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在逆转录病毒Gag多聚蛋白中鉴定出一种细胞质靶向/滞留信号。

Identification of a cytoplasmic targeting/retention signal in a retroviral Gag polyprotein.

作者信息

Choi G, Park S, Choi B, Hong S, Lee J, Hunter E, Rhee S S

机构信息

Laboratory of Molecular Virology, Samsung Biomedical Research Institute, Seoul, Korea.

出版信息

J Virol. 1999 Jul;73(7):5431-7. doi: 10.1128/JVI.73.7.5431-5437.1999.

Abstract

Retroviral capsid assembly can occur by either of two distinct morphogenic processes: in type C viruses, the capsid assembles and buds at the plasma membrane, while in type B and D viruses, the capsid assembles within the cytoplasm and is then transported to the plasma membrane for budding. We have previously reported that a single-amino-acid substitution of a tryptophan for an arginine in the matrix protein (MA) of Mason-Pfizer monkey virus (MPMV) converts its capsid assembly from that of a type D retrovirus to that of the type C viruses (S. S. Rhee and E. Hunter, Cell 63:77-86, 1990). Here we identify a region of 18 amino acids within the MA of MPMV that is responsible for type D-specific morphogenesis. Insertion of these 18 amino acids into the MA of type C Moloney murine leukemia virus causes it to assemble an immature capsid in the cytoplasm. Furthermore, fusion of the MPMV MA to the green fluorescent protein resulted in altered intracellular targeting and a punctate accumulation of the fusion protein in the cytoplasm. These 18 amino acids, which are necessary and sufficient to target retroviral Gag polyproteins to defined sites in the cytoplasm, appear to define a novel mammalian cytoplasmic targeting/retention signal.

摘要

逆转录病毒衣壳组装可通过两种不同的形态发生过程中的任何一种进行

在C型病毒中,衣壳在质膜上组装并出芽,而在B型和D型病毒中,衣壳在细胞质内组装,然后转运至质膜进行出芽。我们之前报道过,在梅森- Pfizer猴病毒(MPMV)的基质蛋白(MA)中,将一个精氨酸替换为色氨酸的单氨基酸取代会将其衣壳组装方式从D型逆转录病毒转变为C型病毒(S. S. Rhee和E. Hunter,《细胞》63:77 - 86,1990年)。在此,我们鉴定出MPMV的MA中一个由18个氨基酸组成的区域,该区域负责D型特异性形态发生。将这18个氨基酸插入C型莫洛尼鼠白血病病毒的MA中,会使其在细胞质中组装出一个未成熟的衣壳。此外,MPMV的MA与绿色荧光蛋白融合导致细胞内靶向改变,且融合蛋白在细胞质中呈点状积累。这18个氨基酸对于将逆转录病毒Gag多聚蛋白靶向到细胞质中的特定位点是必需且充分的,它们似乎定义了一种新的哺乳动物细胞质靶向/保留信号。

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