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A seven-gene signature (cirrhosis risk score) predictsliver fibrosis progression in patients with initially mild chronic hepatitis C.

机译:七基因签名(肝硬化风险评分)可预测最初患有轻度慢性丙型肝炎的患者的肝纤维化进展。

摘要

Fibrosis progression is the main determinant of liver disease outcome in chronic hepatitis C, being influenced by environmental and host factors. Recently, a cirrhosis risk score (CRS) based on seven single-nucleotide polymorphisms was proposed as genetic predictor of cirrhosis in hepatitis C. To assess the role of CRS in predicting fibrosis progression in patients with initially no or minimal to moderate fibrosis, we investigated 271 untreated patients with chronic hepatitis C having initial liver biopsy showing METAVIR stage F0 (n = 104), F1 (n = 101), or F2 (n = 59) who had been followed up without antiviral therapies for at least 60 months (mean 108.5 +/- 71.5 months) and had a liver biopsy at the end of this observation period. Of these, 24.4% showed no histologic progression, 75.6% progressed by at least one stage, 45.0% progressed by at least two stages, and 10.3% progressed by more than two stages. The mean CRS was significantly higher (P = 0.005) in patients with fibrosis progression compared with those without progression, and this difference was particularly evident (P = 0.002) with F0 on initial biopsy. Mean CRS scores were not associated with degree of fibrosis progression. The relative risk of fibrosis progression increased with increasing CRS values. This association was significant in males but not in females and was most evident in males with F0 at initial biopsy (odds ratio 16.5, 95% confidence interval 1.6-166; P= 0.02) in the presence of high CRS. Multivariate analysis confirmed the significant association of CRS score with fibrosis progression. The predictive value of CRS was confirmed in hepatitis C virus patients admitting significant alcohol intake. Conclusion: Host genetics defined by CRS predict fibrosis progression in males with initially mild chronic hepatitis C and may become a useful parameter for prognostic evaluation and treatment decision.
机译:纤维化进程是慢性丙型肝炎肝病预后的主要决定因素,受环境和宿主因素的影响。最近,有人提出了基于七种单核苷酸多态性的肝硬化危险性评分(CRS)作为丙型肝炎肝硬化的遗传预测指标。为了评估CRS在预测最初无或轻度至中度纤维化患者的纤维化进展中的作用,我们调查了271例未经治疗的慢性丙型肝炎患者,初次肝活检显示METAVIR分期为F0(n = 104),F1(n = 101)或F2(n = 59),并且接受了至少60个月的无抗病毒治疗的随访(平均) 108.5 +/- 71.5个月),并且在此观察期结束时进行了肝活检。其中,24.4%无组织学进展,至少1个阶段进展75.6%,至少2个阶段进展45.0%,2个以上阶段进展10.3%。有纤维化进展的患者的平均CRS显着高于无纤维化进展的患者(P = 0.005),这种差异在首次活检时为F0尤其明显(P = 0.002)。平均CRS分数与纤维化进展程度无关。纤维化进展的相对风险随着CRS值的增加而增加。这种相关性在男性中是显着的,而在女性中则不显着,并且在存在高CRS的情况下,在初次活检时F0的男性中最明显(比值16.5,95%置信区间1.6-166; P = 0.02)。多变量分析证实了CRS评分与纤维化进展之间存在显着相关性。 CRS的预测值在承认大量饮酒的丙型肝炎病毒患者中得到证实。结论:由CRS定义的宿主遗传学可预测最初患有轻度慢性C型肝炎的男性的纤维化进程,并可能成为评估预后和治疗决策的有用参数。

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