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肠道真菌菌群的一个成员可调节宿主嘌呤代谢,加剧小鼠的结肠炎。

A member of the gut mycobiota modulates host purine metabolism exacerbating colitis in mice.

作者信息

Chiaro Tyson R, Soto Ray, Zac Stephens W, Kubinak Jason L, Petersen Charisse, Gogokhia Lasha, Bell Rickesha, Delgado Julio C, Cox James, Voth Warren, Brown Jessica, Stillman David J, O'Connell Ryan M, Tebo Anne E, Round June L

机构信息

Division of Microbiology and Immunology, Department of Pathology, University of Utah School of Medicine, Salt Lake City, UT 84112, USA.

ARUP Laboratories, 500 Chipeta Way, Salt Lake City, UT 84108, USA.

出版信息

Sci Transl Med. 2017 Mar 8;9(380). doi: 10.1126/scitranslmed.aaf9044.

Abstract

The commensal microbiota has an important impact on host health, which is only beginning to be elucidated. Despite the presence of fungal, archaeal, and viral members, most studies have focused solely on the bacterial microbiota. Antibodies against the yeast are found in some patients with Crohn's disease (CD), suggesting that the mycobiota may contribute to disease severity. We report that exacerbated intestinal disease in a mouse model of colitis and increased gut barrier permeability. Transcriptome analysis of colon tissue from germ-free mice inoculated with or another fungus, , revealed that colonization affected the intestinal barrier and host metabolism. A fecal metabolomics screen of germ-free animals demonstrated that colonization enhanced host purine metabolism, leading to an increase in uric acid production. Treatment with uric acid alone worsened disease and increased gut permeability. Allopurinol, a clinical drug used to reduce uric acid, ameliorated colitis induced by in mice. In addition, we found a positive correlation between elevated uric acid and anti-yeast antibodies in human sera. Thus, yeast in the gut may be able to potentiate metabolite production that negatively affects the course of inflammatory bowel disease.

摘要

共生微生物群对宿主健康具有重要影响,而这一影响才刚刚开始被阐明。尽管存在真菌、古菌和病毒成员,但大多数研究仅聚焦于细菌微生物群。在一些克罗恩病(CD)患者体内发现了抗酵母菌的抗体,这表明真菌微生物群可能会加重疾病的严重程度。我们报告称,在结肠炎小鼠模型中,[具体真菌名称未给出]会加剧肠道疾病并增加肠道屏障通透性。对接种了[具体真菌名称未给出]或另一种真菌[具体真菌名称未给出]的无菌小鼠的结肠组织进行转录组分析,结果显示[具体真菌名称未给出]的定殖会影响肠道屏障和宿主代谢。对无菌动物进行的粪便代谢组学筛查表明,[具体真菌名称未给出]的定殖会增强宿主嘌呤代谢,导致尿酸生成增加。单独使用尿酸进行治疗会使疾病恶化并增加肠道通透性。别嘌醇是一种用于降低尿酸的临床药物,它能改善小鼠因[具体真菌名称未给出]诱发的结肠炎。此外,我们发现人体血清中尿酸升高与抗酵母菌抗体之间存在正相关。因此,肠道中的酵母菌可能会增强代谢产物的生成,从而对炎症性肠病的病程产生负面影响。

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