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The molecular virology of hepatitis B virus

机译:乙型肝炎病毒的分子病毒学

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Hepatitis B virus (HBV) is one of the smallest enveloped DNA viruses and the prototype member of the family of Hepadnaviridae that causes acute and chronic infections of mammals (including human) and birds. HBV has evolved an extreme adaptation and dependency to differentiated hepatocytes of its host. Despite its very limited coding capacity with only four open-reading frames, HBV is able to evade the immune system of the host and persist lifelong within infected hepatocytes. During active replication, HBV produces enormous viral loads in the blood and a massive surplus of subviral surface antigen particles in the serum of infected patients without killing their hepatocytes. Together with the use of a reverse transcriptase during replication, it provides an enormous genetic flexibility for selection of viral mutants upon selective pressure, for example, by the immune system or antiviral therapy. In addition, viral wild-type and mutated genomes are stably archived in the nucleus of the infected hepatocyte in an episomal DNA form that provides independence from cellular replication or integration within the host genome. We are just beginning to understand the delicate molecular and cellular interactions during the HBV replicative cycle within infected hepatocytes, so further studies are urgently needed to provide a better basis for further diagnostic and therapeutic options.
机译:乙型肝炎病毒(HBV)是最小的包膜DNA病毒之一,是引起哺乳动物(包括人)和鸟类的急性和慢性感染的肝炎病毒科的原型成员。 HBV对宿主的分化肝细胞已经形成了极端的适应性和依赖性。尽管HBV的编码能力非常有限,只有四个开放阅读框,但它能够逃避宿主的免疫系统,并在感染的肝细胞中持续终生。在主动复制过程中,HBV在血液中产生巨大的病毒载量,在感染患者的血清中产生大量过量的亚病毒表面抗原颗粒,而不会杀死他们的肝细胞。与在复制过程中使用逆转录酶一起,在选择压力(例如通过免疫系统或抗病毒疗法)后,它为选择病毒突变体提供了巨大的遗传灵活性。另外,病毒野生型和突变的基因组以游离DNA形式稳定地保存在被感染肝细胞的核中,该游离DNA形式提供了与宿主基因组内细胞复制或整合的独立性。我们才刚刚开始了解被感染的肝细胞在HBV复制周期中微妙的分子和细胞相互作用,因此迫切需要进一步的研究,以便为进一步的诊断和治疗选择提供更好的基础。

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