胆汁酸
免疫系统
肠道菌群
血脂异常
免疫失调
免疫学
生物
淋巴细胞
脂质代谢
脱氧胆酸
医学
新陈代谢
内科学
先天免疫系统
失调
粪便
鹅去氧胆酸
T细胞
G蛋白偶联胆汁酸受体
作者
Jiayue Xia,Yinqi Shao,Bin Li,Tianyu Wu,Zhi He,Zhiyuan Feng,Ze Zhang,Shiyu Yin,Yuanyuan Wang,Junhui Yu,J.P. Wang,Guiju Sun
出处
期刊:iScience
[Cell Press]
日期:2025-11-11
卷期号:28 (12): 114001-114001
被引量:2
标识
DOI:10.1016/j.isci.2025.114001
摘要
B cells in patients with dyslipidemia, alongside increased specific bile acids in fecal samples and distinct alterations in gut microbiota composition. The animal model confirmed changes in gut microbiota, bile acid metabolism, and percentage of specific lymphocyte subsets. Also, we identified downregulated hepatic expressions of bile acid metabolism-related proteins in hyperlipidemic rats. Integrated analysis suggested potential associations among gut microbiota, bile acid pathways, and immune dysregulation. Overall, these data highlight the critical role of the potential gut microbiota-bile acid metabolism-immune axis in dyslipidemia, providing potential therapeutic targets for diseases associated with lipid metabolism disorders.
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