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通过细胞可渗透的HBx蛋白从调节蛋白缺陷型乙型肝炎病毒基因组中重建基因表达。

Reconstitution of gene expression from a regulatory-protein-deficient hepatitis B virus genome by cell-permeable HBx protein.

作者信息

Hafner Angela, Brandenburg Boerries, Hildt Eberhard

机构信息

Robert Koch-Institut, Nordufer 20, D-13353 Berlin, Germany.

出版信息

EMBO Rep. 2003 Aug;4(8):767-73. doi: 10.1038/sj.embor.embor903. Epub 2003 Jul 18.

Abstract

Various functions are ascribed to the HBx regulatory protein of the hepatitis B virus (HBV). Due to the low expression level of HBx, it has been difficult to correlate spatial and temporal HBx expression levels with specific functions. Based on a novel cell-permeable peptide, known as the translocation motif (TLM), cell-permeable HBx fusion proteins were generated. The TLM-HBx fusion protein is rapidly internalized from the medium into almost all cells, whereas no significant internalization was seen with wild-type HBx. The major fraction of internalized HBx protein moves from the cytoplasm to the nucleus. The cytosolic fraction, however, activates c-RAF1/extracellular-signal-related kinase 2 signalling and causes activation of activator protein 1 (AP1) and nuclear factor-kappaB. The TLM-HBx protein rescues HBV gene expression from an activator-deficient HBV genome. These results indicate that cell-permeable regulatory proteins provide a novel, efficient tool for a clearly defined, dose-dependent analysis of regulatory protein function, without affecting the integrity of the cell, and can be used for the safe reconstitution of virus production from a regulatory-protein-deficient virus genome.

摘要

乙型肝炎病毒(HBV)的HBx调节蛋白具有多种功能。由于HBx的表达水平较低,很难将其时空表达水平与特定功能联系起来。基于一种新型的细胞穿透肽,即转位基序(TLM),制备了细胞穿透性HBx融合蛋白。TLM-HBx融合蛋白能迅速从培养基内化到几乎所有细胞中,而野生型HBx则未见明显内化。内化的HBx蛋白大部分从细胞质转移到细胞核。然而,胞质部分可激活c-RAF1/细胞外信号相关激酶2信号通路,并导致激活蛋白1(AP1)和核因子κB的活化。TLM-HBx蛋白可从激活因子缺陷的HBV基因组中拯救HBV基因表达。这些结果表明,细胞穿透性调节蛋白为明确、剂量依赖性分析调节蛋白功能提供了一种新型、高效的工具,且不影响细胞的完整性,可用于从调节蛋白缺陷的病毒基因组中安全重建病毒生产。

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