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Genetic Heterogeneity of Hypervariable Region 1 of the Hepatitis C Virus (HCV) Genome and Sensitivity of HCV to Alpha Interferon Therapy

机译:丙型肝炎病毒(HCV)基因组高变区1的遗传异质性和HCV对α干扰素治疗的敏感性

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摘要

Hepatitis C virus (HCV) populations persist in vivo as a mixture of heterogeneous viruses called quasispecies. The relationship between the genetic heterogeneity of these variants and their responses to antiviral treatment remains to be elucidated. We have studied 26 virus strains to determine the influence of hypervariable region 1 (HVR-1) of the HCV genome on the effectiveness of alpha interferon (IFN-α) therapy. Following PCR amplification, we cloned and sequenced HVR-1. Pretreatment serum samples from 13 individuals with chronic hepatitis C whose virus was subsequently eradicated by treatment were compared with samples from 13 nonresponders matched according to the major factors known to influence the response, i.e., sex, genotype, and pretreatment serum HCV RNA concentration. The degree of virus variation was assessed by analyzing 20 clones per sample and by calculating nucleotide sequence entropy (complexity) and genetic distances (diversity). Types of mutational changes were also determined by calculating nonsynonymous substitutions per nonsynonymous site (Ka) and synonymous substitutions per synonymous site (Ks). The paired-comparison analysis of the nucleotide sequence entropy and genetic distance showed no statistical differences between responders and nonresponders. By contrast, nonsynonymous substitutions were more frequent than synonymous substitutions (P ≤ 0.05) in responders, but there was no significant difference in nonresponders. Nonsynonymous substitutions tended to be more frequent than synonymous substitutions in women (P = 0.06) but not in men. Nucleotide entropy and genetic distances were significantly related to serum RNA concentration (P ≤ 0.01). Our findings suggest that after controlling for the major determinants of interferon response, neither complexity nor diversity of the HVR-1 region is associated per se with virus eradication. Because a higher proportion of nonsynonymous substitutions than synonymous substitutions was found only in responders, host anti-HCV-specific immune response rather than viral factors may be playing an important role in the interferon response.
机译:丙型肝炎病毒(HCV)群体作为称为准种的异质病毒的混合物在体内持续存在。这些变体的遗传异质性与它们对抗病毒治疗的反应之间的关系仍有待阐明。我们研究了26种病毒株,以确定HCV基因组的高变区1(HVR-1)对α干扰素(IFN-α)治疗的有效性的影响。 PCR扩增后,我们克隆并测序了HVR-1。将13例慢性丙型肝炎患者的治疗前血清样本与随后通过治疗消除病毒的13种无反应者样本进行了比较,这些样本根据已知的影响应答的主要因素(即性别,基因型和治疗前血清HCV RNA浓度)进行了匹配。通过分析每个样品20个克隆并通过计算核苷酸序列的熵(复杂性)和遗传距离(多样性)来评估病毒变异的程度。还通过计算每个非同义位点(Ka)和每个同义位点(Ks)的同义取代来确定突变变化的类型。核苷酸序列熵和遗传距离的配对比较分析显示应答者和非应答者之间无统计学差异。相比之下,在响应者中,非同义替换比同义替换(P≤0.05)更频繁,但在非响应者中没有显着差异。在女性中,非同义替换比同义替换的频率更高(P = 0.06),而在男性中则没有。核苷酸的熵和遗传距离与血清RNA浓度显着相关(P≤0.01)。我们的发现表明,在控制干扰素应答的主要决定因素之后,HVR-1区域的复杂性或多样性本身与根除病毒无关。因为仅在应答者中发现比同义取代更高比例的非同义取代,所以宿主抗HCV特异性免疫应答而非病毒因子可能在干扰素应答中起重要作用。

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