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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >From the Cover: Exposure to Oral Antibiotics Induces Gut Microbiota Dysbiosis Associated with Lipid Metabolism Dysfunction and Low-Grade Inflammation in Mice
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From the Cover: Exposure to Oral Antibiotics Induces Gut Microbiota Dysbiosis Associated with Lipid Metabolism Dysfunction and Low-Grade Inflammation in Mice

机译:从封面开始:口服抗生素引起的肠道菌群代谢异常与脂质代谢功能异常和小鼠低度炎症相关

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摘要

Due to a long history of improper and excessive use, Penicillin G (Pen G) and erythromycin (Ery) are regularly detected in environmental samples and pose a great threat to human health. Here, we set out to investigate effects of Pen G, Ery or their mixture on lipid metabolism and gut microbiota in order to better understand their toxicological mechanisms. Male C57BL/6J mice were exposed either to 60 mu g/ml Pen G, Ery or a half mixture of both for 6 weeks or to 10 mu g/ml Pen G, Ery or a half mixture of both for 14 weeks. In a recovery experiment, male mice were exposed to 60 mu g/ml Pen G or Ery for 2 weeks and then maintained without antibiotics for up to 8 weeks. It was observed that oral exposure to Pen G, Ery or their mixture induced lipid metabolism dysfunction, characterized by significantly increased lipid accumulations, triglycerides (TG) levels and expression of key genes involved in free fatty acid (FFA) synthesis, FFA transport and TG synthesis in the liver. In addition, Pen G and Ery exposure induced an inflammatory response as indicated by the increase of serum lipopolysaccharide levels and the up-regulation of key genes that regulate immune responses in the liver, fat, colon and ileum. Moreover, Pen G and Ery exposure rapidly and dramatically altered the composition of the microbiota in feces and cecum. Furthermore, high throughput sequencing of V3-V4 region of bacterial 16S rRNA gene revealed additional significant changes in the cecal microbiota of antibiotics-treated mice. Importantly, it took a very long time to reconstitute the normal composition of the gut microbiota after it was imbalanced by antibiotics exposure. Orally administered Pen G and Ery (especially to the latter) can induce gut microbiota dysbiosis, which may indirectly link antibiotic exposure to host metabolic disorders and inflammation.
机译:由于长期不当使用和过量使用的历史,经常在环境样品中检测到青霉素G(Pen G)和红霉素(Ery),对人类健康构成极大威胁。在这里,我们着手研究Pen G,Ery或其混合物对脂质代谢和肠道菌群的影响,以便更好地了解它们的毒理学机理。将雄性C57BL / 6J小鼠暴露于60μg / ml的Pen G,Ery或二者的一半混合物中,或暴露于10μg / ml Pen G的Ery或二者的一半混合物中,持续14周。在恢复实验中,将雄性小鼠暴露于60μg / ml的Pen G或Ery中2周,然后不使用抗生素维持长达8周。观察到口服Pen G,Ery或它们的混合物会引起脂质代谢功能障碍,其特征是脂质蓄积,甘油三酸酯(TG)水平和参与游离脂肪酸(FFA)合成,FFA转运和TG的关键基因表达明显增加在肝脏中合成。此外,Pen G和Ery暴露引起炎症反应,血清脂质多糖水平升高以及调节肝脏,脂肪,结肠和回肠中免疫反应的关键基因上调表明了炎症反应。此外,Pen G和Ery的暴露迅速且显着地改变了粪便和盲肠中微生物群的组成。此外,细菌16S rRNA基因的V3-V4区的高通量测序揭示了用抗生素治疗的小鼠的盲肠微生物群中的其他重大变化。重要的是,在肠道微生物群由于抗生素暴露而失衡之后,花费很长时间来重新构建其正常组成。口服Pen G和Ery(尤其是后者)会诱发肠道菌群失调,这可能会将抗生素暴露与宿主代谢紊乱和炎症间接联系起来。

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