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一种蛋白质隔离系统揭示了转录共激活因子HCF-1对细胞程序的调控。

A protein sequestering system reveals control of cellular programs by the transcriptional coactivator HCF-1.

作者信息

Khurana Bharat, Kristie Thomas M

机构信息

Laboratory of Viral Diseases, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Biol Chem. 2004 Aug 6;279(32):33673-83. doi: 10.1074/jbc.M401255200. Epub 2004 Jun 8.

Abstract

The mammalian transcriptional coactivator HCF-1 is a critical component of the multiprotein herpes simplex virus immediate early gene enhancer core complex. The protein has also been implicated in basic cellular processes such as cell-cycle progression, transcriptional coactivation, and mRNA processing. Functions have been attributed to HCF-1 primarily from analyses of protein-protein interactions and from the cell-cycle-arrested phenotype of an HCF-1 temperature-sensitive mutant. However, neither the mechanisms involved nor specific cellular transcriptional targets have been identified. As the protein is essential for cell viability and proliferation, a genetic system was developed to specifically sequester the nuclear factor in the cell cytoplasm in a regulated manner. This approach exhibits no significant cell toxicity yet clearly demonstrates the requirement of available nuclear HCF-1 for herpes simplex virus immediate early gene expression during productive infection. Additionally, cellular transcriptional events were identified that contribute to understanding the functions ascribed to the protein and implicate the protein in events that impact the regulation of critical cellular processes.

摘要

哺乳动物转录共激活因子HCF-1是多蛋白单纯疱疹病毒立即早期基因增强子核心复合物的关键组成部分。该蛋白还参与细胞周期进程、转录共激活和mRNA加工等基本细胞过程。HCF-1的功能主要来自对蛋白质-蛋白质相互作用的分析以及对HCF-1温度敏感突变体的细胞周期停滞表型的研究。然而,所涉及的机制和特定的细胞转录靶点均未确定。由于该蛋白对细胞活力和增殖至关重要,因此开发了一种遗传系统,以受调控的方式将核因子特异性隔离在细胞质中。这种方法没有明显的细胞毒性,但清楚地证明了在生产性感染期间,可用的核HCF-1对单纯疱疹病毒立即早期基因表达的必要性。此外,还确定了细胞转录事件,这有助于理解赋予该蛋白的功能,并表明该蛋白参与了影响关键细胞过程调控的事件。

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