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Metabolic and metagenomic outcomes from early-life pulsed antibiotic treatment

机译:早期脉冲抗生素治疗的代谢和宏基因组结果

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Mammalian species have co-evolved with intestinal microbial communities that can shape development and adapt to environmental changes, including antibiotic perturbation or nutrient flux. In humans, especially children, microbiota disruption is common, yet the dynamic microbiome recovery from early-life antibiotics is still uncharacterized. Here we use a mouse model mimicking paediatric antibiotic use and find that therapeutic-dose pulsed antibiotic treatment (PAT) with a beta-lactam or macrolide alters both host and microbiota development. Early-life PAT accelerates total mass and bone growth, and causes progressive changes in gut microbiome diversity, population structure and metagenomic content, with microbiome effects dependent on the number of courses and class of antibiotic. Whereas control microbiota rapidly adapts to a change in diet, PAT slows the ecological progression, with delays lasting several months with previous macrolide exposure. This study identifies key markers of disturbance and recovery, which may help provide therapeutic targets for microbiota restoration following antibiotic treatment.
机译:哺乳动物物种与肠道微生物群落共同进化,可以塑造发育并适应环境变化,包括抗生素扰动或营养通量。在人类尤其是儿童中,微生物群破坏很常见,但是从早期生命的抗生素中动态恢复微生物组的特征仍然未知。在这里,我们使用模仿小儿抗生素使用的小鼠模型,发现使用β-内酰胺或大环内酯的治疗剂量脉冲抗生素治疗(PAT)会同时改变宿主和微生物群的发育。生命早期的PAT加速了总质量和骨骼的生长,并导致肠道微生物组多样性,种群结构和宏基因组学含量的逐步改变,微生物组的作用取决于疗程的数量和抗生素的种类。对照微生物群可以迅速适应饮食的变化,而PAT可以减缓生态进程,并且与以前的大环内酯类药物接触会持续数月。这项研究确定了干扰和恢复的关键标志,这可能有助于为抗生素治疗后微生物群的恢复提供治疗目标。

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