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乙型肝炎病毒X蛋白(HBx)的细胞内定位

Intracellular localization of the hepatitis B virus HBx protein.

作者信息

Henkler Frank, Hoare Jonathan, Waseem Naushin, Goldin Robert D, McGarvey Michael J, Koshy Rajen, King Ian A

机构信息

National Institute for Medical Research, Division of Membrane Biology, The Ridgeway, Mill Hill, London NW7 1AA, UK1.

Department of Medicine2 and Department of Histopathology5, Imperial College School of Medicine, St Mary's Campus, South Wharf Road, London W2 INY, UK.

出版信息

J Gen Virol. 2001 Apr;82(Pt 4):871-882. doi: 10.1099/0022-1317-82-4-871.

Abstract

The hepatitis B virus (HBV) X protein (HBx) was originally suggested to be a viral transcriptional activator, but its functional mechanisms are still unclear. In this study we have analysed the intracellular localization of HBx in transfected cells and demonstrate that its compartmentalization is dependent on overall expression levels. HBx was exclusively or predominantly localized in the nuclei in weakly expressing cells. However, elevated cellular levels correlated with its accumulation in the cytoplasm, suggesting that the capacity of HBx for nuclear compartmentalization might be limited. Cytoplasmic HBx was detected either as punctate granular staining or in dispersed, finely granular patterns. We have further analysed the detailed cytoplasmic compartmentalization, using confocal microscopy, and show no association with the endoplasmic reticulum, plasma membrane or lysosomes, but a substantial association of HBx with mitochondria. However, a major fraction of cytoplasmic HBx did not localize in mitochondria, indicating the presence of two distinctly compartmentalized cytoplasmic populations. Furthermore, high levels of HBx expression led to an abnormal mitochondrial distribution, involving clumping and organelle aggregation, which was not observed at lower expression levels. The data presented here provide novel insights into the compartmentalization of HBx and may prove important for future evaluations of its functions, both in the viral life-cycle and in the pathology of HBV-related liver disease.

摘要

乙肝病毒(HBV)X蛋白(HBx)最初被认为是一种病毒转录激活因子,但其功能机制仍不清楚。在本研究中,我们分析了转染细胞中HBx的细胞内定位,并证明其区室化依赖于整体表达水平。在低表达细胞中,HBx仅或主要定位于细胞核。然而,细胞水平升高与其在细胞质中的积累相关,这表明HBx进行核区室化的能力可能有限。细胞质中的HBx检测为点状颗粒染色或分散的细颗粒模式。我们使用共聚焦显微镜进一步分析了详细的细胞质区室化,结果显示其与内质网、质膜或溶酶体无关联,但HBx与线粒体有大量关联。然而,大部分细胞质HBx并不定位于线粒体,这表明存在两种明显区室化的细胞质群体。此外,高水平的HBx表达导致线粒体分布异常,包括聚集和细胞器聚集,而在较低表达水平时未观察到这种情况。本文提供的数据为HBx的区室化提供了新的见解,可能对未来评估其在病毒生命周期和HBV相关肝病病理学中的功能具有重要意义。

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