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全球乙肝病毒基因型的遗传多样性与肝细胞癌风险

Worldwide genetic diversity of HBV genotypes and risk of hepatocellular carcinoma.

作者信息

Pujol Flor Helene, Navas Maria-Cristina, Hainaut Pierre, Chemin Isabelle

机构信息

Laboratorio de Virología Molecular, CMBC, IVIC, Apdo 20632, Caracas 1020-A, Venezuela.

出版信息

Cancer Lett. 2009 Dec 1;286(1):80-8. doi: 10.1016/j.canlet.2009.07.013. Epub 2009 Aug 14.

Abstract

Hepatitis B viruses (HBV) are responsible for over 50% of the worldwide attributable risk of hepatocellular carcinoma (HCC) and this figure increases even further in regions of high endemicity. Systematic sequencing of HBV genomes has identified that this common virus existed as eight distinct genotypes (denoted A-H), each regrouping variants with less than 8% divergence in their DNA sequence. These genotypes differ by their geographic distribution in populations around the globe. There is evidence that HBV genotypes also differ by their pathogenic properties, including their risk of persistence as chronic infection and their capacity to induce precursor disease or cancer. On the other hand, HBV genes may undergo mutations that become selected during the course of chronic infection and progressive liver disease. The most significant of these mutations in the context of HCC are those occurring in the pre-core (Pre-C) and basal core promoter (BCP) regions. These mutations may upregulate HBV expression and increase its virulence. These mutations may occur in all HBV genotypes but are more common in genotypes associated with more severe disease and cancer, in particular genotype C. Understanding the molecular basis of pathological variations between HBV variants is critical for prediction of disease severity. It will also be important to determine whether differences among genotypes may have an impact on the long-term protective efficacy of universal HBV vaccination.

摘要

乙型肝炎病毒(HBV)导致了全球肝细胞癌(HCC)归因风险的50%以上,在高流行地区这一比例甚至更高。对HBV基因组进行系统测序发现,这种常见病毒以八种不同的基因型(分别标记为A - H)存在,每种基因型又将DNA序列差异小于8%的变异体归为一组。这些基因型在全球人群中的地理分布有所不同。有证据表明,HBV基因型在致病特性方面也存在差异,包括其作为慢性感染持续存在的风险以及诱导前驱疾病或癌症的能力。另一方面,HBV基因可能会发生突变,这些突变在慢性感染和进行性肝病过程中会被选择出来。在HCC背景下,这些突变中最重要的是发生在前核心(Pre - C)区和基本核心启动子(BCP)区的突变。这些突变可能会上调HBV表达并增加其毒力。这些突变可能发生在所有HBV基因型中,但在与更严重疾病和癌症相关的基因型中更为常见,尤其是C基因型。了解HBV变异体之间病理差异的分子基础对于预测疾病严重程度至关重要。确定基因型之间的差异是否可能对通用HBV疫苗接种的长期保护效果产生影响也很重要。

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