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Consumption of a Western-Style Diet Modulates the Response of the Murine Gut Microbiome to Ciprofloxacin

机译:西式饮食的消耗调节小鼠肠道微生物组的反应至环丙沙星

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Dietary composition and antibiotic use have major impacts on the structure and function of the gut microbiome, often resulting in dysbiosis. Despite this, little research has been done to explore the role of host diet as a determinant of antibiotic-induced microbiome disruption. Here, we utilize a multi-omic approach to characterize the impact of Western-style diet consumption on ciprofloxacin-induced changes to gut microbiome structure and transcriptional activity. We found that Western diet consumption dramatically increased Bacteroide s abundances and shifted the community toward the metabolism of simple sugars and mucus glycoproteins. Mice consuming a Western-style diet experienced a greater expansion of Firmicutes following ciprofloxacin treatment than those eating a control diet. Transcriptionally, we found that ciprofloxacin reduced the abundance of tricarboxylic acid (TCA) cycle transcripts on both diets, suggesting that carbon metabolism plays a key role in the response of the gut microbiome to this antibiotic. Despite this, we observed extensive diet-dependent differences in the impact of ciprofloxacin on microbiota function. In particular, at the whole-community level we detected an increase in starch degradation, glycolysis, and pyruvate fermentation following antibiotic treatment in mice on the Western diet, which we did not observe in mice on the control diet. Similarly, we observed diet-specific changes in the transcriptional activity of two important commensal bacteria, Akkermansia muciniphila and Bacteroides thetaiotaomicron , involving diverse cellular processes such as nutrient acquisition, stress responses, and capsular polysaccharide (CPS) biosynthesis. These findings demonstrate that host diet plays a role in determining the impacts of ciprofloxacin on microbiome composition and microbiome function. IMPORTANCE Due to the growing incidence of disorders related to antibiotic-induced dysbiosis, it is essential to determine how our “Western”-style diet impacts the response of the microbiome to antibiotics. While diet and antibiotics have profound impacts on gut microbiome composition, little work has been done to examine their combined effects. Previous work has shown that nutrient availability, influenced by diet, plays an important role in determining the extent of antibiotic-induced disruption to the gut microbiome. Thus, we hypothesize that the Western diet will shift microbiota metabolism toward simple sugar and mucus degradation and away from polysaccharide utilization. Because of bacterial metabolism’s critical role in antibiotic susceptibility, this change in baseline metabolism will impact how the structure and function of the microbiome are impacted by ciprofloxacin exposure. Understanding how diet modulates antibiotic-induced microbiome disruption will allow for the development of dietary interventions that can alleviate many of the microbiome-dependent complications of antibiotic treatment.
机译:膳食成分和抗生素使用对肠道微生物组的结构和功能产生重大影响,通常导致脱敏。尽管如此,已经完成了很少的研究以探讨宿主饮食作为抗生素诱导的微生物组破坏的决定性的作用。在这里,我们利用了一种多OMIC方法来表征西式饮食消耗对环氧化物诱导的肠道微生物结构和转录活性的变化的影响。我们发现西方饮食消耗大大增加了菌株的大量,并将群体转移到综合糖和粘液糖蛋白的新陈代谢。消耗西兰式饮食的小鼠在环丙沙星治疗后的巨大膨胀,而不是吃对照饮食。经过细胞,我们发现环丙沙星在两种饮食中降低了三羧酸(TCA)循环转录物的丰度,表明碳代谢在肠道微生物组对该抗生素的响应中起关键作用。尽管如此,我们观察到了对CiProfloxacin对微生物群功能的影响广泛的饮食依赖性差异。特别是,在全社区一级,我们检测到淀粉降解,糖酵解和丙酮酸和丙酮酸在西方饮食中的抗生素治疗后的增加,我们在对小鼠上观察到对照饮食中的小鼠。类似地,我们观察到两种重要的共谋细菌,Akkermansia粘蛋白和拟菌甲像中的转录活动的特异性变化,涉及多种细胞过程,例如营养采集,应激反应和囊状多糖(CPS)生物合成。这些研究结果表明,宿主饮食在确定环丙沙星对微生物组成和微生物组函数的影响方面发挥作用。由于患有抗生素诱导的消化不良有关的疾病发病率越来越重要,必须确定我们的“西方” - 饮食如何影响微生物组对抗生素的响应。虽然饮食和抗生素对肠道微生物组成的影响深远,但已经做到了很少的作品来检查它们的组合效果。以前的作品表明,受饮食影响的营养可用性在确定抗生素诱导的肠道微生物组中断的程度上起着重要作用。因此,我们假设西方饮食将微生物脂肪植物代谢移向简单的糖和粘液降解,远离多糖利用。由于细菌代谢在抗生素易感性中的关键作用,基线新陈代谢的这种变化会影响微生物组的结构和功能如何受环丙沙星暴露的影响。了解饮食如何调节抗生素诱导的微生物组中断将允许开发饮食干预,这可以缓解许多抗生素治疗的微生物组依赖性并发症。

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