肠道微生物组和类风湿关节炎之间的分子模拟:目前的概念。

Q1 Medicine
Anandanarayan Muruganandam, Filippo Migliorini, Naveen Jeyaraman, Raju Vaishya, Sangeetha Balaji, Swaminathan Ramasubramanian, Nicola Maffulli, Madhan Jeyaraman
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引用次数: 0

摘要

类风湿性关节炎(RA)是一种受遗传和环境因素共同影响的自身免疫性疾病,其中肠道微生物组(GMB)是影响其发生的环境因素之一。RA患者GMB的组成明显改变,其特征是多样性减少和明显的细菌改变。GMB由生活在胃肠道内的大约35000种细菌组成,作为人类健康和疾病发病机制的关键贡献者,已经引起了相当大的关注。本文深入探讨了GMB在RA背景下的复杂参与。口腔- gmb轴强调了细菌在RA发病机制中的复杂作用,细菌通过分子模拟产生瓜氨酸化蛋白(ACPAs)抗体。生态失调影响Tregs、细胞因子水平和RA疾病活动性,表明调节细胞因子可能是控制RA炎症的一种策略。GMB还对药物反应和毒性具有重要意义,从而产生了药物组微生物学领域。微生物群的组成可以影响药物的疗效和毒性,而微生物群的代谢物可以影响药物反应。最近的研究已经确定了与类风湿性关节炎相关的特定细菌、代谢物和免疫反应,为个性化治疗提供了潜在的目标。然而,一些挑战,包括微生物组成的变化,建立因果关系,考虑混杂因素,并将研究结果转化为临床实践,需要解决。微生物组靶向治疗仍处于早期阶段,需要进一步研究和标准化才能有效实施。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Molecular Mimicry Between Gut Microbiome and Rheumatoid Arthritis: Current Concepts.

Rheumatoid arthritis (RA) represents an autoimmune condition impacted by a combination of genetic and environmental factors, with the gut microbiome (GMB) being one of the influential environmental factors. Patients with RA display notable modifications in the composition of their GMB, characterised by decreased diversity and distinct bacterial alterations. The GMB, comprising an extensive array of approximately 35,000 bacterial species residing within the gastrointestinal tract, has garnered considerable attention as a pivotal contributor to both human health and the pathogenesis of diseases. This article provides an in-depth exploration of the intricate involvement of the GMB in the context of RA. The oral-GMB axis highlights the complex role of bacteria in RA pathogenesis by producing antibodies to citrullinated proteins (ACPAs) through molecular mimicry. Dysbiosis affects Tregs, cytokine levels, and RA disease activity, suggesting that regulating cytokines could be a strategy for managing inflammation in RA. The GMB also has significant implications for drug responses and toxicity, giving rise to the field of pharmacomicrobiomics. The composition of the microbiota can impact the efficacy and toxicity of drugs, while the microbiota's metabolites can influence drug response. Recent research has identified specific bacteria, metabolites, and immune responses associated with RA, offering potential targets for personalised management. However, several challenges, including the variation in microbial composition, establishing causality, accounting for confounding factors, and translating findings into clinical practice, need to be addressed. Microbiome-targeted therapy is still in its early stages and requires further research and standardisation for effective implementation.

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