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人巨细胞病毒蛋白PP65和IEP72定位于受感染的人胚胎成纤维细胞核及核基质中的不同区室。

Human cytomegalovirus proteins PP65 and IEP72 are targeted to distinct compartments in nuclei and nuclear matrices of infected human embryo fibroblasts.

作者信息

Arcangeletti M C, De Conto F, Ferraglia F, Pinardi F, Gatti R, Orlandini G, Calderaro A, Motta F, Medici M C, Martinelli M, Valcavi P, Razin S V, Chezzi C, Dettori G

机构信息

Microbiology Section, Department of Pathology and Laboratory Medicine, University of Parma, Parma, Italy.

出版信息

J Cell Biochem. 2003 Dec 1;90(5):1056-67. doi: 10.1002/jcb.10655.

Abstract

The cellular distribution of the human cytomegalovirus (HCMV)-specific UL83 phosphoprotein (pp65) and UL123 immediate-early protein (IEp72) in lytically infected human embryo fibroblasts was studied by means of indirect immunofluorescence and confocal microscopy. Both proteins were found to have a nuclear localization, but they were concentrated in different compartments within the nuclei. The pp65 was located predominantly in the nucleoli; this was already evident with the parental viral protein, which was targeted to the above nuclear compartment very soon after infection. The nucleolar localization of pp65 was also observed at later stages of the HCMV infectious cycle. After chromatin extraction (in the so-called in situ nuclear matrices), a significant portion of the pp65 remained associated with nucleoli within the first hour after infection, then gradually redistributed in a perinucleolar area, as well as throughout the nucleus, with a granular pattern. A quite different distribution was observed for IEp72 at very early stages after infection of human embryo fibroblasts with HCMV; indeed, this viral protein was found in bright foci, clearly observable in both non-extracted nuclei and in nuclear matrices. At later stages of infection, IEp72 became almost homogeneously distributed within the whole nucleus, while the foci increased in size and were more evenly spread; in several infected cells some of them lay within nucleoli. This peculiar nuclear distribution of IEp72 was preserved in nuclear matrices as well. The entire set of data is discussed in terms of the necessity of integration for HCMV-specific products into the pre-existing nuclear architecture, with the possibility of subsequent adaptation of nuclear compartments to fit the needs of the HCMV replicative cycle.

摘要

通过间接免疫荧光和共聚焦显微镜研究了人巨细胞病毒(HCMV)特异性UL83磷蛋白(pp65)和UL123立即早期蛋白(IEp72)在人胚成纤维细胞裂解感染中的细胞分布。发现这两种蛋白都有核定位,但它们集中在细胞核内的不同区域。pp65主要位于核仁中;这在亲本病毒蛋白中已经很明显,感染后很快就靶向到上述核区域。在HCMV感染周期的后期也观察到pp65的核仁定位。在染色质提取后(在所谓的原位核基质中),感染后第一小时内,相当一部分pp65仍与核仁相关,然后逐渐重新分布到核仁周围区域以及整个细胞核中,呈颗粒状分布。在人胚成纤维细胞感染HCMV后的早期阶段,观察到IEp72的分布完全不同;实际上,这种病毒蛋白在明亮的焦点中被发现,在未提取的细胞核和核基质中都清晰可见。在感染后期,IEp72几乎均匀地分布在整个细胞核内,而焦点增大且分布更均匀;在一些感染细胞中,其中一些位于核仁内。IEp72这种特殊的核分布在核基质中也得以保留。根据将HCMV特异性产物整合到预先存在的核结构中的必要性,以及随后核区域可能进行调整以适应HCMV复制周期需求的可能性,对这组完整数据进行了讨论。

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