The microbiota–gut–brain axis in Huntington's disease: pathogenic mechanisms and therapeutic targets

肠-脑轴 失调 亨廷顿病 肠道菌群 疾病 痴呆 神经科学 生物 生物信息学 医学 免疫学 内科学
作者
Millicent N. Ekwudo,Carolina Gubert,Anthony J. Hannan
出处
期刊:FEBS Journal [Wiley]
被引量:5
标识
DOI:10.1111/febs.17102
摘要

Huntington's disease (HD) is a currently incurable neurogenerative disorder and is typically characterized by progressive movement disorder (including chorea), cognitive deficits (culminating in dementia), psychiatric abnormalities (the most common of which is depression), and peripheral symptoms (including gastrointestinal dysfunction). There are currently no approved disease‐modifying therapies available for HD, with death usually occurring approximately 10–25 years after onset, but some therapies hold promising potential. HD subjects are often burdened by chronic diarrhea, constipation, esophageal and gastric inflammation, and a susceptibility to diabetes. Our understanding of the microbiota–gut–brain axis in HD is in its infancy and growing evidence from preclinical and clinical studies suggests a role of gut microbial population imbalance (gut dysbiosis) in HD pathophysiology. The gut and the brain can communicate through the enteric nervous system, immune system, vagus nerve, and microbiota‐derived‐metabolites including short‐chain fatty acids, bile acids, and branched‐chain amino acids. This review summarizes supporting evidence demonstrating the alterations in bacterial and fungal composition that may be associated with HD. We focus on mechanisms through which gut dysbiosis may compromise brain and gut health, thus triggering neuroinflammatory responses, and further highlight outcomes of attempts to modulate the gut microbiota as promising therapeutic strategies for HD. Ultimately, we discuss the dearth of data and the need for more longitudinal and translational studies in this nascent field. We suggest future directions to improve our understanding of the association between gut microbes and the pathogenesis of HD, and other ‘brain and body disorders’.
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