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Genetic variability of hepatitis C virus in HBV/HCV co-infection and HCV single-infection.

机译:HBV / HCV合并感染和HCV单一感染中丙型肝炎病毒的遗传变异性。

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摘要

To describe the virological profile of HCV in HBV/HCV co-infection, we investigated the variability of HVR-1 and NS5A domains, which may be involved in viral persistence and replication efficiency. We studied 95 patients: 37 with serological markers of HBV/HCV co-infection, 33 with single HBV and 25 with single HCV infection. HVR-1 complexity and NS5A gene variability were respectively explored by means of PCR-SSCP and direct sequencing. Serum HBV genomes were detected in all coinfected patients: 19 also had circulating HCV particles (group BC-I), whereas HCV were undetectable in the other 18 (group BC-II). Group BC-I was characterised by a significantly lower HBV replication capacity, that reflects the replicative dominance of HCV, although the dominant virus had the same degree of variability as the HCV in single infection. HBV viral load was higher in group BC-II, but not significantly different from that observed in the single infection. Our data indicate an alternation in replicative dominance in co-infection: HBV can suppress HCV replication to undetectable levels, whereas HCV may reduce but does not abrogate the replication capacity of HBV. Furthermore, in the cases of HCV dominance, circulating HBV genomes did not have a significant effect on the viral heterogeneity of HCV.
机译:为了描述HCV在HBV / HCV共感染中的病毒学特征,我们调查了HVR-1和NS5A域的变异性,这可能与病毒的持久性和复制效率有关。我们研究了95例患者:37例具有HBV / HCV合并感染的血清学标志物,33例患有单个HBV,25例患有单个HCV感染。通过PCR-SSCP和直接测序分别研究了HVR-1的复杂性和NS5A基因的变异性。在所有合并感染的患者中均检测到血清HBV基因组:19例也有循环的HCV颗粒(BC-I组),而其他18例(BC-II组)则检测不到HCV。 BC-1组的特征是HBV复制能力明显降低,这反映了HCV的复制优势,尽管在一次感染中优势病毒的变异性与HCV相同。 BC-II组的HBV病毒载量较高,但与单次感染无明显差异。我们的数据表明,共感染中复制优势的改变:HBV可以将HCV复制抑制到无法检测的水平,而HCV可以降低但不会消除HBV的复制能力。此外,在HCV优势的情况下,循环的HBV基因组对HCV的病毒异质性没有显着影响。

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