Evaluation of predictors of liver fibrosis progression in patients with hepatitis C after successful virus elimination

S. Malov, L. Orlova, L. A. Stepanenko, O. Ogarkov, I. Malov, N. D. Yushchuk
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Abstract

Objective. To determine environmental and genetic factors associated with fibrosis progression after virus elimination as a result of direct-acting antiviral therapy by follow-up dispensary observation of patients with chronic hepatitis C with moderate and severe liver fibrosis (F2–F3 according to the METAVIR scoring system). Patients and methods. This study included 301 patients (166 men and 135 women) aged 20-64 years with chronic hepatitis C virus (HCV). A sustained virologic response was achieved in all patients after therapy with direct-acting antiviral agents. Patients were followed up for an average of 38 weeks (16–64). Patients were divided into two groups in order to perform comparative evaluation: group I included 257 patients with regression of liver fibrosis and group II – 44 patients with progression of liver fibrosis. Questionnaire and clinical and laboratory data were assessed. In addition, genetic studies of 24 singlenucleotide polymorphisms of genes involved in intracellular immune signaling pathway activation, interferon synthesis, metabolic regulation and cell proliferation were performed in both groups. Results. It was revealed that validated predictors of liver fibrosis progression in patients with chronic HCV after successful virus elimination as a result of therapy with direct-acting antiviral agents are the presence of concomitant type 2 diabetes mellitus, low ALT activity and serum osteopontin levels over 80 ng/mL at the beginning of therapy. Genetic predisposition to liver fibrosis progression is mediated by carriage of the AA genotype of HNF4α rs4812829 (OR = 3.55; 95% CI 1.21–10.41; p = 0.015). Additionally, the G-allele of NAT2 rs1495741, which marks fast xenobiotic acetylation, was found to have protective properties in the dominant genetic model. Carriers of GG- and GA-genotypes had an almost 2-fold lower risk of liver fibrosis progression after antiviral therapy than AA-genotype carriers (OR = 0.49; 95% CI 0.25–0.94; p = 0.029). Conclusion. The risk after successful hepatitis C virus elimination is significantly higher in patients with concomitant type 2 diabetes mellitus. ALT activity and serum osteopontin levels at the beginning of therapy can be estimated as predictors of liver fibrosis progression among laboratory parameters. Moreover, some genetic markers in the form of single-nucleotide polymorphisms of the HNF4α and NAT2 genes were established, which can be used to predict the development of liver fibrosis in patients with hepatitis C after therapy with direct-acting antiviral agents. Key words: hepatitis C, liver fibrosis, predictors, risk factors, diabetes mellitus, osteopontin, single-nucleotide polymorphisms, HNF4α gene, NAT2 gene
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成功消除病毒后丙型肝炎患者肝纤维化进展预测因素的评估
目标。通过对慢性丙型肝炎合并中重度肝纤维化(METAVIR评分系统F2-F3)患者的随访药房观察,确定直接作用抗病毒治疗消除病毒后纤维化进展的环境和遗传因素。患者和方法。本研究纳入了301例年龄在20-64岁的慢性丙型肝炎病毒(HCV)患者(166名男性和135名女性)。所有患者在接受直接抗病毒药物治疗后均取得了持续的病毒学应答。患者平均随访38周(16 ~ 64周)。将患者分为两组进行比较评价:I组257例肝纤维化消退患者,II组44例肝纤维化进展患者。对问卷调查、临床和实验室数据进行评估。此外,对两组小鼠细胞内免疫信号通路激活、干扰素合成、代谢调节和细胞增殖相关基因的24个单核苷酸多态性进行遗传研究。结果。结果显示,在直接抗病毒药物治疗成功消除病毒后,慢性HCV患者肝纤维化进展的有效预测因素是伴有2型糖尿病、低ALT活性和治疗开始时血清骨桥蛋白水平超过80 ng/mL。携带HNF4α rs4812829 AA基因型介导肝纤维化进展的遗传易感性(OR = 3.55;95% ci 1.21-10.41;P = 0.015)。此外,在显性遗传模型中,发现NAT2 rs1495741的g等位基因具有快速外源乙酰化的保护特性。GG-和ga基因型携带者在抗病毒治疗后肝纤维化进展的风险比aa基因型携带者低近2倍(OR = 0.49;95% ci 0.25-0.94;P = 0.029)。结论。伴有2型糖尿病的丙型肝炎病毒清除成功后的风险明显更高。治疗开始时ALT活性和血清骨桥蛋白水平可作为肝纤维化进展的预测指标。此外,还建立了HNF4α和NAT2基因单核苷酸多态性的遗传标记,可用于预测直接作用抗病毒药物治疗后丙型肝炎患者肝纤维化的发展。关键词:丙型肝炎,肝纤维化,预测因素,危险因素,糖尿病,骨桥蛋白,单核苷酸多态性,HNF4α基因,NAT2基因
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来源期刊
Infektsionnye Bolezni
Infektsionnye Bolezni Medicine-Infectious Diseases
CiteScore
1.30
自引率
0.00%
发文量
15
期刊介绍: The journal publishes original research works, reviews of literature, lectures, methodological recommendations, clinical observations. Main topics: problems of etiology, pathogenesis, clinical manifestations of infectious diseases, new techniques and methods of their diagnosis, prevention and treatment; special attention is paid to the problems of antibacterial and antiviral therapy, the use of immunoglobulins and interferons, and also to intensive therapy of critical states. The journal is in the List of leading scientific journals and periodicals of the Supreme Attestation Committee, where the principal results of doctoral dissertations should be published.
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