The role of the microbiota in glaucoma

IF 8.7 2区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Ling Huang , Yiwen Hong , Xiangyu Fu , Haishan Tan , Yongjiang Chen , Yujiao Wang , Danian Chen
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引用次数: 0

Abstract

Glaucoma is a common irreversible vision loss disorder because of the gradual loss of retinal ganglion cells (RGCs) and the optic nerve axons. Major risk factors include elder age and high intraocular pressure (IOP). However, high IOP is neither necessary nor sufficient to cause glaucoma. Some non-IOP signaling cascades can mediate RGC degeneration. In addition, gender, diet, obesity, depression, or anxiety also contribute to the development of glaucoma. Understanding the mechanism of glaucoma development is crucial for timely diagnosis and establishing new strategies to improve current IOP-reducing therapies. The microbiota exerts a marked influence on the human body during homeostasis and disease. Many glaucoma patients have abnormal compositions of the microbiota (dysbiosis) in multiple locations, including the ocular surface, intraocular cavity, oral cavity, stomach, and gut. Here, we discuss findings in the last ten years or more about the microbiota and metabolite changes in animal models, patients with three risk factors (aging, obesity, and depression), and glaucoma patients. Antigenic mimicry and heat stress protein (HSP)-specific T-cell infiltration in the retina may be responsible for commensal microbes contributing to glaucomatous RGC damage. LPS-TLR4 pathway may be the primary mechanism of oral and ocular surface dysbiosis affecting glaucoma. Microbe-derived metabolites may also affect glaucoma pathogenesis. Homocysteine accumulation, inflammatory factor release, and direct dissemination may link gastric H. pylori infection and anterior chamber viral infection (such as cytomegalovirus) to glaucoma. Potential therapeutic protocols targeting microbiota include antibiotics, modified diet, and stool transplant. Later investigations will uncover the underlying molecular mechanism connecting dysbiosis to glaucoma and its clinical applications in glaucoma management.

微生物群在青光眼中的作用。
青光眼是一种常见的不可逆性视力丧失障碍,因为视网膜神经节细胞(RGCs)和视神经轴突逐渐丧失。主要危险因素包括年龄较大和高眼压。然而,高IOP既不必要也不足以引起青光眼。一些非IOP信号级联可以介导RGC变性。此外,性别、饮食、肥胖、抑郁或焦虑也会导致青光眼的发展。了解青光眼发展的机制对于及时诊断和制定新的策略来改善目前的眼压降低治疗至关重要。微生物群在体内平衡和疾病期间对人体产生显著影响。许多青光眼患者在多个部位出现微生物群组成异常(微生态失调),包括眼表、眼内、口腔、胃和肠道。在这里,我们讨论了过去十年或更长时间内关于动物模型、有三种危险因素(衰老、肥胖和抑郁)的患者和青光眼患者的微生物群和代谢产物变化的研究结果。视网膜中的抗原拟态和热应激蛋白(HSP)特异性T细胞浸润可能是导致青光眼RGC损伤的共生微生物的原因。LPS-TLR4通路可能是口腔和眼表微生态失调影响青光眼的主要机制。微生物衍生的代谢产物也可能影响青光眼的发病机制。同型半胱氨酸积聚、炎症因子释放和直接传播可能将胃幽门螺杆菌感染和前房病毒感染(如巨细胞病毒)与青光眼联系起来。针对微生物群的潜在治疗方案包括抗生素、改良饮食和粪便移植。稍后的研究将揭示将微生态失调与青光眼联系起来的潜在分子机制及其在青光眼治疗中的临床应用。
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
Molecular Aspects of Medicine
Molecular Aspects of Medicine 医学-生化与分子生物学
CiteScore
18.20
自引率
0.00%
发文量
85
审稿时长
55 days
期刊介绍: Molecular Aspects of Medicine is a review journal that serves as an official publication of the International Union of Biochemistry and Molecular Biology. It caters to physicians and biomedical scientists and aims to bridge the gap between these two fields. The journal encourages practicing clinical scientists to contribute by providing extended reviews on the molecular aspects of a specific medical field. These articles are written in a way that appeals to both doctors who may struggle with basic science and basic scientists who may have limited awareness of clinical practice issues. The journal covers a wide range of medical topics to showcase the molecular insights gained from basic science and highlight the challenging problems that medicine presents to the scientific community.
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