacy and clinical success of antimicrobial therapy. Here, we focus on the central role that (p)ppGpp and the stringent response play in the phenomenon of antibiotic tolerance, as well as the acquisition, development, and expression of antibiotic resistance. We review these consequences of stringent response activation in relation to the main proteins involved in (p)ppGpp production and control, in particular the complex interplay between monofunctional and bifunctional long RelA/SpoT homologues (RSHs) and small alarmone synthetases (SASs). We also review the growing evidence to suggest that there are multiple other indirect pathways of stringent response induction that can affect antibiotic efficacy. Finally, we summarize recent studies that indicate the and clinical impact of (p)ppGpp production on antibiotic treatment outcomes. We conclude by reviewing the progress to date in the search for novel therapeutics that target the stringent response.

摘要

1969年,卡舍尔和加兰特首次在饥饿的细菌细胞中观察到(p)ppGpp——严紧反应的信号分子——的存在。五十年后,(p)ppGpp和严紧反应不仅已成为细菌应激反应的重要主调控因子,还几乎是细菌生理学、毒力和免疫逃逸各个方面的重要主调控因子。更令人担忧的是,现在大量数据表明,(p)ppGpp和严紧反应激活对抗菌治疗的疗效和临床成功构成了严重威胁。在此,我们聚焦于(p)ppGpp和严紧反应在抗生素耐受性现象以及抗生素耐药性的获得、发展和表达中所起的核心作用。我们回顾严紧反应激活的这些后果,涉及参与(p)ppGpp产生和调控的主要蛋白质,特别是单功能和双功能长RelA/SpoT同源物(RSHs)与小警报素合成酶(SASs)之间复杂的相互作用。我们还回顾越来越多的证据表明存在多种其他诱导严紧反应的间接途径,它们会影响抗生素疗效。最后,我们总结近期研究,这些研究表明(p)ppGpp产生对抗生素治疗结果的影响及临床意义。我们通过回顾迄今为止在寻找针对严紧反应的新型疗法方面取得的进展来得出结论。

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