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运动重塑与阿克曼氏菌相关的类花生酸代谢以减轻肠道衰老:多组学见解

Exercise Remodels Akkermansia-Associated Eicosanoid Metabolism to Alleviate Intestinal Senescence: Multi-Omics Insights.

作者信息

Yu Chunxia, Liu Xuanyu, Li Yitong, Li Silin, Huang Yating, Liu Sujuan, Shao Heng, Shen Yanna, Fu Li

机构信息

School of Medical Technology, Tianjin Medical University, Tianjin 300070, China.

School of Basic Medical Science, Tianjin Medical University, Tianjin 300070, China.

出版信息

Microorganisms. 2025 Jun 13;13(6):1379. doi: 10.3390/microorganisms13061379.

Abstract

Aerobic exercise mitigates age-related intestinal senescence through gut microbiota modulation, but the underlying mechanism has remained unclear. In this study, we performed 16S rRNA sequencing of gut contents from young, old, and old exercise C57BL/6J mice to assess exercise-induced alterations in microbiota community structure. Differential taxa analyses were applied to reveal age-associated bacterial signatures, gut barrier integrity, and systemic inflammation. Additionally, untargeted metabolomic profiling was employed to characterize gut metabolic profiles and reveal the key pathways through differential metabolite enrichment analyses. Aging significantly exacerbated the senescence-associated secretory phenotypes and the overgrowth of pathogenic bacteria in mice. However, aerobic exercise ameliorated these age-related deteriorations, restored gut microbial homeostasis, and reduced intestinal permeability. Notably, exercise intervention led to a significant increase in Akkermansia abundance in feces, establishing this mucin-degrading bacterium as a prominent exercise-responsive microbe. Metabolomic profiling identified eicosanoid metabolism as the most significantly perturbed pathway, and chronic exercise was found to regulate 14,15-Dhet levels. Our multi-omics integration confirmed that exercise is a potent modulator of the gut-microbiota-metabolite axis during aging. Elucidating the "Akkermansia-eicosanoid signaling" axis provided mechanistic insights into how exercise promotes healthy aging, identifying novel targets for anti-aging strategies via microbiota.

摘要

有氧运动通过调节肠道微生物群减轻与年龄相关的肠道衰老,但其潜在机制尚不清楚。在本研究中,我们对年轻、老年和老年运动的C57BL/6J小鼠的肠道内容物进行了16S rRNA测序,以评估运动引起的微生物群落结构变化。应用差异分类群分析来揭示与年龄相关的细菌特征、肠道屏障完整性和全身炎症。此外,采用非靶向代谢组学分析来表征肠道代谢谱,并通过差异代谢物富集分析揭示关键途径。衰老显著加剧了小鼠衰老相关的分泌表型和病原菌的过度生长。然而,有氧运动改善了这些与年龄相关的衰退,恢复了肠道微生物稳态,并降低了肠道通透性。值得注意的是,运动干预导致粪便中阿克曼氏菌丰度显著增加,使这种粘蛋白降解细菌成为一种显著的运动反应性微生物。代谢组学分析确定类花生酸代谢是最受干扰的途径,并且发现长期运动可调节14,15-二羟基二十碳四烯酸(14,15-Dhet)水平。我们的多组学整合证实,运动是衰老过程中肠道微生物群-代谢物轴的有效调节因子。阐明“阿克曼氏菌-类花生酸信号”轴为运动如何促进健康衰老提供了机制性见解,为通过微生物群的抗衰老策略确定了新的靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0853/12195349/6cb99ff55ee4/microorganisms-13-01379-g001.jpg

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