Effects of hepatitis B virus mutations on its replication and liver disease severity.

The Open Virology Journal Pub Date : 2013-01-01 Epub Date: 2013-01-23 DOI:10.2174/1874357901307010012
Abdulrahim Hakami, Abdelwahid Ali, Ahmed Hakami
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Abstract

Hepatitis B virus (HBV), nowadays, is one of the major human pathogens worldwide. Approximately, 400 million people worldwide have chronic HBV infection. Only 5% of persons infected during adulthood develop chronic infection. The reverse is true for those infected at birth or in early childhood, i.e. more than 90% of these persons progress to chronic infection. Currently, eight different genotypes o f HBV have been identified, differing in nucleotide sequence by greater than 8%. In addition, numerous subgenotypes have a l s o been recognized based on the nucleotide sequence variability of 4- 8%. It has invariably been found that these genotypes and mutations play a pivotal role in the liver disease aggravation and virus replication. The precore mutations (G1896A) and the double mutation (T1762/A1764) in the basal core promoter are important mutations that alter expression of the hepatitis B e antigen (HBeAg). The HBeAg is important for establishing viral persistence. The precore G1896A mutation abrogates the expression of HBeAg. Numerous other mutations alter the disease severity and progression. It is predictive that the infected patient has high risk of hepatocellular carcinoma if the genotype C is incriminated or if HBV possesses basal core promoter double mutation. Association of the remaining genotypes have been noted but with less degree than genotype C. Phenotypic assays of the different HBV protein markers with different molecular techniques illustrate the replication efficiency of the virus in cell lines. This review will discuss various mutations into their association with liver disease severity and progression as well as virus replication.

乙型肝炎病毒变异对其复制和肝病严重程度的影响。
乙型肝炎病毒(HBV)是当今全球主要的人类病原体之一。全球约有 4 亿人患有慢性乙型肝炎病毒感染。只有 5%的成年感染者会发展为慢性感染。出生时或幼儿期感染者的情况正好相反,即 90% 以上的感染者会发展为慢性感染。目前,已发现八种不同的 HBV 基因型,其核苷酸序列差异超过 8%。此外,根据 4-8%的核苷酸序列差异,还发现了许多亚基因型。研究发现,这些基因型和变异在肝病恶化和病毒复制中起着关键作用。基础核心启动子中的前核心突变(G1896A)和双突变(T1762/A1764)是改变乙肝 e 抗原(HBeAg)表达的重要突变。HBeAg 对于建立病毒持久性非常重要。前核 G1896A 突变会抑制 HBeAg 的表达。其他许多突变也会改变疾病的严重程度和进展。如果基因型为 C 或 HBV 具有基核启动子双突变,则可预测感染者罹患肝细胞癌的风险很高。通过不同的分子技术对不同的 HBV 蛋白标记进行表型检测,可以说明病毒在细胞系中的复制效率。本综述将讨论各种基因突变与肝病严重程度和进展以及病毒复制的关系。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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