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乙型肝炎病毒作为人类肝细胞癌中的一种插入诱变剂。

Hepatitis B virus as an insertional mutagene in a human hepatocellular carcinoma.

作者信息

Dejean A, de Thé H

机构信息

Unité de Recombinaison et Expression Génétique (INSERM U.163, CNRS UA 271), Institut Pasteur, Paris, France.

出版信息

Mol Biol Med. 1990 Jun;7(3):213-22.

PMID:2170809
Abstract

Chronic hepatitis B virus (HBV) infection is etiologically related to human hepatocellular carcinoma (HCC). Most HCCs contain integrated HBV DNA in the liver cellular DNA, suggesting that the integration may be involved in carcinogenesis. From a comparison of a single HBV integration site present in a hepatoma with the corresponding unoccupied site in the non-tumourous tissue of the same liver, we have shown that HBV DNA inserted in a putative cellular exon with striking similarity to the DNA-binding domain of the thyroid/steroid hormone receptors. The corresponding cDNA has been isolated (hap gene) and shown to encode the retinoic acid receptor. In the original patient, integration took place so that the first codons of the viral surface protein gene became fused in frame with most of the hap gene. Because retinoic acid is known to regulate the transcription of target genes crucial for cellular growth and differentiation, it is most probable that consequent to the HBV insertion, hap, usually transcribed at a very low level in normal hepatocytes, became inappropriately expressed as an altered chimaeric retinoic acid receptor, thus contributing to the cell transformation. These results strongly support the possibility that HBV may play a direct role in liver carcinogenesis by insertional mutagenesis.

摘要

慢性乙型肝炎病毒(HBV)感染在病因学上与人类肝细胞癌(HCC)相关。大多数肝癌在肝细胞DNA中含有整合的HBV DNA,这表明整合可能参与致癌过程。通过比较肝癌中存在的单个HBV整合位点与同一肝脏非肿瘤组织中相应的未占据位点,我们发现插入到一个假定的细胞外显子中的HBV DNA与甲状腺/类固醇激素受体的DNA结合结构域具有惊人的相似性。相应的cDNA已被分离出来(hap基因),并显示其编码视黄酸受体。在最初的患者中,发生了整合,使得病毒表面蛋白基因的第一个密码子与大部分hap基因读框融合。由于已知视黄酸可调节对细胞生长和分化至关重要的靶基因的转录,因此很可能在HBV插入后,通常在正常肝细胞中以极低水平转录的hap基因,作为一种改变的嵌合视黄酸受体而异常表达,从而导致细胞转化。这些结果有力地支持了HBV可能通过插入诱变在肝癌发生中起直接作用的可能性。

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