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Intestinal microbiota disruption limits the isoniazid mediated clearance of Mycobacterium tuberculosis in mice

机译:肠道微生物群干扰限制了异烟肼的分枝杆菌介导的间隙肺结核在老鼠身上

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Abstract Tuberculosis (TB) continues to remain a global threat due to the emergence of drug‐resistant Mycobacterium tuberculosis (Mtb) strains and toxicity associated with TB drugs. Intestinal microbiota has been reported to affect the host response to immunotherapy and drugs. However, how it affects the potency of first‐line TB drug isoniazid (INH) is largely unknown. Here, we examined the impact of gut microbial dysbiosis on INH efficiency to kill Mtb. In this study, we employed in vivo mouse model, pretreated with broad‐spectrum antibiotics (Abx) cocktail to disrupt their intestinal microbial population prior to Mtb infection and subsequent INH therapy. We demonstrated that microbiota disruption results in the impairment of INH‐mediated Mtb clearance, and aggravated TB‐associated tissue pathology. Further, it suppressed the innate immunity and reduced CD4 T‐cell response against Mtb. Interestingly, a distinct shift of gut microbial profile was noted with abundance of Enterococcus and reduction of Lactobacillus and Bifidobacterium population. Our results show that the intestinal microbiota is crucial determinant in efficacy of INH to kill Mtb and impacts the host immune response against infection. This work provides an intriguing insight into the potential links between host gut microbiota and potency of INH.
机译:摘要结核病继续保持由于出现的全球威胁药物检测耐药结核分枝杆菌(Mtb)菌株和毒性与抗结核药物有关。肠道微生物群的影响宿主免疫疗法和药物。然而,它如何影响效力的第一线结核病药物异烟肼(INH)在很大程度上是未知的。我们检查了肠道微生物生态失调的影响结核分枝杆菌异烟肼效率杀死。使用,体内小鼠模型广泛的光谱抗生素(Abx)鸡尾酒干扰他们的肠道微生物种群结核分枝杆菌在感染和随后的异烟肼治疗。中断导致的损伤结核分枝杆菌异烟肼量调节间隙,加剧结核病相关的组织病理学。抑制CD4细胞的先天免疫和减少结核分枝杆菌检测T细胞反应反对。不同的肠道微生物转移档案大量的肠球菌和减少乳酸菌和双歧杆菌的数量。结果表明,肠道菌群异烟肼杀死的效果的关键因素Mtb和影响宿主的免疫反应感染。了解潜在的宿主肠道之间的联系异烟肼的微生物群和效力。

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