HIV-1 Vpr Induces G2 Cell Cycle Arrest and Apoptosis

HIV-1 Vpr 诱导 G2 细胞周期停滞和凋亡

• 批准号: 6919233
• 负责人: IRVIN S.Y. CHEN
• 金额: $ 32.68万
• 依托单位: UNIVERSITY OF CALIFORNIA LOS ANGELES
• 依托单位国家: 美国
• 财政年份: 1995
• 资助国家: 美国
• 起止时间: 1995-07-18 至 2008-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6919233
• 关键词: HIV infections; apoptosis; cell cycle; cell cycle proteins; clinical research; dendritic cells; helper T lymphocyte; host organism interaction; human immunodeficiency virus 1; human tissue; macrophage; microarray technology; polymerase chain reaction; protein kinase; protein localization; protein structure function; tissue /cell culture; virus DNA; virus RNA; virus infection mechanism; virus protein

DESCRIPTION (provided by applicant): This proposal constitutes a renewal application to study the role of the HIV-1 Vpr gene product. The overall goal of the studies proposed here is to understand the interaction between the various functions of Vpr and how they contribute to the pathogenesis of HIV-1. The hypothesis to be addressed here is that Vpr plays a critical role for HIV-1 replication and pathogenesis. The HIV-1 Vpr gene product is a 96 amino acid protein, which is important for viral replication and likely to be critical for HIV-1 pathogenesis. Vpr is expressed following infection of cells and is also found packaged in virions. In 1995, at the beginning of the initial funding period of this grant, we were among the first to describe a novel phenotype of the Vpr protein whereby cells infected by HIV-1 expressing Vpr undergo arrest at the G2 phase of the cell cycle. We focused our efforts on further characterizing this unique function of the Vpr protein. We have shown that cell cycle arrest is a highly evolutionarily conserved property of Vpr. In addition, we found that cell cycle arrest induced by Vpr is followed by apoptosis of the arrested cells. Other investigators have reported that Vpr enhances virus production and is involved in cytokine regulation. During the past funding period we made the important observation that Vpr that is packaged into virions is capable of inducing both cell cycle arrest and apoptosis independent of subsequent events in the viral lifecycle. Recently, we made the observation that virion Vpr is critical for expression from unintegrated viral DNA. Thus, in combination these results indicate that Vpr plays an important role in HIV-1 pathogenesis through the immediate early upregulation of viral gene expression and longer term effects upon T-cell metabolism. During the previous funding periods we have generated a considerable amount of preliminary data about Vpr action, developed a number of unique assays for assessment of Vpr function, and developed reagents which will allow us to effectively carry forward further studies on the mechanism of Vpr action. The specific aims are: Aim 1) To further characterize cell cycle arrest and apoptosis mediated by Vpr. Aim 2) To characterize the newly described process of Vpr mediated transactivation of unintegrated HIV-1 DNA. Aim 3) To further characterize the role of Vpr in viral pathogenesis.

描述（由申请人提供）：本提案构成了研究HIV-1 Vpr基因产物作用的再申请。本文提出的研究的总体目标是了解Vpr的各种功能之间的相互作用以及它们如何有助于HIV-1的发病机制。这里要解决的假设是Vpr在HIV-1复制和发病机制中起着关键作用。HIV-1 Vpr基因产物是一种96个氨基酸的蛋白质，它对病毒复制很重要，可能对HIV-1的发病机制至关重要。Vpr在细胞感染后表达，也被发现包装在病毒体中。在1995年，在该基金的初始资助期开始时，我们是第一批描述Vpr蛋白的新表型的人之一，即被表达Vpr的HIV-1感染的细胞在细胞周期的G2期被阻滞。我们集中精力进一步表征Vpr蛋白的这种独特功能。我们已经表明，细胞周期阻滞是Vpr的一个高度进化保守的属性。此外，我们发现，Vpr诱导的细胞周期阻滞后，被阻滞的细胞凋亡。其他研究者已经报道Vpr增强病毒产生并参与细胞因子调节。在过去的资助期间，我们进行了重要的观察，即包装到病毒体中的Vpr能够诱导细胞周期停滞和凋亡，而不依赖于病毒生命周期中的后续事件。最近，我们观察到病毒粒子Vpr对于从未整合的病毒DNA表达是至关重要的。因此，结合这些结果表明，Vpr通过病毒基因表达的立即早期上调和对T细胞代谢的长期影响在HIV-1发病机制中起重要作用。 在以前的资助期间，我们已经产生了相当数量的关于Vpr作用的初步数据，开发了一些独特的检测方法来评估Vpr功能，并开发了试剂，这将使我们能够有效地进行进一步的研究Vpr的作用机制。具体目的是：目的1）进一步表征Vpr介导的细胞周期阻滞和凋亡。目的2）研究Vpr介导的HIV-1DNA反式激活过程。目的3）进一步研究Vpr在病毒致病中的作用。