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非洲铁海棠素A通过调节针对分枝杆菌的宿主免疫反应来预防原发性和复发性结核病。

Withaferin A Protects against Primary and Recurrent Tuberculosis by Modulating Mycobacterium-Specific Host Immune Responses.

作者信息

Kumari Anjna, Pahuja Isha, Negi Kriti, Ghoshal Antara, Mukopadhyay Suparba, Agarwal Meetu, Mathew Babu, Maras Jaswinder Singh, Chaturvedi Shivam, Bhaskar Ashima, Dwivedi Ved Prakash

机构信息

Immunobiology Group, International Centre for Genetic Engineering and Biotechnology, New Delhi, India.

Department of Molecular Medicine, Jamia Hamdard University, New Delhi, India.

出版信息

Microbiol Spectr. 2023 Mar 14;11(2):e0058323. doi: 10.1128/spectrum.00583-23.

Abstract

The fate of Mycobacterium tuberculosis infection is governed by immune signaling pathways that can either eliminate the pathogen or result in tuberculosis (TB). Anti-TB therapy (ATT) is extensive and is efficacious only against active, drug-sensitive strains of M. tuberculosis. Due to severe side effects, ATT often causes impairment of host immunity, making it imperative to use novel immunotherapeutics for better clinical outcomes. In this study, we have explored the immunomodulatory potential of withaferin A (WA) as an immunotherapeutic against TB. Here, we demonstrate that WA can constrain intracellular drug-sensitive and -resistant strains of M. tuberculosis by augmenting host immune responses. We also established the potential of WA treatment in conjunction with isoniazid. We show that WA directs the host macrophages toward defensive M1 polarization and enhances T1 and T17 immune responses against M. tuberculosis infection. The reduced bacterial burden upon T cell adoptive transfer further corroborated the augmented T cell responses. Interestingly, WA stimulated the generation of T cell memory populations by instigating STAT signaling, thereby reducing the rate of TB recurrence due to reactivation and reinfection. We substantiate the prospects of WA as a potent adjunct immunomodulator that enriches protective memory cells by prompting STAT signaling and improves host defense against M. tuberculosis. Despite being extensive, conventional antituberculosis therapy (ATT) is barely proficient in providing sterile immunity to tuberculosis (TB). Failure to constrain the escalating global TB burden due to the emergence of drug-resistant bacterial strains and immune dampening effects of ATT necessitates adjunct immunotherapeutics for better clinical outcomes. We evaluated the prospects of withaferin A (WA), an active constituent of Withania somnifera, as an adjunct immunomodulator against diverse M. tuberculosis strains. WA efficiently restricts the progression of TB by stimulating antimycobacterial host responses, protective immune signaling, and activation of diverse immune cell populations. Protective effects of WA can be attributed to the enrichment of memory T cells by induction of STAT signaling, thereby enhancing resistance to reinfections and reactivation of disease. We ascertained the immunotherapeutic potential of WA in boosting host immune responses against M. tuberculosis.

摘要

结核分枝杆菌感染的转归受免疫信号通路的调控,这些通路要么能清除病原体,要么导致结核病(TB)。抗结核治疗(ATT)应用广泛,但仅对结核分枝杆菌的活跃、药物敏感菌株有效。由于严重的副作用,ATT常常会损害宿主免疫力,因此必须使用新型免疫疗法以获得更好的临床疗效。在本研究中,我们探索了睡茄内酯A(WA)作为抗结核免疫疗法的免疫调节潜力。在此,我们证明WA可通过增强宿主免疫反应来抑制细胞内结核分枝杆菌的药物敏感和耐药菌株。我们还确定了WA与异烟肼联合治疗的潜力。我们表明,WA可引导宿主巨噬细胞向防御性的M1极化,并增强针对结核分枝杆菌感染的T1和T17免疫反应。T细胞过继转移后细菌负荷的降低进一步证实了T细胞反应的增强。有趣的是,WA通过激活STAT信号来刺激T细胞记忆群体的产生,从而降低因再激活和再感染导致的结核病复发率。我们证实了WA作为一种有效的辅助免疫调节剂的前景,它通过激活STAT信号来富集保护性记忆细胞,并改善宿主对结核分枝杆菌的防御。尽管传统抗结核治疗(ATT)应用广泛,但在为结核病(TB)提供无菌免疫方面却几乎无能为力。由于耐药菌株的出现以及ATT的免疫抑制作用,未能控制不断上升的全球结核病负担,因此需要辅助免疫疗法以获得更好的临床疗效。我们评估了睡茄的活性成分睡茄内酯A(WA)作为针对多种结核分枝杆菌菌株的辅助免疫调节剂的前景。WA通过刺激抗分枝杆菌的宿主反应、保护性免疫信号以及多种免疫细胞群体的激活,有效地限制了结核病的进展。WA的保护作用可归因于通过诱导STAT信号来富集记忆T细胞,从而增强对再感染和疾病再激活的抵抗力。我们确定了WA在增强宿主针对结核分枝杆菌的免疫反应方面的免疫治疗潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8cf1/10100980/b396bb1be1dd/spectrum.00583-23-f002.jpg

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