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尽管Tat和Rev高效表达,但星形胶质细胞中1型人类免疫缺陷病毒产量减少是由于gag、env和nef mRNA翻译效率低下所致。

Diminished production of human immunodeficiency virus type 1 in astrocytes results from inefficient translation of gag, env, and nef mRNAs despite efficient expression of Tat and Rev.

作者信息

Gorry P R, Howard J L, Churchill M J, Anderson J L, Cunningham A, Adrian D, McPhee D A, Purcell D F

机构信息

AIDS Cellular, Victoria, Australia.

出版信息

J Virol. 1999 Jan;73(1):352-61. doi: 10.1128/JVI.73.1.352-361.1999.

Abstract

Astrocytes infected with human immunodeficiency virus type 1 (HIV-1) produce only minimal quantities of virus. The molecular events that limit acute-phase HIV-1 infection of astrocytes were examined after inducing acute-phase replication by transfection with the pNL4-3 proviral plasmid. The levels of HIV-1 mRNA were similarly high in both astrocytes and HeLa cells, but astrocytes produced approximately 50-fold less supernatant p24 than HeLa cells. We found that diminished HIV-1 production in astrocytes resulted from inefficient translation of gag, env, and nef mRNAs that were efficiently transported to the cytoplasm. Tat- or Rev-dependent reporter constructs showed no defect in Tat or Rev function in astrocytes compared with HeLa cells. HIV-1 mRNAs were correctly spliced, but only Rev and Tat proteins were efficiently translated from their native mRNAs. Pulse-chase labelling and immunoblot experiments revealed no defect in protein processing, but levels of Gag, Env, or Nef protein expressed were dramatically reduced in astrocytes compared to HeLa cells. These results demonstrate that inefficient translation of HIV-1 structural proteins underlies the restricted infection of astrocytes. The efficient expression of functional Tat and Rev by astrocytes may contribute to HIV-1 neuropathogenesis.

摘要

感染1型人类免疫缺陷病毒(HIV-1)的星形胶质细胞仅产生极少量病毒。在用pNL4-3前病毒质粒转染诱导急性期复制后,研究了限制星形胶质细胞急性期HIV-1感染的分子事件。星形胶质细胞和HeLa细胞中HIV-1 mRNA的水平同样很高,但星形胶质细胞产生的上清液p24比HeLa细胞少约50倍。我们发现,星形胶质细胞中HIV-1产生减少是由于gag、env和nef mRNA向细胞质的有效转运效率低下导致的翻译效率低下所致。与HeLa细胞相比,Tat或Rev依赖性报告基因构建体在星形胶质细胞中的Tat或Rev功能未显示出缺陷。HIV-1 mRNA被正确剪接,但只有Rev和Tat蛋白能从其天然mRNA中有效翻译。脉冲追踪标记和免疫印迹实验表明蛋白质加工没有缺陷,但与HeLa细胞相比,星形胶质细胞中表达的Gag、Env或Nef蛋白水平显著降低。这些结果表明,HIV-1结构蛋白的翻译效率低下是星形胶质细胞感染受限的基础。星形胶质细胞对功能性Tat和Rev的有效表达可能有助于HIV-1神经病理发生。

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