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High-Fat Diet Induces Dysbiosis of Gastric Microbiota Prior to Gut Microbiota in Association With Metabolic Disorders in Mice

机译:高脂饮食会导致肠道菌群代谢失调先于肠道菌群与小鼠代谢紊乱有关。

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摘要

Accumulating evidence suggests that high-fat diet (HFD) induced metabolic disorders are associated with dysbiosis of gut microbiota. However, no study has explored the effect of HFD on the gastric microbiota. This study established the HFD animal model to determine the impact of HFD on the gastric microbiota and its relationship with the alterations of gut microbiota. A total of 40 male C57BL/6 mice were randomly allocated to receive a standard chow diet (CD) or HFD for 12 weeks (12CD group and 12HFD group) and 24 weeks (24CD group and 24HFD group) (n = 10 mice per group). Body weight and length were measured and Lee’s index was calculated at different time points. The insulin sensitivity and serum levels of metabolic parameters including blood glucose, insulin and lipid were also evaluated. The gastric mucosa and fecal microbiota of mice were characterized by 16S rRNA gene sequencing. The body weight was much heavier and the Lee’s index was higher in 24HFD group than 12HFD. The insulin resistance and serum level of lipid were increased in 24HFD group compared to 12HFD, indicating the aggravation of metabolic disorders as HFD went on. 16S rRNA gene sequencing showed dysbiosis of gastric microbiota with decreased community diversity while no significant alteration in gut microbiota after 12 weeks of HFD. The phyla Firmicutes and Proteobacteria tended to increase whereas Bacteroidetes and Verrucomicrobia decrease in the gastric microbiota of 12HFD mice compared to 12CD. Moreover, a remarkable reduction of bacteria especially Akkermansia muciniphila, which has beneficial effects on host metabolism, was observed firstly in the stomach of 12HFD group and then in the gut of 24HFD group, indicating the earlier alterations of microbiota in stomach than gut after HFD. We also found structural segregation of microbiota in the stomach as well as gut between 12HFD and 24HFD group, which is accompanied by the aggregation of metabolic disorders. These data suggest that HFD affects not only gut microbiota but also gastric microbiota and the disruption of microbial ecosystem in the digestive tract may play a part in the development and progression of metabolic diseases although molecular mechanism requires further investigation.
机译:越来越多的证据表明,高脂饮食(HFD)引起的代谢紊乱与肠道菌群的营养不良有关。但是,没有研究探索HFD对胃微生物群的影响。本研究建立了HFD动物模型,以确定HFD对胃微生物群的影响及其与肠道微生物群变化的关系。随机将40只雄性C57BL / 6小鼠随机分配到12周(12CD组和12HFD组)和24周(24CD组和24HFD组)接受标准食物(CD)或HFD(n =每组10只小鼠) )。测量体重和身长,并在不同时间点计算李氏指数。还评估了胰岛素敏感性和包括血糖,胰岛素和脂质在内的代谢参数的血清水平。通过16S rRNA基因测序对小鼠的胃黏膜和粪便微生物群进行了表征。 24HFD组的体重较12HFD重,Lee指数更高。与12HFD相比,24HFD组的胰岛素抵抗和血脂水平升高,表明随着HFD的进行,代谢紊乱加剧。 16S rRNA基因测序显示,HFD 12周后,胃菌群营养不良,群落多样性降低,而肠道菌群无明显改变。与12CD相比,12HFD小鼠的胃菌群中的菌毛和变形杆菌趋于增加,而拟杆菌和Verrucomicrobia则减少。此外,首先在12HFD组的胃中然后在24HFD组的肠中观察到细菌特别是对阿克曼克氏菌(Akkermansia muciniphila)的细菌显着减少,这对宿主代谢具有有益作用,这表明HFD后,胃中微生物群的改变比肠道早。我们还发现胃和12HFD和24HFD组之间的肠道中微生物群的结构性分离,伴随着代谢紊乱的聚集。这些数据表明,HFD不仅影响肠道微生物群,而且影响胃微生物群,并且消化道中微生物生态系统的破坏可能在代谢疾病的发生和发展中起作用,尽管分子机制需要进一步研究。

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