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2b型丙型肝炎病毒(HCV)感染患者3年内丙型肝炎病毒高变区1(HVR1)异质性及HVR1抗体反应的个体发生情况

Ontogeny of hepatitis C virus (HCV) hypervariable region 1 (HVR1) heterogeneity and HVR1 antibody responses over a 3 year period in a patient infected with HCV type 2b.

作者信息

Majid A, Jackson P, Lawal Z, Pearson G M, Parker H, Alexander G J, Allain J P, Petrik J

出版信息

J Gen Virol. 1999 Feb;80 ( Pt 2):317-325. doi: 10.1099/0022-1317-80-2-317.

DOI:10.1099/0022-1317-80-2-317
PMID:10073690
Abstract

Hypervariable region 1 (HVR1) sequences of 96 clones at six time-points representing 27 variants in two major and one minor group were identified in a patient with chronic hepatitis C virus (HCV) infection over 3 years. Major and selected minor variants were used to design synthetic peptides corresponding to the HVR1 C terminus. Peptide ELISA reactivity with IgG was plotted against the corresponding clone frequency, and three patterns emerged: (1) three peptides were unreactive; (2) antibodies against two peptides followed emergence of the corresponding variant, suggesting isolate-specificity; (3) antibodies against four peptides preceded the appearance of the corresponding variant, indicating cross-reactivity or previous exposure. Cross-reactivity was investigated further: sera from six time-points were tested against 11 unrelated HVR1 peptides, seven of which (63.6%) showed cross-reactivity at all time-points. Cross-reactivity of nine patient-specific peptides tested against a panel of 45 heterologous sera from chronic HCV carriers ranged between 0 and 20%. Only three of 27 variants appeared at more than one time-point and in two cases specific and/or cross-reactive HVR1 antibodies coexisted with the corresponding variant, consistent with emergence of escape mutants. In addition, analysis of HVR1 IgG reactivity within a group of closely related patient-specific peptides revealed a loss of reactivity in one peptide attributable to a single amino acid substitution. Interferon-alpha treatment considerably reduced viral RNA but, paradoxically, heterogeneity increased.

摘要

在一名慢性丙型肝炎病毒(HCV)感染患者3年多的时间里,在六个时间点鉴定出了96个克隆的高变区1(HVR1)序列,这些序列代表两个主要组和一个次要组中的27个变体。主要变体和选定的次要变体用于设计对应于HVR1 C末端的合成肽。将肽ELISA与IgG的反应性与相应的克隆频率作图,出现了三种模式:(1)三种肽无反应;(2)针对两种肽的抗体随着相应变体的出现而出现,表明具有分离株特异性;(3)针对四种肽的抗体在相应变体出现之前出现,表明存在交叉反应或既往暴露。进一步研究交叉反应:对来自六个时间点的血清进行11种无关HVR1肽的检测,其中七种(63.6%)在所有时间点均显示交叉反应。针对一组来自慢性HCV携带者的45种异源血清检测的9种患者特异性肽的交叉反应范围在0%至

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