Fecal Mycobiota Combined With Host Immune Factors Distinguish Clostridioides difficile Infection From Asymptomatic Carriage

菌类 UniFrac公司 内转录区 无症状携带者 生物 梭菌纲 微生物学 无症状的 医学 核糖体RNA 内科学 植物 遗传学 细菌 16S核糖体RNA 基因
作者
Yangchun Cao,Yulin Chen,Shanlin Ke,Javier Villafuerte-Gálvez,Nira R. Pollock,Caitlin Barrett,Rebecca Sprague,Kaitlyn Daugherty,Hua Xu,Qianyun Lin,Junhu Yao,Yulin Chen,Ciarán P. Kelly,Yang‐Yu Liu,Xinhua Chen
出处
期刊:Gastroenterology [Elsevier]
卷期号:160 (7): 2328-2339.e6 被引量:25
标识
DOI:10.1053/j.gastro.2021.02.069
摘要

Although the role of gut microbiota in Clostridioides difficile infection (CDI) has been well established, little is known about the role of mycobiota in CDI. Here, we performed mycobiome data analysis in a well-characterized human cohort to evaluate the potential of using gut mycobiota features for CDI diagnosis.Stool samples were collected from 118 hospital patients, divided into 3 groups: CDI (n = 58), asymptomatic carriers (Carrier, n = 28), and Control (n = 32). The nuclear ribosomal DNA internal transcribed spacer 2 was sequenced using the Illumina HiSeq platform to assess the fungal composition. Downstream statistical analyses (including Alpha diversity analysis, ordination analysis, differential abundance analysis, fungal correlation network analysis, and classification analysis) were then performed.Significant differences were observed in alpha and beta diversity between patients with CDI and Carrier (P < .05). Differential abundance analysis identified 2 genera (Cladosporium and Aspergillus) enriched in Carrier. The ratio of Ascomycota to Basidiomycota was dramatically higher in patients with CDI than in Carrier and Control (P < .05). Correlations between host immune factors and mycobiota features were weaker in patients with CDI than in Carrier. Using 4 fungal operational taxonomic units combined with 6 host immune markers in the random forest classifier can achieve very high performance (area under the curve ∼92.38%) in distinguishing patients with CDI from Carrier.Our study provides specific markers of stool fungi combined with host immune factors to distinguish patients with CDI from Carrier. It highlights the importance of gut mycobiome in CDI, which may have been underestimated. Further studies on the diagnostic applications and therapeutic potentials of these findings are warranted.
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