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乙型肝炎病毒基因组变异的临床意义和公共卫生意义。

Clinical relevance and public health significance of hepatitis B virus genomic variations.

出版信息

World J Gastroenterol. 2009 Dec 14;15(46):5761-9. doi: 10.3748/wjg.15.5761.

Abstract

Ten hepatitis B virus (HBV) genotypes (A-J) and 34 HBV subgenotypes have been identified so far. HBV genotypes and subgenotypes have distinct geographical distributions, and have been shown to differ with regard to clinical outcome, prognosis, and response to interferon treatment. Infection with subgenotype A2 is frequently associated with high viral load, resulting in acute infection via horizontal transmission. Genotypes A and B are more sensitive to interferon treatment than genotypes D and C, respectively. Genotype B is more frequent in acute hepatitis than genotype C, whereas genotype C (C2) is more frequently associated with an increased risk of hepatocellular carcinoma (HCC), mostly cirrhotic, as compared with genotype B (B2). Genotype mixture is associated with high viral load and worse outcome of HBV infection. HBV mutations in the S genes, especially amino acids substitution at position 145 (G145R), are associated with immune escape, whereas mutations in the PreS or S genes which impair HBsAg secretion could present a risk to blood safety. HBV variants harboring mutations in the viral polymerase gene that confer resistance to nucleoside analogs may be selected during antiviral therapy. Different genotypes have distinct mutation patterns in the PreS and EnhII/BCP/Precore regions. PreS deletions, C1653T, T1753V, and A1762T/G1764A are associated with an increased risk of HCC. HCC-associated HBV mutants may not transmit via mother-to-child transmission, and are likely generated during HBV-induced pathogenesis. Examination of HBV mutations alone or in combination and host genetic susceptibility will be helpful in classifying the HBV-infected subjects who will develop HCC and need active anti-viral treatments.

摘要

目前已鉴定出 10 种乙型肝炎病毒 (HBV) 基因型 (A-J) 和 34 种 HBV 亚型。HBV 基因型和亚型具有不同的地理分布,并已显示在临床结果、预后和对干扰素治疗的反应方面存在差异。亚基因型 A2 的感染常与高病毒载量相关,通过水平传播导致急性感染。与基因型 D 和 C 相比,基因型 A 和 B 对干扰素治疗更敏感。基因型 B 在急性肝炎中比基因型 C 更为常见,而基因型 C(C2)与肝细胞癌 (HCC) 的风险增加相关,与基因型 B(B2)相比,主要与肝硬化相关。基因型混合与 HBV 感染的高病毒载量和不良结局相关。S 基因中的 HBV 突变,特别是位置 145 处的氨基酸取代 (G145R),与免疫逃逸相关,而 PreS 或 S 基因中的突变会损害 HBsAg 的分泌,可能会对血液安全构成风险。在抗病毒治疗期间,可能会选择在病毒聚合酶基因中具有耐药性突变的 HBV 变体。不同的基因型在 PreS 和 EnhII/BCP/Precore 区域具有不同的突变模式。PreS 缺失、C1653T、T1753V 和 A1762T/G1764A 与 HCC 风险增加相关。与 HCC 相关的 HBV 突变体可能不会通过母婴传播,并且可能在 HBV 诱导的发病机制中产生。单独或联合检查 HBV 突变和宿主遗传易感性将有助于对发生 HCC 并需要积极抗病毒治疗的 HBV 感染患者进行分类。

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