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肠道-脑轴调节与肠易激综合征进展之间相互作用过程中的分子信号传导:综述

Molecular signalling during cross talk between gut brain axis regulation and progression of irritable bowel syndrome: A comprehensive review.

作者信息

Singh Shiv Vardan, Ganguly Risha, Jaiswal Kritika, Yadav Aditya Kumar, Kumar Ramesh, Pandey Abhay K

机构信息

Department of Biochemistry, University of Allahabad, Allahabad (Prayagraj) 211002, Uttar Pradesh, India.

出版信息

World J Clin Cases. 2023 Jul 6;11(19):4458-4476. doi: 10.12998/wjcc.v11.i19.4458.

Abstract

Irritable bowel syndrome (IBS) is a chronic functional disorder which alters gastrointestinal (GI) functions, thus leading to compromised health status. Pathophysiology of IBS is not fully understood, whereas abnormal gut brain axis (GBA) has been identified as a major etiological factor. Recent studies are suggestive for visceral hyper-sensitivity, altered gut motility and dysfunctional autonomous nervous system as the main clinical abnormalities in IBS patients. Bidirectional signalling interactions among these abnormalities are derived through various exogenous and endogenous factors, such as microbiota population and diversity, microbial metabolites, dietary uptake, and psychological abnormalities. Strategic efforts focused to study these interactions including probiotics, antibiotics and fecal transplantations in normal and germ-free animals are clearly suggestive for the pivotal role of gut microbiota in IBS etiology. Additionally, neurotransmitters act as communication tools between enteric microbiota and brain functions, where serotonin (5-hydroxytryptamine) plays a key role in pathophysiology of IBS. It regulates GI motility, pain sense and inflammatory responses particular to mucosal and brain activity. In the absence of a better understanding of various interconnected crosstalks in GBA, more scientific efforts are required in the search of novel and targeted therapies for the management of IBS. In this review, we have summarized the gut microbial composition, interconnected signalling pathways and their regulators, available therapeutics, and the gaps needed to fill for a better management of IBS.

摘要

肠易激综合征(IBS)是一种慢性功能性疾病,会改变胃肠道(GI)功能,从而导致健康状况受损。IBS的病理生理学尚未完全明确,而异常的肠脑轴(GBA)已被确定为主要病因。最近的研究表明,内脏高敏感性、肠道动力改变和自主神经系统功能障碍是IBS患者的主要临床异常表现。这些异常之间的双向信号相互作用是通过各种外源性和内源性因素产生的,如微生物群的数量和多样性、微生物代谢产物、饮食摄入和心理异常。在正常动物和无菌动物中,致力于研究这些相互作用(包括益生菌、抗生素和粪便移植)的策略性努力清楚地表明了肠道微生物群在IBS病因学中的关键作用。此外,神经递质作为肠道微生物群与脑功能之间的通讯工具,其中血清素(5-羟色胺)在IBS的病理生理学中起关键作用。它调节胃肠道动力、痛觉以及对黏膜和脑活动特有的炎症反应。由于对GBA中各种相互关联的串扰缺乏更好的理解,因此需要更多的科学努力来寻找治疗IBS的新型靶向疗法。在这篇综述中,我们总结了肠道微生物组成、相互关联的信号通路及其调节因子、现有的治疗方法,以及为更好地管理IBS而需要填补的空白。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ab85/10353503/ae96e2c7f3fa/WJCC-11-4458-g001.jpg

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