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口腔、粪便和炎症性肠病黏膜活检中弯曲菌属菌株的分子流行病学和比较基因组学。

Molecular epidemiology and comparative genomics of Campylobacter concisus strains from saliva, faeces and gut mucosal biopsies in inflammatory bowel disease.

机构信息

Department of Infectious Diseases, Aalborg University Hospital, Aalborg, Denmark.

Department of Clinical Medicine, Aalborg University, Aalborg, Denmark.

出版信息

Sci Rep. 2018 Jan 30;8(1):1902. doi: 10.1038/s41598-018-20135-4.

Abstract

Campylobacter concisus is an emerging pathogen associated with inflammatory bowel disease (IBD), yet little is known about the genetic diversity of C. concisus in relation to host niches and disease. We isolated 104 C. concisus isolates from saliva, mucosal biopsies and faecal samples from 41 individuals (26 IBD, 3 Gastroenteritis (GE), 12 Healthy controls (HC)). Whole genomes were sequenced and the dataset pan-genome examined, and genomic information was used for typing using multi-locus-sequence typing (MLST). C. concisus isolates clustered into two main groups/genomospecies (GS) with 71 distinct sequence types (STs) represented. Sampling site (p < 0.001), rather than disease phenotype (p = 1.00) was associated with particular GS. We identified 97 candidate genes associated with increase or decrease in prevalence during the anatomical descent from the oral cavity to mucosal biopsies to faeces. Genes related to cell wall/membrane biogenesis were more common in oral isolates, whereas genes involved in cell transport, metabolism and secretory pathways were more prevalent in enteric isolates. Furthermore, there was no correlation between individual genetic diversity and clinical phenotype. This study confirms the genetic heterogeneity of C. concisus and provides evidence that genomic variation is related to the source of isolation, but not clinical phenotype.

摘要

短小弯曲杆菌是一种与炎症性肠病(IBD)相关的新兴病原体,但关于宿主小生境和疾病与短小弯曲杆菌遗传多样性的关系知之甚少。我们从 41 名个体(26 名 IBD、3 名肠胃炎(GE)和 12 名健康对照(HC))的唾液、黏膜活检和粪便样本中分离出 104 株短小弯曲杆菌。对全基因组进行测序并对数据集进行泛基因组分析,并利用多位点序列分型(MLST)对基因组信息进行分型。短小弯曲杆菌分离株聚类为两个主要组/基因组种(GS),有 71 个不同的序列型(ST)。采样部位(p<0.001)而不是疾病表型(p=1.00)与特定 GS 相关。我们确定了 97 个与从口腔到黏膜活检再到粪便的解剖学下降过程中患病率增加或减少相关的候选基因。与细胞壁/膜生物发生相关的基因在口腔分离株中更为常见,而与细胞运输、代谢和分泌途径相关的基因在肠道分离株中更为普遍。此外,个体遗传多样性与临床表型之间没有相关性。本研究证实了短小弯曲杆菌的遗传异质性,并提供了证据表明基因组变异与分离源有关,但与临床表型无关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8260/5790007/dfc9943e09a2/41598_2018_20135_Fig1_HTML.jpg

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