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肠道黏膜宏基因组分析揭示了炎症性肠病早期诊断中特定的真核肠道病毒组特征。

Metagenomic analysis of intestinal mucosa revealed a specific eukaryotic gut virome signature in early-diagnosed inflammatory bowel disease.

机构信息

a IBD Center, Laboratory of Gastrointestinal Immunopathology , Humanitas Clinical and Research Center , Milan , Italy.

b Department of Biomedical Sciences , Humanitas University , Milan , Italy.

出版信息

Gut Microbes. 2019;10(2):149-158. doi: 10.1080/19490976.2018.1511664. Epub 2018 Sep 25.

Abstract

Intestinal dysbiosis is one of the causes underlying the pathogenesis of inflammatory bowel disease (IBD), encompassing ulcerative colitis (UC) and Crohn's disease (CD). Besides bacteria, microbiota comprises both prokaryotic and eukaryotic viruses, that together compose the gut virome. Few works have defined the viral composition of stools, while the virome populating intestinal mucosae from early-diagnosed IBD patients has never been studied. Here we show that, by in-depth metagenomic analysis of RNA-Seq data obtained from gut mucosae of young treatment-naïve patients, early-diagnosed for CD and UC, and from healthy subjects (Ctrl), UC patients display significantly higher levels of eukaryotic Hepadnaviridae transcripts by comparison with both Ctrl and CD patients, whereas CD patients show increased abundance of Hepeviridae versus Ctrl. Moreover, we found that UC gut mucosa is characterized by lower levels of Polydnaviridae and Tymoviridae, whereas the mucosa of patients with CD showed a reduced abundance of Virgaviridae. Our findings support the idea that certain eukaryotic viruses might trigger intestinal inflammation and contribute to IBD pathogenesis and pave the way not only for the discovery of novel diagnostic biomarkers but also for the development of anti-viral drugs for the treatment of IBD.

摘要

肠道菌群失调是炎症性肠病(IBD)发病机制的原因之一,包括溃疡性结肠炎(UC)和克罗恩病(CD)。除了细菌,微生物组还包括原核和真核病毒,它们共同构成肠道病毒组。很少有研究定义粪便中的病毒组成,而从早期诊断的 IBD 患者肠道黏膜中获得的病毒组从未被研究过。在这里,我们通过对来自年轻的未经治疗的初诊 CD 和 UC 患者以及健康对照(Ctrl)的肠道黏膜的 RNA-Seq 数据进行深入的宏基因组分析表明,与 Ctrl 和 CD 患者相比,UC 患者的真核 Hepadnaviridae 转录本水平显著升高,而 CD 患者的 Hepeviridae 丰度高于 Ctrl。此外,我们发现 UC 肠道黏膜的多瘤病毒科和 Tymoviridae 水平较低,而 CD 患者的黏膜中 Virgaviridae 的丰度降低。我们的研究结果支持某些真核病毒可能引发肠道炎症并导致 IBD 发病机制的观点,并为发现新的诊断生物标志物以及开发用于治疗 IBD 的抗病毒药物铺平了道路。

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