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马里巴马科一线抗结核治疗期间抗生素相关微生物组改变的代谢和免疫后果

Metabolic and immune consequences of antibiotic related microbiome alterations during first-line tuberculosis treatment in Bamako, Mali.

作者信息

Diallo Dramane, Sun Shan, Somboro Anou M, Baya Bocar, Koné Amadou, Diarra Bassirou, Nantoumé Mohamed, Koloma Isaac, Diakite Mahamadou, Holl Jane, Maiga Almoustapha Issiaka, Seydi Moussa, Theron Grant, Hou Lifang, Fodor Anthony, Maiga Mamoudou

机构信息

University Clinical Research Center (UCRC), Bamako, Mali.

Department of Bioinformatics and Genomics, University of North Carolina at Charlotte, Charlotte, NC, United States.

出版信息

Front Immunol. 2025 May 14;16:1561459. doi: 10.3389/fimmu.2025.1561459. eCollection 2025.

Abstract

BACKGROUND

Individuals with a history of tuberculosis (TB) treatment are at a higher risk of experiencing a recurrent episode of the disease. Previous cross-sectional studies identified a connection between dysbiosis (alterations) in the gut microbiota composition and the administration of first-line TB antibiotics. However, these studies have not successfully elucidated this dysbiosis's resulting metabolic and immune consequences.

METHODS

In a longitudinal assessment, we studied the antituberculosis drug-related changes in the gut microbiota's composition and the resulting functional consequences. Sputum for TB culture, peripheral blood for metabolomics and cytokines analysis, and stool for shotgun metagenomics were collected from TB participants at Month-0, Month-2, Month-6 of treatment, and 9 Months after treatment (Month-15). Healthy controls were sampled at Month-0 and Month-6.

FINDINGS

We found notable differences in gut microbiota between individuals with TB and healthy controls. While gut microbiota tended to resemble healthy controls at the end of TB treatment, significant differences for many taxa persisted up to Month-15. Concurrently, disturbances in plasma metabolites, including tryptophan, tricarboxylic acids, and cytokine levels were observed. Certain fatty acids associated with inflammation pathways negatively correlated with the abundance of several taxa.

CONCLUSION

We observed alterations in the gut microbiota composition and function during treatment and at Month-15. Numerous changes in bacterial taxa abundances and inflammation-linked metabolites did not reverse at Month-15. This study suggests potential influences of anti-TB drugs and the gut microbiome on the disease outcome, response to treatment, and resistance to future TB infections.

摘要

背景

有结核病(TB)治疗史的个体发生疾病复发的风险更高。先前的横断面研究确定了肠道微生物群组成的生态失调(改变)与一线抗结核抗生素的使用之间存在联系。然而,这些研究尚未成功阐明这种生态失调所导致的代谢和免疫后果。

方法

在一项纵向评估中,我们研究了抗结核药物相关的肠道微生物群组成变化及其产生的功能后果。在治疗的第0个月、第2个月、第6个月以及治疗后9个月(第15个月)从结核病参与者中收集用于结核培养的痰液、用于代谢组学和细胞因子分析的外周血以及用于鸟枪法宏基因组学分析的粪便。在第0个月和第6个月对健康对照进行采样。

研究结果

我们发现结核病患者与健康对照的肠道微生物群存在显著差异。虽然在结核病治疗结束时肠道微生物群趋于类似于健康对照,但许多分类群的显著差异一直持续到第15个月。同时,观察到血浆代谢物(包括色氨酸、三羧酸)和细胞因子水平的紊乱。某些与炎症途径相关的脂肪酸与几个分类群的丰度呈负相关。

结论

我们观察到在治疗期间和第15个月时肠道微生物群的组成和功能发生了改变。细菌分类群丰度和与炎症相关的代谢物的许多变化在第15个月时并未逆转。这项研究表明抗结核药物和肠道微生物群对疾病结局、治疗反应以及未来结核感染的抵抗力可能产生影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3746/12116645/c217bb44f3bb/fimmu-16-1561459-g001.jpg

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