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肝硬化患者丙型肝炎病毒HVR1准种的遗传复杂性和血清反应性

Genetic complexity and serum reactivity of HVR1 quasispecies of hepatitis C virus in patients with cirrhosis.

作者信息

Fan Xiaofeng, Di Bisceglie Adrian M

机构信息

Department of Internal Medicine, Saint Louis University School of Medicine, Missouri 63110-0250, USA.

出版信息

Am J Gastroenterol. 2002 Jun;97(6):1489-95. doi: 10.1111/j.1572-0241.2002.05794.x.

Abstract

OBJECTIVE

The RNA genome of hepatitis C virus varies considerably, especially within the hypervariable region 1 (HVR1), a domain located on the 5' end of the E2/NS1 envelope region. Our previous study has suggested there were greater numbers of quasispecies in the liver than in matched serum, independent of the viral load. However, the significance of this finding has not been examined extensively at genetic and serological levels.

METHODS

By large scale cloning and sequencing, we studied the genetic complexity of HVR1 quasispecies in two selected patients with cirrhosis. The serum reactivity of peptides representing different HVR1 quasispecies isolated from these cases was also estimated by standard ELISA format.

RESULTS

We found the same major (dominant and/or subdominant) viral quasispecies variants in serum and in the cirrhotic liver. Genetic analysis suggested that the evolutionary pressure on HVR1 was higher than on its flanking region in quasispecies derived from the liver, whereas this trend is attenuated in quasispecies from serum. The immunoreactivity to peptides representing different HVR1 quasispecies variants showed considerable cross-reactivity with heterologous sera, whereas the reactivity was strongest against the dominant HVR1 peptide over time in homologous sera.

CONCLUSIONS

These findings indicate that the formation and selection of HVR1 quasispecies may not be driven solely by humoral immune pressure, at least in these two cases.

摘要

目的

丙型肝炎病毒的RNA基因组差异很大,尤其是在高变区1(HVR1)内,该区域位于E2/NS1包膜区域的5'端。我们之前的研究表明,与病毒载量无关,肝脏中的准种数量比配对血清中的更多。然而,这一发现的意义尚未在基因和血清学水平上进行广泛研究。

方法

通过大规模克隆和测序,我们研究了两名选定的肝硬化患者中HVR1准种的遗传复杂性。还通过标准ELISA方法评估了从这些病例中分离出的代表不同HVR1准种的肽段的血清反应性。

结果

我们在血清和肝硬化肝脏中发现了相同的主要(显性和/或次显性)病毒准种变体。遗传分析表明,在源自肝脏的准种中,HVR1上的进化压力高于其侧翼区域,而在血清准种中这种趋势减弱。对代表不同HVR1准种变体的肽段的免疫反应性显示与异源血清有相当大的交叉反应性,而在同源血清中,随着时间的推移,对显性HVR1肽段的反应性最强。

结论

这些发现表明,至少在这两个病例中,HVR1准种的形成和选择可能不仅仅由体液免疫压力驱动。

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