Wang Hui-Ching, Huang Wenya, Lai Ming-Der, Su Ih-Jen
Division of Clinical Research, National Health Research Institutes, National Cheng Kung University College of Medicine, Tainan 704, Taiwan.
Cancer Sci. 2006 Aug;97(8):683-8. doi: 10.1111/j.1349-7006.2006.00235.x.
Although hepatitis B virus (HBV) has been documented to cause hepatocellular carcinoma (HCC), the exact role of HBV in the development of HCC remains enigmatic. Several hypotheses have been proposed to explain the potential mechanism, including insertional mutagenesis of HBV genomes and transcriptional activators of HBV gene products such as hepatitis B x protein (HBx) and truncated middle S mutants. In the past few years, we have identified two types of large HBV surface antigens (LHBs) with deletions at the pre-S1 (DeltaS1-LHBs) and pre-S2 (DeltaS2-LHBs) regions in ground glass hepatocytes. The pre-S mutant LHBs are retained in the endoplasmic reticulum (ER) and escape from immune attack. The pre-S mutants, particularly DeltaS2-LHBs, are increasingly prevalent in patients with hepatitis B e antigen (HBeAg)-positive chronic HBV infection, ranging from 6% before the 3rd decade to 35% in the 6th decade. In HCC patients, the two pre-S mutants were detected in 60% of HCC patients, in the serum and in HCC tissues. Pre-S mutant LHBs can initiate ER stress to induce oxidative DNA damage and genomic instability. Furthermore, pre-S mutant LHBs can upregulate cyclooxygenase-2 and cyclin A to induce cell cycle progression and proliferation of hepatocytes. In transgenic mice, the pre-S mutants can induce dysplasia of hepatocytes and development of HCC. In a nested control study, the presence of pre-S mutants carried a high risk of developing HCC in HBV carriers. In summary, the findings we describe in this review suggest a potential role for HBV pre-S mutants in HBV-related hepatocarcinogenesis, providing a model of viral carcinogenesis associated with ER stress.
尽管已有文献证明乙型肝炎病毒(HBV)可导致肝细胞癌(HCC),但HBV在HCC发生发展中的确切作用仍不清楚。人们提出了几种假说来解释其潜在机制,包括HBV基因组的插入诱变以及HBV基因产物如乙型肝炎x蛋白(HBx)和截短的中S突变体的转录激活。在过去几年中,我们在毛玻璃样肝细胞中发现了两种在前S1区(ΔS1-LHBs)和前S2区(ΔS2-LHBs)有缺失的大HBV表面抗原(LHBs)。前S突变体LHBs保留在内质网(ER)中并逃避免疫攻击。前S突变体,尤其是ΔS2-LHBs,在乙型肝炎e抗原(HBeAg)阳性的慢性HBV感染患者中越来越普遍,从第三个十年前的6%上升到第六个十年的35%。在HCC患者中,在60%的HCC患者的血清和HCC组织中检测到了这两种前S突变体。前S突变体LHBs可引发内质网应激,诱导氧化性DNA损伤和基因组不稳定。此外,前S突变体LHBs可上调环氧化酶-2和细胞周期蛋白A,以诱导肝细胞的细胞周期进程和增殖。在转基因小鼠中,前S突变体可诱导肝细胞发育异常和HCC的发生。在一项巢式对照研究中,前S突变体的存在使HBV携带者发生HCC的风险很高。总之,我们在本综述中描述的研究结果表明HBV前S突变体在HBV相关肝癌发生中具有潜在作用,为与内质网应激相关的病毒致癌作用提供了一个模型。