首页> 美国卫生研究院文献>Journal of Virology >Evolution of Hepatitis C Virus Quasispecies in Hypervariable Region 1 and the Putative Interferon Sensitivity-Determining Region during Interferon Therapy and Natural Infection
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Evolution of Hepatitis C Virus Quasispecies in Hypervariable Region 1 and the Putative Interferon Sensitivity-Determining Region during Interferon Therapy and Natural Infection

机译:干扰素治疗和自然感染过程中高变区1和推定的干扰素敏感性决定区中丙型肝炎病毒准种的演变

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摘要

To study hepatitis C virus (HCV) genetic mutation during interferon (IFN) therapy, the temporal changes in HCV quasispecies heterogeneity were compared before and after treatment for nine patients infected with HCV genotype 1, including four nonresponders, four responders who relapsed after therapy, and one responder who experienced a breakthrough of viremia during therapy. Nine untreated patients with an average time between specimens of 8.4 years served as controls. Sequences from the second envelope glycoprotein gene hypervariable region 1 (HVR1) and the putative IFN sensitivity-determining region (ISDR) of the nonstructural NS5A gene were analyzed by heteroduplex mobility assays and nucleotide sequencing. A strong positive correlation was found between the percent change in a heteroduplex mobility ratio (HMR) and percent change in nucleotide sequence (r = 0.941, P < 0.001). The rate of fixation of mutations in the HVR1 was significantly higher for IFN-treated patients than for controls (6.97 versus 1.31% change in HMR/year; P = 0.02). Similarly, a higher rate of fixation of mutations was observed in the ISDR for IFN-treated patients than for untreated controls, although the result was not significant (1.45 versus 0.15 amino acid changes/year; P = 0.12). On an individual patient basis, IFN therapy was associated with measurable HVR1 and ISDR mutation in nine of nine (100%) and two of nine (22.2%) patients, respectively. Evolution to IFN-resistant ISDR sequences was observed in only one of nine IFN-treated patients. These data suggest that IFN therapy frequently exerts pressure on the HCV envelope region, while pressure on the ISDR was evident in only a subset of patients. Thus, the selection pressures evoked on HCV genotype 1 quasispecies during IFN therapy appear to differ among different patients.
机译:为了研究干扰素(IFN)治疗期间的丙型肝炎病毒(HCV)基因突变,比较了9例HCV基因型1感染患者在治疗前后HCV准种异质性的时间变化,包括4名无反应者,4名在治疗后复发的反应者,一位在治疗期间经历病毒血症突破的反应者。九名未经治疗的患者平均样本间隔为8.4年,作为对照组。通过异源双链迁移分析和核苷酸测序分析了非结构性NS5A基因第二个包膜糖蛋白基因高变区1(HVR1)和推定的IFN敏感性决定区(ISDR)的序列。在异源双链迁移率(HMR)的百分比变化与核苷酸序列的百分比变化之间发现强正相关(r = 0.941,P <0.001)。接受IFN治疗的患者中HVR1突变的固定率显着高于对照组(HMR /年变化为6.97比1.31%; P = 0.02)。同样,用IFN治疗的患者在ISDR中观察到的突变固定率高于未治疗的对照,尽管结果并不显着(1.45对0.15个氨基酸/年; P = 0.12)。在个体患者的基础上,IFN治疗分别与9名患者中的9名(100%)和9名患者中的2名(22.2%)的HVR1和ISDR突变相关。在九名接受IFN治疗的患者中,只有一位观察到向IFN抗性ISDR序列的进化。这些数据表明,干扰素治疗经常对HCV包膜区域施加压力,而对ISDR的压力仅在一部分患者中明显。因此,在IFN治疗期间,对HCV基因1型准种引起的选择压力似乎在不同患者之间有所不同。

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