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Early life microbiome perturbation alters pulmonary responses to ozone in male mice

机译:生命早期的微生物组扰动改变了雄性小鼠的肺对臭氧的反应

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摘要

Early life changes in the microbiome contribute to the development of allergic asthma, but little is known about the importance of the microbiome for other forms of asthma. Ozone is a nonatopic asthma trigger that causes airway hyperresponsiveness and neutrophil recruitment to the lungs. The purpose of this study was to test the hypothesis that early life perturbations in the gut microbiome influence subsequent responses to ozone. To that end, we placed weanling mouse pups from The Jackson Laboratories or from Taconic Farms in sex‐specific cages either with other mice from the same vendor (same‐housed) or with mice from the opposite vendor (cohoused). Mice were maintained with these cagemates until use. The gut microbial community differs in mice from Jackson Labs and Taconic Farms, and cohousing mice transfers fecal microbiota from one mouse to another. Indeed, 16S rRNA sequencing of fecal DNA indicated that differences in the gut microbiomes of Jackson and Taconic same‐housed mice were largely abolished when the mice were cohoused. At 10–12 weeks of age, mice were exposed to room air or ozone (2 ppm for 3 hr). Compared to same‐housed mice, cohoused male but not female mice had reduced ozone‐induced airway hyperresponsiveness and reduced ozone‐induced increases in bronchoalveolar lavage neutrophils. Ozone‐induced airway hyperresponsiveness was greater in male than in female mice and the sex difference was largely abolished in cohoused mice. The data indicate a role for early life microbial perturbations in pulmonary responses to a nonallergic asthma trigger.
机译:微生物组的早期生命变化会导致过敏性哮喘的发展,但是对于微生物组对其他形式的哮喘的重要性知之甚少。臭氧是非特应性哮喘的诱因,可引起气道高反应性和嗜中性白细胞募集至肺部。本研究的目的是检验以下假设:肠道微生物组的早期生命扰动会影响随后对臭氧的反应。为此,我们将来自杰克逊实验室(Jackson Laboratories)或塔科尼奇农场(Taconic Farms)的断奶小鼠幼崽与同一个供应商(同窝)的其他小鼠或同一个供应商(同窝)的其他小鼠放在性别特定的笼子里。将小鼠与这些笼伴侣保持在一起直到使用。肠道微生物群落在杰克逊实验室和塔科尼奇农场的小鼠中有所不同,并且鸡群将粪便微生物群从一只小鼠转移到另一只小鼠。的确,粪便DNA的16S rRNA测序表明,当共同饲养小鼠时,杰克逊和塔科尼克同巢小鼠的肠道微生物区系的差异已基本​​消除。在10-12周龄时,小鼠暴露于室内空气或臭氧中(2 ppm持续3小时)。与同居小鼠相比,同居雄性小鼠而非雌性小鼠降低了臭氧诱导的气道高反应性,并降低了臭氧诱导的支气管肺泡灌洗中性粒细胞增加。雄性小鼠的臭氧诱导的气道高反应性要强于雌性小鼠,而在共同饲养的小鼠中,性别差异已基本​​消除。数据表明,早期生活中的微生物摄动在非过敏性哮喘触发因素的肺反应中具有作用。

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