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Genetic variability in hepatitis C virus and its role in antiviral treatment response.

机译:丙型肝炎病毒的遗传变异性及其在抗病毒治疗反应中的作用。

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Hepatitis C virus (HCV) is a major health problem worldwide, infecting an estimated 170 million people. The high genetic variability of HCV contributes to the chronicity of hepatitis C. Here, we report results from a large-scale sequence analysis of 67 patients infected with HCV genotype 1, 23 with subtype 1a and 44 with subtype 1b. Two regions of the HCV genome were analysed in samples prior to combined therapy with alpha interferon plus ribavirin, one compressing the hypervariable regions (HVR1, HVR2 and HVR3) of the E2 glycoprotein and another one including the interferon-sensitive determining region (ISDR) and the V3 domain of the NS5A protein. Genetic diversity measures showed a clear tendency to higher genetic variability levels in nonresponder patients to antiviral treatment than in responder patients, although highly disperse values were present within each response group for both subtypes. A more detailed analysis of amino acid composition revealed the presence of several subtype-specific variants in a few positions, but no discriminating positions between responder and nonresponder patients were detected. Our results also revealed that most amino acid positions were highly conserved, especially for subtype 1a. We conclude that the outcome of the antiviral treatment might depend not only on the nature of one or a few independent positions, but more likely on the combination of several positions along the HCV genome. Moreover, the own host's ability to generate an appropriate systemic response, in combination with the action of antivirals, is also likely to be essential for treatment outcome.
机译:丙型肝炎病毒(HCV)是全球主要的健康问题,估计感染了1亿7千万人。 HCV的高遗传变异性有助于丙型肝炎的慢性病。在这里,我们报告了67例HCV基因型1、23、1a型和44b,1b型患者的大规模测序结果。在用α干扰素加利巴韦林联合治疗之前,对样品中的HCV基因组的两个区域进行了分析,一个区域压缩E2糖蛋白的高变区(HVR1,HVR2和HVR3),另一个区域包括干扰素敏感的决定区(ISDR)和NS5A蛋白的V3结构域。遗传多样性测度显示,对抗病毒治疗无反应的患者比对反应的患者有更高的遗传变异性趋势,尽管两种亚型在每个反应组中均存在高度分散的值。氨基酸组成的更详细分析显示,在几个位置上存在几种亚型特异性变体,但未检测到反应者和非反应者之间的区别性位置。我们的结果还表明,大多数氨基酸位置是高度保守的,尤其是对于亚型1a。我们得出结论,抗病毒治疗的结果可能不仅取决于一个或几个独立位置的性质,而且更可能取决于沿HCV基因组的几个位置的组合。而且,自身宿主产生适当的全身反应的能力以及抗病毒药的作用,对于治疗结果也很重要。

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