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首页> 外文期刊>Gastroenterology >Intestinal Dysbiosis Featuring Abundance of Ruminococcus gnavus Associates With Allergic Diseases in Infants
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Intestinal Dysbiosis Featuring Abundance of Ruminococcus gnavus Associates With Allergic Diseases in Infants

机译:具有丰富的肠道脱泻,具有丰富的婴儿床婴儿过敏性疾病

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Background & Aims Dysbiosis of the intestinal microbiota has been associated with development of allergies in infants. However, it is not clear what microbes might contribute to this process. We investigated what microbe(s) might be involved in analyses of infant twins and mice. Methods We studied fecal specimens prospectively in a twin cohort (n? 30) and age-matched singletons (n? 14) born at National Taiwan University Childrens Hospital, Taipei, Taiwan, from April 2011 to March 2013. Clinical parameters (gestational age, birth body weight, mode of delivery and feeding, immunizations, and medical events) were recorded. Fecal samples were collected beginning immediately after birth and for 1 year; the children were followed until 3 years of age and allergic symptoms (repetitive and continuous for at least 6 months) were noted. A skin prick test was used to ascertain atopy. Bacterial communities in fecal samples were profiled by 16S ribosomal RNA-based polymerase chain reactiontemporal temperature gradient gel electrophoresis and next-generation sequencing. BALB/c mice without and with ovalbumin sensitization/challenge were infected with candidate bacteria by oral gauge intragastric intubation. Fecal, serum, lung, and colon tissue samples were collected from mice and analyzed for mechanisms of allergy development. Results During the investigation period, 20 children (45.5%) developed allergic diseases, including respiratory (allergic rhinitis and asthma) and skin (atopic dermatitis and eczema) allergies. Lachnospiraceae were detected at significantly higher frequency in allergic infants than nonallergic infants ( P Ruminococcus gnavus , which爐ended to have a low frequency in nonallergic subjects ( P ? .0004). Increased R gnavus was observed before the onset of allergic manifestations, and was associated with respiratory allergies ( P P ?R gnavus grew rapidly after sensitization and challenge with ovalbumin. Mice gavaged with purified R gnavus developed airway hyper-responsiveness and had histologic evidence of airway inflammation (asthma). Expansion of R gnavus in mice stimulated secretion of cytokines (interleukin [IL] 25, IL33, and thymic stromal lymphopoietin) by colon tissues, which activated type 2 innate lymphoid cells and dendritic cells to promote differentiation of T-helper 2 cells and production of their cytokines (IL4, IL5, and IL13). This led to infiltration of the colon and lung parenchyma by eosinophils and mast cells. Conclusions In a study of a twin cohort (some infants with,爏ome without allergies), we associated development of allergies, particularly respiratory allergies, with increased fecal abundance of R gnavus . Mice fed R gnavus developed airway inflammation, characterized by expansion of T-helper 2 cells in the colon and lung, and infiltration of colon and lung parenchyma by eosinophils and mast cells. Graphical abstract Display Omitted
机译:背景和AIMS肠道微生物群的消化不良与婴儿过敏的发展有关。但是,目前尚不清楚微生物可能对此过程有所贡献。我们调查了婴幼儿双胞胎和小鼠的分析中可能参与的微生物。方法我们在双胞胎群组(N'30)和年龄匹配的单身(N-34)中前瞻性地研究了粪便标本(N-34),从2011年4月到2013年4月到2013年3月到3月。临床参数(胎龄,记录出生体重,交付方式和喂养,免疫和医疗事件)。在出生后立即收集粪便样本,并在出生后立即收集;注意到儿童直至3岁,过敏症状(重复和连续至少6个月)。皮肤刺试验用于确定特性。通过16S核糖体RNA的聚合酶链反应血温梯度凝胶电泳和下一代测序,通过16S核糖体RNA的聚合酶链的细菌群体进行分析。通过口服仪表肠道插管,患有蛋白化细菌的Balb / c小鼠没有卵泡致敏/挑战。从小鼠收集粪便,血清,肺和结肠组织样品,并分析过敏发育机制。结果在调查期间,20名儿童(45.5%)发育过敏性疾病,包括呼吸道(过敏性鼻炎和哮喘)和皮肤(特应性皮炎和湿疹)过敏。在过敏性婴儿的频率明显较高的频率下检测到Lachnospiraceae(p喇叭仪,其中炉结束在非过敏性受试者中具有低频率(p≤0004)。在过敏表现前观察到r Gnavus增加,并且是与呼吸过敏有关(PP?r Gnavus在致敏和癌症后迅速增长。用纯化的R Gnavus致致挑战,发育了Airway超响应性,并且具有气道炎症(哮喘)的组织学证据。在小鼠中扩张刺激细胞因子的分泌刺激细胞因子的分泌刺激分泌细胞因子(白细胞介素[IL] 25,IL33和胸腺基质淋巴泛肝异蛋白)通过结肠组织,其活化2型先天淋巴细胞和树突细胞,以促进T-Helper 2细胞的分化和它们的细胞因子(IL4,IL5和IL13)的产生。这导致嗜酸性粒细胞和肥大细胞渗透结肠和肺实质。在一对双胞胎队队的研究中结论(一些婴儿在没有过敏的情况下,我们关联过敏,特别是呼吸过敏的开发,随着R GNavus的粪便丰富增加。喂养R吉乌斯的小鼠开发了气道炎症,其特征在于结肠和肺中的T-辅助2细胞,并通过嗜酸性粒细胞和肥大细胞浸润结肠癌和肺部薄膜。省略了图形抽象显示

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