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首页> 外文期刊>The Journal of Clinical Investigation: The Official Journal of the American Society for Clinical Investigation >Metabolomic networks connect host-microbiome processes to human Clostridioides difficile infections
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Metabolomic networks connect host-microbiome processes to human Clostridioides difficile infections

机译:代谢组学网络将宿主微生物组过程与人类艰难梭菌感染联系起来

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摘要

Clostridioides difficile infection (CDI) accounts for a substantial proportion of deaths attributable to antibiotic-resistant bacteria in the United States. Although C. difficile can be an asymptomatic colonizer, its pathogenic potential is most commonly manifested in patients with antibiotic-modified intestinal microbiomes. In a cohort of 186 hospitalized patients, we showed that host and microbe-associated shifts in fecal metabolomes had the potential to distinguish patients with CDI from those with non-C. difficile diarrhea and C. difficile colonization. Patients with CDI exhibited a chemical signature of Stickland amino acid fermentation that was distinct from those of uncolonized controls. This signature suggested that C. difficile preferentially catabolizes branched chain amino acids during CDI. Unexpectedly, we also identified a series of noncanonical, unsaturated bile acids that were depleted in patients with CDI. These bile acids may derive from an extended host-microbiome dehydroxylation network in uninfected patients. Bile acid composition and leucine fermentation defined a prototype metabolomic model with potential to distinguish clinical CDI from asymptomatic C. difficile colonization.
机译:在美国,艰难梭菌感染 (CDI) 占抗生素耐药细菌死亡的很大一部分。尽管艰难梭菌可以是无症状的定植者,但其致病潜力最常见于抗生素修饰的肠道微生物组患者。在 186 名住院患者的队列中,我们发现粪便代谢组的宿主和微生物相关变化有可能区分 CDI 患者和非 C 患者。艰难梭菌腹泻和艰难梭菌定植。CDI 患者表现出 Stickland 氨基酸发酵的化学特征,与未定植对照组不同。该特征表明艰难梭菌在 CDI 期间优先分解代谢支链氨基酸。出乎意料的是,我们还发现了一系列非经典的不饱和胆汁酸,这些胆汁酸在CDI患者中被耗尽。这些胆汁酸可能来自未感染患者中扩展的宿主-微生物组脱羟基化网络。胆汁酸组成和亮氨酸发酵定义了一个原型代谢组学模型,该模型有可能区分临床 CDI 和无症状艰难梭菌定植。

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