核受体反应元件在乙型肝炎病毒复制中的关键作用
Critical roles of nuclear receptor response elements in replication of hepatitis B virus.
作者信息
Yu X, Mertz J E
机构信息
McArdle Laboratory for Cancer Research, University of Wisconsin Medical School, Madison, Wisconsin 53706-1599, USA.
出版信息
J Virol. 2001 Dec;75(23):11354-64. doi: 10.1128/JVI.75.23.11354-11364.2001.
Functional analysis of the roles of the nuclear receptor response elements (NRREs) in the transcription and replication of hepatitis B virus (HBV) in the context of its whole genome has been hampered by the extensive overlapping of the NRREs with the regions encoding viral proteins. We introduced point mutations that inactivate the NRREs individually without altering the open reading frames of viral proteins. These mutations in the context of a plasmid containing 1.2 copies of the HBV genome were transiently transfected into the human hepatoma cell line Huh7. Inactivation of the NRRE in either the preC promoter (NRRE(preC)) or enhancer I (NRRE(enhI)) led to moderate reductions in synthesis of viral RNAs. Concurrent inactivation of both NRREs led to 7- to 8-fold reductions in synthesis of the preC, pregenomic, and preS RNAs and a 15-fold reduction in synthesis of the S RNA. The accumulation of viral DNA in the cytoplasmic nucleocapsids and virion particles in the culture medium was also reduced seven- to eightfold. These results suggest that these NRREs are critical for the efficient propagation of HBV in hepatocytes. In cotransfection experiments we also found that overexpression of PPARalpha-RXRalpha in the presence of their respective ligands led to a fourfold increase in pregenomic RNA synthesis and a four- to fivefold increase in viral DNA synthesis, while it had little or no effect on synthesis of the other viral RNAs. Similar effects were observed with overexpression of PPARgamma-RXRalpha in the presence of their respective ligands. This activation was dependent on NRRE(preC), because the increase in synthesis of viral RNA and DNA was not observed when this site was mutated. Likewise, no activation of synthesis of pregenomic RNA and viral DNA by PPARalpha-RXRalpha was observed in a naturally occurring NRRE(preC)(-) mutant of HBV. Our results suggest that interactions between nuclear receptors and NRREs present in the HBV genome may play critical roles in regulating its transcription and replication during HBV infection of hepatocytes.
核受体反应元件(NRREs)在乙型肝炎病毒(HBV)全基因组背景下对其转录和复制作用的功能分析,一直受到NRREs与编码病毒蛋白区域广泛重叠的阻碍。我们引入了点突变,这些突变能单独使NRREs失活,而不改变病毒蛋白的开放阅读框。将这些突变引入含有1.2份HBV基因组的质粒中,然后瞬时转染到人肝癌细胞系Huh7中。前C启动子(NRRE(preC))或增强子I(NRRE(enhI))中的NRRE失活,会导致病毒RNA合成适度减少。两个NRRE同时失活,会导致前C、前基因组和前S RNA的合成减少7至8倍,S RNA的合成减少15倍。培养基中细胞质核衣壳和病毒粒子内病毒DNA的积累也减少了7至8倍。这些结果表明,这些NRREs对HBV在肝细胞中的有效传播至关重要。在共转染实验中,我们还发现,在各自配体存在的情况下,过表达PPARα-RXRα会导致前基因组RNA合成增加4倍,病毒DNA合成增加4至5倍,而对其他病毒RNA的合成几乎没有影响。在各自配体存在的情况下,过表达PPARγ-RXRα也观察到了类似的效果。这种激活依赖于NRRE(preC),因为当该位点发生突变时,未观察到病毒RNA和DNA合成的增加。同样,在HBV的自然发生的NRRE(preC)(-)突变体中,未观察到PPARα-RXRα对前基因组RNA和病毒DNA合成的激活作用。我们的结果表明,核受体与HBV基因组中存在的NRREs之间的相互作用,可能在肝细胞感染HBV期间调节其转录和复制中起关键作用。
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