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来自过敏母亲的新生儿的肺部微生物群落失调会使新生儿对次优过敏原产生反应。

Dysbiotic lung microbial communities of neonates from allergic mothers confer neonate responsiveness to suboptimal allergen.

作者信息

Bloodworth Jeffery C, Hoji Aki, Wolff Garen, Mandal Rabindra K, Schmidt Nathan W, Deshane Jessy S, Morrow Casey D, Kloepfer Kirsten M, Cook-Mills Joan M

机构信息

Herman B Wells Center for Pediatric Research, Department of Pediatrics, Indiana University School of Medicine, Indianapolis, IN, United States.

Department of Microbiology and Immunology, Indiana University School of Medicine, Indianapolis, IN, United States.

出版信息

Front Allergy. 2023 Mar 10;4:1135412. doi: 10.3389/falgy.2023.1135412. eCollection 2023.

Abstract

In humans and animals, offspring of allergic mothers have increased responsiveness to allergens. This is blocked in mice by maternal supplementation with α-tocopherol (αT). Also, adults and children with allergic asthma have airway microbiome dysbiosis with increased Proteobacteria and may have decreased Bacteroidota. It is not known whether αT alters neonate development of lung microbiome dysbiosis or whether neonate lung dysbiosis modifies development of allergy. To address this, the bronchoalveolar lavage was analyzed by 16S rRNA gene analysis (bacterial microbiome) from pups of allergic and non-allergic mothers with a basal diet or αT-supplemented diet. Before and after allergen challenge, pups of allergic mothers had dysbiosis in lung microbial composition with increased Proteobacteria and decreased Bacteroidota and this was blocked by αT supplementation. We determined whether intratracheal transfer of pup lung dysbiotic microbial communities modifies the development of allergy in recipient pups early in life. Interestingly, transfer of dysbiotic lung microbial communities from neonates of allergic mothers to neonates of non-allergic mothers was sufficient to confer responsiveness to allergen in the recipient pups. In contrast, neonates of allergic mothers were not protected from development of allergy by transfer of donor lung microbial communities from either neonates of non-allergic mothers or neonates of αT-supplemented allergic mothers. These data suggest that the dysbiotic lung microbiota is dominant and sufficient for enhanced neonate responsiveness to allergen. Importantly, infants within the INHANCE cohort with an anti-inflammatory profile of tocopherol isoforms had an altered microbiome composition compared to infants with a pro-inflammatory profile of tocopherol isoforms. These data may inform design of future studies for approaches in the prevention or intervention in asthma and allergic disease early in life.

摘要

在人类和动物中,过敏母亲的后代对过敏原的反应性增强。在小鼠中,母体补充α-生育酚(αT)可阻断这种情况。此外,患有过敏性哮喘的成人和儿童存在气道微生物群失调,变形菌增加,拟杆菌门可能减少。目前尚不清楚αT是否会改变新生儿肺部微生物群失调的发展,或者新生儿肺部失调是否会改变过敏的发展。为了解决这个问题,通过16S rRNA基因分析(细菌微生物群)对食用基础饮食或补充αT饮食的过敏和非过敏母亲的幼崽进行支气管肺泡灌洗分析。在过敏原激发前后,过敏母亲的幼崽肺部微生物组成失调,变形菌增加,拟杆菌门减少,而补充αT可阻断这种情况。我们确定了幼崽肺部失调的微生物群落经气管内转移是否会改变受体幼崽早期生命中过敏的发展。有趣的是,将过敏母亲新生儿的失调肺部微生物群落转移到非过敏母亲的新生儿中,足以使受体幼崽对过敏原产生反应。相比之下,过敏母亲的新生儿并未因转移来自非过敏母亲新生儿或补充αT的过敏母亲新生儿的供体肺部微生物群落而免受过敏发展的影响。这些数据表明,失调的肺部微生物群占主导地位,足以增强新生儿对过敏原的反应性。重要的是,与具有促炎型生育酚异构体的婴儿相比,INHANCE队列中具有抗炎型生育酚异构体的婴儿的微生物群组成发生了改变。这些数据可能为未来预防或干预生命早期哮喘和过敏性疾病的研究方法设计提供参考。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f411/10036811/e053614d4e28/falgy-04-1135412-g001.jpg

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