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理解和利用抗结核药物对宿主线粒体功能和生物能量的影响。

Understanding and Exploiting the Effect of Tuberculosis Antimicrobials on Host Mitochondrial Function and Bioenergetics.

机构信息

TB Immunology Group, Department of Clinical Medicine, Trinity Translational Medicine Institute, Trinity College Dublin, Dublin, Ireland.

出版信息

Front Cell Infect Microbiol. 2020 Sep 15;10:493. doi: 10.3389/fcimb.2020.00493. eCollection 2020.

Abstract

Almost 140 years after its discovery, tuberculosis remains the leading infectious cause of death globally. For half a century, patients with drug-sensitive and drug-resistant tuberculosis have undergone long, arduous, and complex treatment processes with several antimicrobials that primarily function through direct bactericidal activity. Long-term utilization of these antimicrobials has been well-characterized and associated with numerous toxic side-effects. With the prevalence of drug-resistant strains on the rise and new therapies for tuberculosis urgently required, a more thorough understanding of these antimicrobials is a necessity. In order to progress from the "one size fits all" treatment approach, understanding how these antimicrobials affect mitochondrial function and bioenergetics may provide further insight into how these drugs affect the overall functions of host immune cells during tuberculosis infection. Such insights may help to inform future studies, instigate discussion, and help toward establishing personalized approaches to using such antimicrobials which could help to pave the way for more tailored treatment regimens. While recent research has highlighted the important role mitochondria and bioenergetics play in infected host cells, only a small number of studies have examined how these antimicrobials affect mitochondrial function and immunometabolic processes within these immune cells. This short review highlights how these antimicrobials affect key elements of mitochondrial function, leading to further discussion on how they affect bioenergetic processes, such as glycolysis and oxidative phosphorylation, and how antimicrobial-induced alterations in these processes can be linked to downstream changes in inflammation, autophagy, and altered bactericidal activity.

摘要

尽管结核病被发现至今已近 140 年,但它仍然是全球首要的传染病死因。半个世纪以来,无论是对药物敏感的结核病患者还是耐药结核病患者,都要接受长期、艰苦和复杂的治疗过程,使用几种主要通过直接杀菌活性发挥作用的抗微生物药物。这些抗微生物药物的长期使用情况已得到充分研究,它们与许多毒副作用相关。随着耐药菌株的流行率不断上升,急需新的结核病疗法,因此更深入地了解这些抗微生物药物是必要的。为了从“一刀切”的治疗方法向前推进,了解这些抗微生物药物如何影响线粒体功能和生物能量学,可能有助于进一步了解这些药物如何影响宿主免疫细胞在结核病感染期间的整体功能。这些见解可能有助于为未来的研究提供信息,引发讨论,并有助于建立使用这些抗微生物药物的个性化方法,为更具针对性的治疗方案铺平道路。尽管最近的研究强调了线粒体和生物能量学在受感染宿主细胞中的重要作用,但只有少数研究检查了这些抗微生物药物如何影响这些免疫细胞中的线粒体功能和免疫代谢过程。本综述简要介绍了这些抗微生物药物如何影响线粒体功能的关键要素,并进一步讨论了它们如何影响糖酵解和氧化磷酸化等生物能量过程,以及这些过程中抗菌药物诱导的改变如何与下游炎症、自噬和杀菌活性改变相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/703b/7522306/7dd3a9a0bafc/fcimb-10-00493-g0001.jpg

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