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首页> 外文期刊>Journal of cellular biochemistry. >Cell-cycle-dependent localization of human cytomegalovirus UL83 phosphoprotein in the nucleolus and modulation of viral gene expression in human embryo fibroblasts in vitro.
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Cell-cycle-dependent localization of human cytomegalovirus UL83 phosphoprotein in the nucleolus and modulation of viral gene expression in human embryo fibroblasts in vitro.

机译:人巨细胞病毒UL83磷蛋白在核仁中的细胞周期依赖性定位和体外人胚成纤维细胞中病毒基因表达的调节。

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摘要

The nucleolus is a multifunctional nuclear compartment widely known to be involved in several cellular processes, including mRNA maturation and shuttling to cytoplasmic sites, control of the cell cycle, cell proliferation, and apoptosis; thus, it is logical that many viruses, including herpesvirus, target the nucleolus in order to exploit at least one of the above-mentioned functions. Recent studies from our group demonstrated the early accumulation of the incoming ppUL83 (pp65), the major tegument protein of human cytomegalovirus (HCMV), in the nucleolus. The obtained results also suggested that a functional relationship might exist between the nucleolar localization of pp65, rRNA synthesis, and the development of the lytic program of viral gene expression. Here we present new data which support the hypothesis of a potentially relevant role of HCMV pp65 and its nucleolar localization for the control of the cell cycle by HCMV (arrest of cell proliferation in G1-G1/S), and for the promotion of viral infection. We demonstrated that, although the incoming pp65 amount in the infected cells appears to be constant irrespective of the cell-cycle phase, its nucleolar accumulation is prominent in G1 and G1/S, but very poor in S or G2/M. This correlates with the observation that only cells in G1 and G1/S support an efficient development of the HCMV lytic cycle. We propose that HCMV pp65 might be involved in regulatory/signaling pathways related to nucleolar functions, such as the cell-cycle control. Co-immunoprecipitation experiments have permitted to identify nucleolin as one of the nucleolar partners of pp65.
机译:核仁是一个多功能核区室,众所周知,它参与多个细胞过程,包括mRNA成熟和穿梭到细胞质部位,控制细胞周期,细胞增殖和凋亡。因此,合乎逻辑的是,包括疱疹病毒在内的许多病毒都以核仁为靶标,以便利用至少一种上述功能。我们小组的最新研究表明,传入核糖核酸ppUL83(pp65)是人巨细胞病毒(HCMV)的主要被膜蛋白的早期积累。所得结果还表明,在pp65的核仁定位,rRNA合成与病毒基因表达的裂解程序的发展之间可能存在功能关系。在这里,我们提供了新的数据,这些数据支持HCMV pp65及其核仁定位对于HCMV控制细胞周期(G1-G1 / S中细胞增殖的停止)以及促进病毒感染的潜在相关作用的假设。 。我们证明,尽管受感染细胞中pp65的传入量似乎是恒定的,而与细胞周期阶段无关,但其核仁积累在G1和G1 / S中很明显,但在S或G2 / M中非常差。这与只有G1和G1 / S中的细胞支持HCMV裂解周期的有效发展的观察结果相关。我们建议HCMV pp65可能参与与核仁功能(例如细胞周期控制)相关的调节/信号通路。共同免疫沉淀实验已允许将核仁蛋白鉴定为pp65的核仁伴侣之一。

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