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首页> 外文期刊>Hepatology: Official Journal of the American Association for the Study of Liver Diseases >Circulating let-7 levels in plasma and extracellular vesicles correlate with hepatic fibrosis progression in chronic hepatitis C
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Circulating let-7 levels in plasma and extracellular vesicles correlate with hepatic fibrosis progression in chronic hepatitis C

机译:血浆和细胞外囊泡中循环let-7水平与慢性丙型肝炎肝纤维化进展相关

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The goal of this study was to determine whether an association exists between circulating microRNA (miRNA) levels and disease progression in chronic hepatitis C (CHC), whether plasma or extracellular vesicles (EVs) were optimal for miRNA measurement and their correlation with hepatic miRNA expression, and the mechanistic plausibility of this association. We studied 130 CHC patients prospectively followed over several decades. A comprehensive miRNA profile in plasma using microarray with 2578 probe sets showed 323 miRNAs differentially expressed between healthy individuals and CHC patients, but only six that distinguished patients with mild versus severe chronic hepatitis. Eventually, let-7a/7c/7d-5p and miR-122-5p were identified as candidate predictors of disease progression. Cross-sectional analyses at the time of initial liver biopsy showed that reduced levels of let-7a/7c/7d-5p (let-7s) in plasma were correlated with advanced histological hepatic fibrosis stage and other fibrotic markers, whereas miR-122-5p levels in plasma were positively correlated with inflammatory activity, but not fibrosis. Measuring let-7s levels in EVs was not superior to intact plasma for discriminating significant hepatic fibrosis. Longitudinal analyses in 60 patients with paired liver biopsies showed that let-7s levels in plasma markedly declined over time in parallel with fibrosis progression. However, circulating let-7s levels did not parallel those in the liver. Conclusion: Of all miRNAs screened, the let-7 family showed the best correlation with hepatic fibrosis in CHC. A single determination of let-7s levels in plasma did not have superior predictive value for significant hepatic fibrosis compared with that of fibrosis-4 index, but the rate of let-7s decline in paired longitudinal samples correlated well with fibrosis progression. Pathway analysis suggested that low levels of let-7 may influence hepatic fibrogenesis through activation of transforming growth factor signaling in hepatic stellate cells. (Hepatology 2016;64:732-745)
机译:这项研究的目的是确定在慢性丙型肝炎(CHC)中循环microRNA(miRNA)水平与疾病进展之间是否存在关联,血浆或细胞外囊泡(EVs)是否最适合miRNA测量及其与肝miRNA表达的相关性,以及该关联的机械合理性。我们对130名CHC患者进行了前瞻性研究,历时数十年。使用带有2578个探针组的微阵列在血浆中的全面miRNA谱图显示,健康个体和CHC患者之间有323个miRNA差异表达,但只有六个能区分轻度和重度慢性肝炎患者。最终,let-7a / 7c / 7d-5p和miR-122-5p被确定为疾病进展的候选预测因子。初次肝活检时的横断面分析显示,血浆中let-7a / 7c / 7d-5p(let-7s)水平的降低与肝组织纤维化进展期及其他纤维化标记物有关,而miR-122-血浆中5p的水平与炎症活动呈正相关,但与纤维化无关。测量电动汽车中let-7s的水平并不能优于完整血浆来区分明显的肝纤维化。对60例肝活检配对患者进行的纵向分析显示,血浆中let-7s的水平随着纤维化的进展而随时间明显下降。但是,循环中let-7s的水平与肝脏中的水平不相称。结论:在所有筛选的miRNA中,let-7家族与CHC肝纤维化的相关性最好。血浆let-7s水平的单一测定与明显的fibrosis-4指数相比,对肝纤维化的预测价值不高,但是成对的纵向样本中let-7s下降的速率与纤维化进展密切相关。通路分析表明,低水平的let-7可能通过激活肝星状细胞中的转化生长因子信号传导来影响肝纤维化。 (肝病2016; 64:732-745)

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