Prolonged release pirfenidone restores miRNA expression and CpG island methylation in patients with HCV sustained virological response and residual liver fibrosis

IF 3.7 3区医学 Q2 GASTROENTEROLOGY & HEPATOLOGY

Annals of hepatology Pub Date : 2025-04-01 DOI:10.1016/j.aohep.2025.101889

Eira Cerda-Reyes , Ricardo de la Rosa-Bibiano , Ana Sandoval-Rodriguez , Rebeca Rosas-Campos , Rebeca Escutia-Gutiérrez , Ángel Vázquez-Esqueda , Stefanny Cornejo-Hernández , Alejandro Gutiérrez-Átemis , Salvador Amezquita-Pérez , Jorge Luis Poo , Gildardo Agustin Garrido-Sanchez , Juan Ramón-Aguilar , Juan Armendáriz-Borunda

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引用次数: 0

Abstract

Introduction and Objectives

Patients with residual liver fibrosis after hepatitis C virus-infection clearance represent an important challenge due to the risk of progression and hepatocarcinoma development. The primary end of this study was to evaluate epigenetic marks in DAA-responders HCV non-European patients presenting remaining fibrosis. The secondary aim was to assess the efficacy of 12 months of treatment with prolonged-release pirfenidone (PR-PFD) in liver fibrosis regression.

Materials and Patients

Forty-four DAA-responders HCV patients presenting remaining fibrosis (73% women) were enrolled in the study and received PR-PFD (1200 mg/day) for 12 months. Six patients dropped out. Liver biopsies and serum samples were analyzed at the beginning and end of treatment. Besides, six non-fibrotic controls were included to compare epigenetics marks.

Results

After 12 months of treatment, 28.94% of patients showed a reduction in at least 1 fibrosis stage based on liver biopsies, while 57.57% experienced fibrosis reversion according to transient elastography. Bilirubin, alkaline phosphatase, AST, INR, and APRI values significantly decreased, and only minor adverse events were reported. Profibrogenic miRNAs displayed a significant increase in expression in advanced fibrosis versus controls without fibrosis. Noteworthy, PR-PFD treatment induced their decrease and restored the expression of miR-34a, miR-16, miR-192, miR-200a and miR-122 correlating with the downgrade of fibrosis stage. Specific PDGFa CpGs exhibited hypermethylation in both cell-free-DNA and liver biopsies in both mild and advanced fibrosis. Interestingly, four CpGs in PPARd promoter were hypomethylated versus controls. PR-PFD treatment resulted in hypermethylation in three TGFb1-CpGs after 12 months, suggesting down-regulation of this profibrogenic cytokine.

Conclusions

These findings suggest, for the first time, that PR-PFD might exert its therapeutic effects in Hispanic patients with residual fibrosis by modulating the expression of miRNAs and methylation of specific CpG sites.

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缓释吡非尼酮可恢复HCV持续病毒学反应和残余肝纤维化患者的miRNA表达和CpG岛甲基化

丙型肝炎病毒感染清除后残留肝纤维化患者由于进展和肝癌发展的风险，是一个重要的挑战。本研究的主要目的是评估daa应答的HCV非欧洲患者存在剩余纤维化的表观遗传标记。次要目的是评估12个月缓释吡非尼酮（PR-PFD）治疗对肝纤维化消退的疗效。材料和患者44名daa应答的HCV患者（73%为女性）被纳入研究，并接受PR-PFD （1200mg /天）治疗12个月。6名患者退出了研究。在治疗开始和结束时进行肝活检和血清样本分析。此外，还包括6个非纤维化对照，以比较表观遗传标记。结果治疗12个月后，28.94%的患者肝活检显示至少1个纤维化阶段减少，而根据瞬时弹性成像，57.57%的患者出现纤维化逆转。胆红素、碱性磷酸酶、AST、INR和APRI值显著降低，仅报告轻微不良事件。与无纤维化的对照组相比，促纤维化mirna在晚期纤维化中的表达显著增加。值得注意的是，PR-PFD治疗诱导了它们的降低，并恢复了与纤维化分期降低相关的miR-34a、miR-16、miR-192、miR-200a和miR-122的表达。特异性PDGFa CpGs在轻度和晚期纤维化的无细胞dna和肝脏活检中均表现出高甲基化。有趣的是，与对照组相比，PPARd启动子中的4个CpGs低甲基化。PR-PFD治疗12个月后导致3个TGFb1-CpGs高甲基化，表明该促纤维化细胞因子下调。结论这些发现首次表明PR-PFD可能通过调节mirna的表达和特定CpG位点的甲基化来发挥其对西班牙裔残余纤维化患者的治疗作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Annals of hepatology 医学-胃肠肝病学

CiteScore

7.90

自引率

2.60%

发文量

183

审稿时长

4-8 weeks

期刊介绍： Annals of Hepatology publishes original research on the biology and diseases of the liver in both humans and experimental models. Contributions may be submitted as regular articles. The journal also publishes concise reviews of both basic and clinical topics.