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肺动脉高压患者肠道微生物组谱的改变。

Altered Gut Microbiome Profile in Patients With Pulmonary Arterial Hypertension.

机构信息

From the Department of Physiology and Functional Genomics (S.K., E.M.R., M.K.R.), College of Medicine, University of Florida, Gainesville.

Gilead Sciences, Foster City, California (S.K.).

出版信息

Hypertension. 2020 Apr;75(4):1063-1071. doi: 10.1161/HYPERTENSIONAHA.119.14294. Epub 2020 Feb 24.

Abstract

Pulmonary arterial hypertension (PAH) is considered a disease of the pulmonary vasculature. Limited progress has been made in preventing or arresting progression of PAH despite extensive efforts. Our previous studies indicated that PAH could be considered a systemic disease since its pathology involves interplay of multiple organs. This, coupled with increasing implication of the gut and its microbiome in chronic diseases, led us to hypothesize that patients with PAH exhibit a distinct gut microbiome that contributes to, and predicts, the disease. Fecal microbiome of 18 type 1 PAH patients (mean pulmonary arterial pressure, 57.4, SD 16.7 mm Hg) and 13 reference subjects were compared by shotgun metagenomics to evaluate this hypothesis. Significant taxonomic and functional changes in microbial communities in the PAH cohort were observed. Pathways for the synthesis of arginine, proline, and ornithine were increased in PAH cohort compared with reference cohort. Additionally, groups of bacterial communities associated with trimethylamine/ trimethylamine N-oxide and purine metabolism were increased in PAH cohort. In contrast, butyrate-and propionate-producing bacteria such as Coprococcus, Butyrivibrio, Lachnospiraceae, Eubacterium, Akkermansia, and Bacteroides were increased in reference cohort. A random forest model predicted PAH from the composition of the gut microbiome with 83% accuracy. Finally, virome analysis showed enrichment of Enterococcal and relative depletion of Lactococcal phages in the PAH cohort. In conclusion, patients with PAH exhibit a unique microbiome profile that has the high predictive potential for PAH. This highlights previously unknown roles of gut bacteria in this disease and could lead to new therapeutic, diagnostic, or management paradigms for PAH.

摘要

肺动脉高压(PAH)被认为是肺血管系统的一种疾病。尽管付出了广泛的努力,但在预防或阻止 PAH 进展方面进展有限。我们之前的研究表明,PAH 可以被认为是一种全身性疾病,因为其病理学涉及多个器官的相互作用。再加上肠道及其微生物群在慢性疾病中的作用越来越大,这促使我们假设 PAH 患者表现出独特的肠道微生物群,该微生物群有助于并预测疾病。通过 shotgun 宏基因组学比较了 18 名 1 型 PAH 患者(平均肺动脉压 57.4,SD 16.7mmHg)和 13 名参考对象的粪便微生物组,以验证该假说。在 PAH 队列中观察到微生物群落的分类和功能发生了显著变化。与参考队列相比,PAH 队列中精氨酸、脯氨酸和鸟氨酸合成途径增加。此外,与三甲胺/氧化三甲胺和嘌呤代谢相关的细菌群落也在 PAH 队列中增加。相反,在参考队列中,丁酸和丙酸产生菌如 Coprococcus、Butyrivibrio、Lachnospiraceae、Eubacterium、Akkermansia 和 Bacteroides 增加。随机森林模型根据肠道微生物组的组成预测 PAH 的准确率为 83%。最后,病毒组分析显示 PAH 队列中肠球菌富集,乳球菌噬菌体相对减少。总之,PAH 患者表现出独特的微生物组谱,对 PAH 具有高预测潜力。这突显了肠道细菌在这种疾病中的未知作用,并可能为 PAH 带来新的治疗、诊断或管理模式。

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