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来自马拉维营养不良儿童、可导致饮食依赖性肠病的靶向IgA细菌类群的功能特征。

Functional characterization of IgA-targeted bacterial taxa from undernourished Malawian children that produce diet-dependent enteropathy.

作者信息

Kau Andrew L, Planer Joseph D, Liu Jie, Rao Sindhuja, Yatsunenko Tanya, Trehan Indi, Manary Mark J, Liu Ta-Chiang, Stappenbeck Thaddeus S, Maleta Kenneth M, Ashorn Per, Dewey Kathryn G, Houpt Eric R, Hsieh Chyi-Song, Gordon Jeffrey I

机构信息

Center for Genome Sciences and Systems Biology, Washington University School of Medicine, St. Louis, MO 63108, USA. Department of Medicine, Washington University School of Medicine, St. Louis, MO 63110, USA.

Center for Genome Sciences and Systems Biology, Washington University School of Medicine, St. Louis, MO 63108, USA.

出版信息

Sci Transl Med. 2015 Feb 25;7(276):276ra24. doi: 10.1126/scitranslmed.aaa4877.

Abstract

To gain insights into the interrelationships among childhood undernutrition, the gut microbiota, and gut mucosal immune/barrier function, we purified bacterial strains targeted by immunoglobulin A (IgA) from the fecal microbiota of two cohorts of Malawian infants and children. IgA responses to several bacterial taxa, including Enterobacteriaceae, correlated with anthropometric measurements of nutritional status in longitudinal studies. The relationship between IgA responses and growth was further explained by enteropathogen burden. Gnotobiotic mouse recipients of an IgA(+) bacterial consortium purified from the gut microbiota of undernourished children exhibited a diet-dependent enteropathy characterized by rapid disruption of the small intestinal and colonic epithelial barrier, weight loss, and sepsis that could be prevented by administering two IgA-targeted bacterial species from a healthy microbiota. Dissection of a culture collection of 11 IgA-targeted strains from an undernourished donor, sufficient to transmit these phenotypes, disclosed that Enterobacteriaceae interacted with other consortium members to produce enteropathy. These findings indicate that bacterial targets of IgA responses have etiologic, diagnostic, and therapeutic implications for childhood undernutrition.

摘要

为深入了解儿童期营养不良、肠道微生物群以及肠道黏膜免疫/屏障功能之间的相互关系,我们从两组马拉维婴幼儿的粪便微生物群中纯化了免疫球蛋白A(IgA)靶向的细菌菌株。在纵向研究中,对包括肠杆菌科在内的几种细菌类群的IgA反应与营养状况的人体测量指标相关。肠道病原体负担进一步解释了IgA反应与生长之间的关系。从营养不良儿童的肠道微生物群中纯化出的IgA(+)细菌联合体的无菌小鼠受体表现出一种饮食依赖性肠病,其特征为小肠和结肠上皮屏障迅速破坏、体重减轻和败血症,而给予来自健康微生物群的两种IgA靶向细菌物种可预防这些症状。对来自一名营养不良供体的11种IgA靶向菌株的培养物进行分析,这些菌株足以传递这些表型,结果显示肠杆菌科与其他联合体成员相互作用导致肠病。这些发现表明,IgA反应的细菌靶点对儿童期营养不良具有病因学、诊断和治疗意义。

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