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首页> 外文期刊>Nature Microbiology >Antibiotic-mediated gut microbiome perturbation accelerates development of type 1 diabetes in mice
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Antibiotic-mediated gut microbiome perturbation accelerates development of type 1 diabetes in mice

机译:抗生素介导的肠道微生物组扰动可加速小鼠1型糖尿病的发展

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The early life microbiome plays important roles in host immunological and metabolic development. Because the incidence of type 1 diabetes (T1D) has been increasing substantially in recent decades, we hypothesized that early-life antibiotic use altersgut microbiota, which predisposes to disease. Using non-obese diabetic mice that are genetically susceptible to T1D, we examined the effects of exposure to either continuous low-dose antibiotics or pulsed therapeutic antibiotics (PAT) early in life, mimicking childhood exposures. We found that in mice receiving PAT, T1D incidence was significantly higher, and microbial community composition and structure differed compared with controls. In pre-diabetic male PAT mice, the intestinal lamina propria had lower Th17 and Treg proportions and intestinal SAA expression than in controls, suggesting key roles in transducing the altered microbiota signals. PAT affected microbial lipid metabolism and host cholesterol biosynthetic gene expression. These findings show that early-life antibiotic treatments alter the gut microbiota and its metabolic capacities, intestinal gene expression and T-cell populations, accelerating T1D onset in non-obese diabetic mice.
机译:早期微生物组在宿主免疫和代谢发育中起重要作用。由于近几十年来1型糖尿病(T1D)的发病率已大大增加,因此我们假设早期使用抗生素会改变易感染微生物的菌群。我们使用对T1D具有遗传易感性的非肥胖糖尿病小鼠,检查了生命早期暴露于连续小剂量抗生素或脉冲治疗性抗生素(PAT)的影响,模仿了儿童期的暴露。我们发现在接受PAT的小鼠中,T1D发生率显着更高,并且微生物群落的组成和结构与对照组相比有所不同。在糖尿病前期雄性PAT小鼠中,固有层肠固有层的Th17和Treg比例以及肠道SAA表达均低于对照组,表明在转导改变的微生物群信号中起关键作用。 PAT影响微生物脂质代谢和宿主胆固醇生物合成基因表达。这些发现表明,早期生命的抗生素治疗会改变肠道微生物群及其代谢能力,肠道基因表达和T细胞数量,从而加速非肥胖糖尿病小鼠的T1D发作。

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