A Cascade of Microbiota-Leaky Gut-Inflammation- Is it a Key Player in Metabolic Disorders?

IF 9.5 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

Current Obesity Reports Pub Date : 2025-04-10 DOI:10.1007/s13679-025-00624-0

Sidharth Mishra, Shalini Jain, Bryan Agadzi, Hariom Yadav

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Abstract

Purpose of review: This review addresses critical gaps in knowledge and provides a literature overview of the molecular pathways connecting gut microbiota dysbiosis to increased intestinal permeability (commonly referred to as "leaky gut") and its contribution to metabolic disorders. Restoring a healthy gut microbiota holds significant potential for enhancing intestinal barrier function and metabolic health. These interventions offer promising therapeutic avenues for addressing leaky gut and its associated pathologies in metabolic syndrome.

Recent findings: In metabolic disorders such as obesity and type 2 diabetes (T2D), beneficial microbes such as those producing short-chain fatty acids (SCFAs) and other key metabolites like taurine, spermidine, glutamine, and indole derivatives are reduced. Concurrently, microbes that degrade toxic metabolites such as ethanolamine also decline, while proinflammatory, lipopolysaccharide (LPS)-enriched microbes increase. These microbial shifts place a higher burden on intestinal epithelial cells, which are in closest proximity to the gut lumen, inducing detrimental changes that compromise the structural and functional integrity of the intestinal barrier. Such changes include exacerbation of tight junction protein (TJP)s dysfunction, particularly through mechanisms such as destabilization of zona occludens (Zo)-1 mRNA or post-translational modifications. Emerging therapeutic strategies including ketogenic and Mediterranean diets, as well as probiotics, prebiotics, synbiotics, and postbiotics have demonstrated efficacy in restoring beneficial microbial populations, enhancing TJP expression and function, supporting gut barrier integrity, reducing leaky gut and inflammation, and ultimately improving metabolic disorders. This review summarizes the mechanisms by which gut microbiota contribute to the development of leaky gut and inflammation associated with metabolic syndrome. It also explores strategies for restoring gut microbiota balance and functionality by promoting beneficial microbes, increasing the production of beneficial metabolites, clearing toxic metabolites, and reducing the proportion of proinflammatory microbes. These approaches can alleviate the burden on intestinal epithelial cells, reduce leaky gut and inflammation, and improve metabolic health.

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微生物群渗漏的肠道炎症级联-它是代谢紊乱的关键因素吗？

综述目的：本综述解决了知识上的关键空白，并提供了连接肠道微生物群失调与肠道通透性增加（通常称为“漏肠”）的分子途径及其对代谢紊乱的贡献的文献综述。恢复健康的肠道微生物群对增强肠道屏障功能和代谢健康具有重要的潜力。这些干预措施为解决代谢综合征中的肠漏及其相关病理提供了有希望的治疗途径。最近发现：在代谢紊乱如肥胖和2型糖尿病（T2D）中，有益微生物如产生短链脂肪酸（SCFAs）和其他关键代谢物如牛磺酸、亚精胺、谷氨酰胺和吲哚衍生物的有益微生物减少。同时，降解有毒代谢物（如乙醇胺）的微生物也减少，而促炎、富含脂多糖（LPS）的微生物增加。这些微生物的转移给肠上皮细胞带来了更高的负担，而肠上皮细胞离肠腔最近，诱发了有害的变化，损害了肠屏障的结构和功能完整性。这些变化包括紧密连接蛋白（TJP）功能障碍的加剧，特别是通过诸如关闭带(Zo)-1 mRNA的不稳定或翻译后修饰等机制。新兴的治疗策略，包括生酮饮食和地中海饮食，以及益生菌、益生元、合成菌和后生菌，已经证明在恢复有益微生物种群、增强TJP表达和功能、支持肠道屏障完整性、减少肠道渗漏和炎症，并最终改善代谢紊乱方面具有功效。本文综述了肠道微生物群促进代谢综合征相关肠漏和炎症发展的机制。它还探讨了通过促进有益微生物，增加有益代谢物的产生，清除有毒代谢物和减少促炎微生物比例来恢复肠道微生物群平衡和功能的策略。这些方法可以减轻肠上皮细胞的负担，减少肠漏和炎症，改善代谢健康。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Current Obesity Reports Medicine-General Medicine

CiteScore

16.40

自引率

1.10%

发文量

期刊介绍： The main objective of Current Obesity Reports is to provide expert review articles on recent advancements in the interdisciplinary field of obesity research. Our aim is to offer clear, insightful, and balanced contributions that will benefit all individuals involved in the treatment and prevention of obesity, as well as related conditions such as cardiovascular diseases, endocrine disorders, gynecological issues, cancer, mental health, respiratory complications, and rheumatological diseases. We strive to redefine the way knowledge is expressed and provide organized content for the benefit of our readership.