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An initial assessment of correlations between host- and virus-related factors affecting analogues antiviral therapy in HBV chronically infected patients

机译:HBV慢性感染患者宿主和病毒相关因素影响类似物抗病毒治疗的相关性的初步评估

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Background Success in treating hepatitis B virus (HBV) infection with nucleoside analogues drugs is limited by the emergence of drug-resistant viral strains upon prolonged therapy. In addition to mutation patterns in the viral polymerase gene, host factors are assumed to contribute to failure of treatment in chronic HBV infections. The aim of this study was to analyze the correlation between efficacy of antiviral therapy and the prevalence of HBV pretreatment drug-resistant variants. We also analyzed the role of heterogeneity in the promoter region of the IL-10 on the HBV [i]pol/s[/i] gene polymorphisms and efficacy of analogues-driven therapy. Material and Methods HBV DNA was extracted from 54 serum samples from chronic hepatitis B (CHB) patients. Drug-resistance mutations were analyzed using MALDI-TOF mass spectrometry technology (MALDI-TOF MS) and Multi-temperature single-strand conformation polymorphism (MSSCP). IL-10 gene promoter region polymorphisms at positions -1082, -819, and -592 were determined in allele-specific PCR reactions (AS-PCR). Results Drug-resistance mutations were detected in 74% of na?ve and 93% of experienced patients, but the effect of pre-existence of drug-resistant HBV variants on antiviral therapy was not statistically significant (p=0.86). The role of polymorphisms at positions –1082 (p=0.88), –819 (p=0.26), and –592 (p=0.26) of IL-10 promoter region polymorphisms was excluded from the response-predicting factors. The main host factors predicting successful response to antiviral therapy were female sex (p=0.007) and young age (p=0.013). Conclusions The presence of drug-resistant HBV variants in baseline is not a viral predictor of good response to nucleosideucleotide analogues therapy. Only low HBV viral load predicted positive response to antiviral therapy. The ideal candidate for antiviral therapy is an immunocompetent, young female with low HBV viral load and elevated ALT activity.
机译:背景技术通过长期治疗出现耐药病毒株,限制了用核苷类似物药物治疗乙型肝炎病毒(HBV)感染的成功。除了病毒聚合酶基因中的突变模式外,还假定宿主因素会导致慢性HBV感染治疗失败。这项研究的目的是分析抗病毒治疗的疗效与HBV预处理耐药变异的发生率之间的相关性。我们还分析了HBV [i] pol / s [/ i]基因多态性在IL-10启动子区域中异质性的作用以及类似物驱动疗法的功效。材料和方法从慢性乙型肝炎(CHB)患者的54个血清样本中提取HBV DNA。使用MALDI-TOF质谱技术(MALDI-TOF MS)和多温度单链构象多态性(MSSCP)分析了耐药性突变。在等位基因特异性PCR反应(AS-PCR)中确定了IL-10基因启动子区域-1082,-819和-592的多态性。结果在74%的初次接受治疗的患者和93%的经验丰富的患者中均检测到耐药性突变,但耐药性HBV变异体的存在对抗病毒治疗的影响无统计学意义(p = 0.86)。 IL-10启动子区域多态性在位置–1082(p = 0.88),– 819(p = 0.26)和–592(p = 0.26)的多态性的作用已从响应预测因素中排除。预测抗病毒治疗成功反应的主要宿主因素是女性(p = 0.007)和年轻(p = 0.013)。结论基线中存在耐药性HBV变异体并不是病毒对核苷/核苷酸类似物疗法产生良好反应的预测指标。只有低HBV病毒载量可预测抗病毒治疗的阳性反应。抗病毒治疗的理想人选是具有免疫能力的年轻女性,HBV病毒载量低,ALT活性高。

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