首页> 美国卫生研究院文献>Journal of Virology >Hepatitis Delta Virus Replication Generates Complexes of Large Hepatitis Delta Antigen and Antigenomic RNA That Affiliate with and Alter Nuclear Domain 10
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Hepatitis Delta Virus Replication Generates Complexes of Large Hepatitis Delta Antigen and Antigenomic RNA That Affiliate with and Alter Nuclear Domain 10

机译:肝炎三角洲病毒复制会产生大肝炎三角洲抗原和抗基因组RNA的复合物这些抗原与并改变核域10

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摘要

Hepatitis delta virus (HDV), a single-stranded RNA virus, bears a single coding region whose product, the hepatitis delta antigen (HDAg), is expressed in two isoforms, small (S-HDAg) and large (L-HDAg). S-HDAg is required for replication of HDV, while L-HDAg inhibits viral replication and is required for the envelopment of the HDV genomic RNA by hepatitis B virus proteins. Here we have examined the spatial distribution of HDV RNA and proteins in infected nuclei, with particular reference to specific nuclear domains. We found that L-HDAg was aggregated in specific nuclear domains and that over half of these domains were localized beside nuclear domain 10 (ND10). At later times, ND10-associated proteins like PML were found in larger HDAg complexes that had developed into apparently hollow spheres. In these larger complexes, PML was found chiefly in the rims of the spheres, while the known ND10 components Sp100, Daxx, and NDP55 were found in the centers of the spheres. Thus, ND10 proteins that normally are closely linked separate within HDAg-associated complexes. Viral RNA of antigenomic polarity, whether expressed from genomic RNA or directly from introduced plasmids, colocalizes with L-HDAg and the transcriptional repressor PML. In contrast, HDV genomic RNA was distributed more uniformly throughout the nucleus. These results suggest that different host protein complexes may assemble on viral RNA strands of different polarities, and they also suggest that this RNA virus, like DNA viruses, can alter the distribution of ND10-associated proteins. The fact that viral components specifically linked to repression of replication can associate with one of the ND10-associated proteins (PML) raises the possibility that this host protein may play a role in the regulation of HDV RNA synthesis.
机译:肝炎三角洲病毒(HDV)是一种单链RNA病毒,具有单个编码区,其产物肝炎三角洲抗原(HDAg)以两种同工型表达,即小(S-HDAg)和大(L-HDAg)。 S-HDAg是HDV复制所必需的,而L-HDAg则抑制病毒复制,并且是乙型肝炎病毒蛋白包裹HDV基因组RNA所必需的。在这里,我们检查了HDV RNA和蛋白质在受感染核中的空间分布,特别是针对特定的核域。我们发现L-HDAg聚集在特定的核域中,并且这些域的一半以上位于核域10(ND10)旁。后来,在较大的HDAg复合物中发现了与ND10相关的蛋白质,如PML,这些复合物已发展成明显的空心球。在这些较大的复合物中,PML主要存在于球体的边缘,而已知的ND10组分Sp100,Daxx和NDP55则存在于球体的中心。因此,通常紧密连接的ND10蛋白在与HDAg相关的复合物中分开。具有反基因组极性的病毒RNA,无论是从基因组RNA还是直接从导入的质粒表达,都与L-HDAg和转录阻遏物PML共定位。相反,HDV基因组RNA在整个细胞核中分布更均匀。这些结果表明,不同的宿主蛋白复合物可能在极性不同的病毒RNA链上组装,并且还表明,这种RNA病毒与DNA病毒一样,可以改变ND10相关蛋白的分布。特异性与复制抑制相关的病毒成分可以与ND10相关蛋白(PML)之一结合的事实,增加了这种宿主蛋白​​可能在调节HDV RNA合成中发挥作用的可能性。

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