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Impact of Early Life Antibiotic Exposure and Neonatal Hyperoxia on the Murine Microbiome and Lung Injury

机译:早期抗生素暴露和新生儿高氧血症对小鼠微生物组和肺损伤的影响

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摘要

Cross talk between the intestinal microbiome and the lung and its role in lung health remains unknown. Perinatal exposure to antibiotics disrupts the neonatal microbiome and may have an impact on the preterm lung. We hypothesized that perinatal antibiotic exposure leads to long-term intestinal dysbiosis and increased alveolar simplification in a murine hyperoxia model. Pregnant C57BL/6 wild type dams and neonatal mice were treated with antibiotics before and/or immediately after delivery. Control mice received phosphate-buffered saline (PBS). Neonatal mice were exposed to 95% oxygen for 4 days or room air. Microbiome analysis was performed using 16S rRNA gene sequencing. Pulmonary alveolarization and vascularization were analyzed at postnatal day (PND) 21. Perinatal antibiotic exposure modified intestinal beta diversity but not alpha diversity in neonatal mice. Neonatal hyperoxia exposure altered intestinal beta diversity and relative abundance of commensal bacteria in antibiotic treated mice. Hyperoxia disrupted pulmonary alveolarization and vascularization at PND 21; however, there were no differences in the degree of lung injury in antibiotic treated mice compared to vehicle treated controls. Our study suggests that exposure to both hyperoxia and antibiotics early in life may cause long-term alterations in the intestinal microbiome, but intestinal dysbiosis may not significantly influence neonatal hyperoxic lung injury.
机译:肠道微生物组与肺之间的串扰及其在肺健康中的作用仍然未知。围产期接触抗生素会破坏新生儿微生物组,并可能对早产肺产生影响。我们假设围产期抗生素暴露会导致长期的肠道营养不良,并在鼠高氧血症模型中增加肺泡的简化。在分娩前和/或分娩后立即用抗生素治疗孕妇的C57BL / 6野生型水坝和新生小鼠。对照小鼠接受磷酸盐缓冲盐水(PBS)。新生小鼠暴露于95%的氧气中4天或室内空气。使用16S rRNA基因测序进行微生物组分析。在出生后第21天分析肺泡和血管化。围产期抗生素暴露可改变新生小鼠的肠道β多样性,但不能改变α多样性。新生儿高氧暴露改变了抗生素治疗小鼠的肠道β多样性和共生细菌的相对丰度。高氧血症破坏了PND 21的肺泡和血管形成;然而,与溶媒处理的对照组相比,用抗生素处理的小鼠的肺损伤程度没有差异。我们的研究表明,在生命早期接触高氧和抗生素可能会引起肠道微生物组的长期变化,但肠道营养不良可能不会显着影响新生儿高氧肺损伤。

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