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早期亚治疗剂量抗生素处理(STAT)对超重的影响是显著的,尽管肠道微生物发生了转移。

The impact of early-life sub-therapeutic antibiotic treatment (STAT) on excessive weight is robust despite transfer of intestinal microbes.

机构信息

Department of Medicine, New York University Langone Medical Center, New York, NY, 10016, USA.

Computational Biology Program, Memorial Sloan-Kettering Cancer Center, New York, NY, 10065, USA.

出版信息

ISME J. 2019 May;13(5):1280-1292. doi: 10.1038/s41396-019-0349-4. Epub 2019 Jan 16.

Abstract

The high-fat, high-calorie diets of westernized cultures contribute to the global obesity epidemic, and early life exposure to antibiotics may potentiate those dietary effects. Previous experiments with mice had shown that sub-therapeutic antibiotic treatment (STAT)-even restricted to early life-affected the gut microbiota, altered host metabolism, and increased adiposity throughout the lifetime of the animals. Here we carried out a large-scale cohousing experiment to investigate whether cohousing STAT and untreated (Control) mice would transfer the STAT-perturbed microbiota and transmit its impact on weight. We exposed pregnant dams and their young offspring to either low-dose penicillin (STAT) or water (Control) until weaning, and then followed the offspring as they grew and endured a switch from normal to high-fat diet at week 17 of life. Cohousing, which started at week 4, rapidly approximated the microbiota within cages, lowering the weight of STAT mice relative to non-cohoused mice. The effect, however, varied between cages, and was restricted to the first 16 weeks when diet consisted of normal chow. Once mice switched to high-fat diet, the microbiota α- and β-diversity expanded and the effect of cohousing faded: STAT mice, again, were heavier than control mice independently of cohousing. Metabolomics revealed serum metabolites associated with STAT exposure, but no significant differences were detected in glucose or insulin tolerance. Our results show that cohousing can partly ameliorate the impact of STAT on the gut microbiota but not prevent increased weight with high-fat diet. These observations have implications for microbiota therapies aimed to resolve the collateral damage of antibiotics and their load on human obesity.

摘要

西方化文化中的高脂肪、高热量饮食导致了全球肥胖流行,而早期生活中接触抗生素可能会增强这些饮食的影响。以前的小鼠实验表明,亚治疗剂量的抗生素治疗(STAT)——即使仅限于早期生活——会影响肠道微生物群,改变宿主代谢,并在动物的整个生命周期内增加肥胖。在这里,我们进行了一项大规模的共同饲养实验,以研究共同饲养 STAT 和未处理(对照)的小鼠是否会转移 STAT 扰乱的微生物群,并传递其对体重的影响。我们让怀孕的母鼠和它们的幼崽在断奶前接受低剂量青霉素(STAT)或水(对照)处理,然后在它们生长并在生命的第 17 周从正常饮食切换到高脂肪饮食时对它们进行跟踪。从第 4 周开始的共同饲养迅速接近笼子内的微生物群,使 STAT 小鼠的体重相对于非共同饲养的小鼠减轻。然而,这种影响在笼子之间有所不同,并且仅在饮食由正常饲料组成的前 16 周内受到限制。一旦小鼠切换到高脂肪饮食,微生物群的 α-和 β-多样性就会扩大,共同饲养的影响就会消失:STAT 小鼠的体重再次比对照小鼠重,而不管是否共同饲养。代谢组学揭示了与 STAT 暴露相关的血清代谢物,但在葡萄糖或胰岛素耐量方面没有检测到显著差异。我们的结果表明,共同饲养可以部分改善 STAT 对肠道微生物群的影响,但不能防止高脂肪饮食引起的体重增加。这些观察结果对旨在解决抗生素的附带损害及其对人类肥胖影响的微生物组疗法具有重要意义。

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