结合代谢组学和 16S rRNA 测序研究粪便微生物群移植干预对衰老小鼠的影响

Tianxin Zhu , Ling Yang , Zhizhong Luo , Jiqian He , Xuefeng Xu , Duosheng Luo
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引用次数: 0

摘要

衰老是一个复杂的生理过程,伴随着导致衰老的代谢和免疫紊乱。衰老过程会导致肠道微生物群发生巨大变化。然而,关于肠道微生物群在衰老过程中的机理作用的证据却很有限。我们将年轻(4 个月)或年老(22 个月)的供体小鼠的粪便微生物群移植到年老(22 个月)或年轻(4 个月)的受体小鼠体内。接受年轻供体肠道微生物群的老年小鼠逆转了血清和问题中与衰老相关的炎症,老年小鼠的自发活动、站立时间、跌倒次数和潜伏时间等行为特征也得到了缓解。相反,接受老年供体肠道微生物群的年轻小鼠会促进炎症的发展,并加剧衰老的行为特征。在老年小鼠体内,Odoribacter、Flexispira、Veillonella 和 Prevotellaceae_Prevotella 的相对丰度显著增加,而在接受年轻供体肠道微生物群的老年小鼠体内,这种变化被逆转。吲哚丙烯酸、LPC(18:1/0:0)、LPC(15:0/0:0)、LPC(0:0/15:0)等代谢物上调,黄嘌呤、肌苷、别嘌呤醇、N6-甲基腺苷代谢物下调。老年小鼠接受年轻供体肠道微生物群后,这些代谢物的变化也发生了逆转。对微生物群、代谢物和炎症细胞因子之间相关性的分析表明,吲哚丙烯酸、LPC(18:1/0:0)、LPC(15:0/0:0)和 LPC(0:0/15:0)与阿德勒克鲁兹菌呈负相关,而与维氏菌、普雷沃特菌、链球菌和奥德菌呈正相关。1-甲基肌苷、L-甲基腺苷、别嘌呤醇和 N6-甲基腺苷与脱硫弧菌呈正相关,而与 Veillonella 和 Prevotellaceae_Prevotella 呈负相关。吲哚丙烯酸与 TGF-β 呈负相关。LPC(18:1/0:0)、LPC(15:0/0:0)和 LPC(0:0/15:0)与 IL-10 呈正相关。1-甲基肌苷、L-甲基腺苷、N6-甲基腺苷和肌苷与 IL-6 和 LPS 呈负相关。我们的研究结果表明,调节肠道微生物组可能是一种促进健康老龄化的适当治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Combining metabolomics and 16S rRNA sequencing to investigate the effects of fecal microbiota transplantation intervention in aging mice

Aging is a complex physiological process, accompanied by metabolic and immune disorders leading to aging. The aging process yields dramatic alterations in the gut microbiota. However, there is limited evidence for a mechanistic role of the gut microbiota in aging processes. We conducted fecal microbiota transplantation from either young (4 months) or aged (22 months) donor mice into aged recipient mice (22 months) or young (4 months). Aged mice receiving young donor gut microbiota reversed aging-associated inflammation in serum and issues, and the behavioral characteristics with spontaneous activities, standing times, the number of falls, and the latency time in aged mice were alleviated. Conversely, young mice receiving aged donor gut microbiota promoted the development of inflammation, and the behavioral characteristics of aging were intensified. The relative abundance of Odoribacter, Flexispira, Veillonella, and Prevotellaceae_Prevotella were significantly enriched in aged mice, while changes were reversed in aged mice receiving young donor gut microbiota. The metabolites including indole acrylic acid, LPC (18:1/0:0), LPC (15:0/0:0), LPC (0:0/15:0) were up-regulated, and xanthine, inosine, allopurinol, N6-methyladenosine metabolites were down-regulated. After aged mice receiving young donor gut microbiota, these metabolite changes were reversed too. Analysis of the correlation between the microbiota, metabolites, and inflammatory cytokines showed indoleacrylic acid, LPC (18:1/0:0), LPC (15:0/0:0), and LPC (0:0/15:0) were negatively associated with Adlercreutzia, while positively correlated with Veillonella, Prevotellaceae_Prevotella, Streptococcus, and Odoribacter. 1-methylinosine, L-methyladenosine, allopurinol, and N6-methyladenosine were positively correlated with Desulfovibrio, and negatively correlated with Veillonella and Prevotellaceae_Prevotella. Indoleacrylic acid was negatively correlated with TGF-β. LPC (18:1/0:0), LPC (15:0/0:0), and LPC (0:0/15:0) were positively correlated with IL-10. 1-methylinosine, L-methyladenosine, N6-methyladenosine and inosine were negatively correlated with IL-6 and LPS. Our findings suggest that modulating the gut microbiome may be an appropriate treatment to promote healthy aging.

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