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APOE genotype influences the gut microbiome structure and function in humans and mice: relevance for Alzheimer’s disease pathophysiology

机译: APOE 基因型影响人类和小鼠肠道微生物组的结构和功能:与阿尔茨海默氏病病理生理学的相关性

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Apolipoprotein E ( APOE ) genotype is the strongest prevalent genetic risk factor for Alzheimer’s disease (AD). Numerous studies have provided insights into the pathologic mechanisms. However, a comprehensive understanding of the impact of APOE genotype on microflora speciation and metabolism is completely lacking. In this study, we investigated the association between APOE genotype and the gut microbiome composition in human and APOE –targeted replacement (TR) transgenic mice. Fecal microbiota amplicon sequencing from matched individuals with different APOE genotypes revealed no significant differences in overall microbiota diversity in group-aggregated human APOE genotypes. However, several bacterial taxa showed significantly different relative abundance between APOE genotypes. Notably, we detected an association of Prevotellaceae and Ruminococcaceae and several butyrate-producing genera abundances with APOE genotypes. These findings were confirmed by comparing the gut microbiota of APOE -TR mice. Furthermore, metabolomic analysis of murine fecal water detected significant differences in microbe-associated amino acids and short-chain fatty acids between APOE genotypes. Together, these findings indicate that APOE genotype is associated with specific gut microbiome profiles in both humans and APOE -TR mice. This suggests that the gut microbiome is worth further investigation as a potential target to mitigate the deleterious impact of the APOE4 allele on cognitive decline and the prevention of AD.—Tran, T. T. T., Corsini, S., Kellingray, L., Hegarty, C., Le Gall, G., Narbad, A., Müller, M., Tejera, N., O’Toole, P. W., Minihane, A.-M., Vauzour, D. APOE genotype influences the gut microbiome structure and function in humans and mice: relevance for Alzheimer’s disease pathophysiology.
机译:载脂蛋白E(APOE)基因型是阿尔茨海默氏病(AD)最强的流行遗传危险因素。许多研究提供了对病理机制的见解。但是,完全缺乏对APOE基因型对微生物区系形成和代谢的影响的全面了解。在这项研究中,我们调查了人类和APOE靶向替代(TR)转基因小鼠中APOE基因型与肠道微生物组组成之间的关联。从具有不同APOE基因型的匹配个体进行的粪便微生物群扩增子测序显示,在群体聚集的人类APOE基因型中,总体微生物群多样性没有显着差异。但是,几种细菌类群显示APOE基因型之间的相对丰度显着不同。值得注意的是,我们检测到了前藻科和Ruminococcaceae以及一些与APOE基因型相关的产生丁酸酯的属。通过比较APOE -TR小鼠的肠道菌群,证实了这些发现。此外,对小鼠粪便水的代谢组学分析发现,APOE基因型之间的微生物相关氨基酸和短链脂肪酸存在显着差异。总之,这些发现表明,在人和APOE-TR小鼠中,APOE基因型均与特定的肠道微生物组谱相关。这表明肠道微生物组作为减轻APOE4等位基因对认知能力下降和AD的有害影响的潜在目标值得进一步研究。-Tran,TTT,Corsini,S.,Kellingray,L.,Hegarty,C 。,Le Gall,G.,Narbad,A.,Müller,M.,Tejera,N.,O'Toole,PW,Minihane,A.-M.,Vauzour,D.APOE基因型影响肠道微生物组的结构和功能在人类和小鼠中:与阿尔茨海默氏病病理生理学的相关性。

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