Structure-Function Analyses of HIV Rev and HTLV Rex

HIV Rev 和 HTLV Rex 的结构功能分析

• 批准号: 6766820
• 负责人: Patrick Lee Green
• 金额: $ 4.03万
• 依托单位: OHIO STATE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2002
• 资助国家: 美国
• 起止时间: 2002-08-15 至 2005-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6766820
• 关键词: Italy; RNA splicing; cell transformation; conformation; cooperative study; deltaretrovirus; gene expression; human immunodeficiency virus; phosphorylation; protein kinase C; protein structure function; virus protein; virus replication

DESCRIPTION (provided by applicant): The present HIV-AIDS and Related Illnesses Research Collaboration (FIRCA) application proposes studies that will strengthen a newly developed collaboration between two highly productive research groups at The Ohio State University, USA (Dr. Patrick Green) and the University of Padova, Italy (Dr. Donna D'Agostino). Joint research projects between the participating laboratories emerged following the principal investigators' participation in the "10th International Conference on Human Retrovirology: HTLV and Related Viruses held in Dublin, Ireland, June 25-29, 2001. During the meeting, joint projects were discussed as outlined in the following proposal. Critical to the continuation of these productive exchanges are funds to allow the collaborations to mature for the benefit of the United States investigator and to enable expansion of the research capacity of the laboratory at the University of Padova, Italy. The proposed research will combine the resources that are established in each institution to be used for the collective benefit of both participants. HIV and HTLV are complex retroviruses whose expression is controlled by the viral regulatory proteins Tat and Rev (HIV) and Tax and Rex (HTLV). Together, our research laboratories have performed basic studies to define the role of regulatory proteins of each virus and are in a unique position to determine how these analogous regulatory proteins influence gene expression and replication of these complex retroviruses. Dr. Green's research group has shown that Tax is essential for cellular transformation and has identified a novel phosphorylation domain of Rex-2 that regulates its function. Dr. D'Agostino has shown that, through altemative splicing, HTLV-2 may produce truncated forms of Rex-2 termed x-III proteins that act as repressors of full-length Rex-2. More recently, her group demonstrated the functional importance of a loop region in Rev that influences several properties of the protein that are essential to its function. Specific aims that will be addressed in our proposed collaborative research are: 1) to explore the role of phosphorylation in the activity of the x-III proteins and examine their effect on HTLV-2 replication; and 2) to investigate the control of Rev's conformation and function by protein kinase C-mediated phosphorylation at serine residues and by isomerization of prolines in the loop region. The combined facilities and expertise brought together by the proposed AIDS-related FIRCA are unique, productive, and fulfill the mission of the Fogarty International Center to support collaborative research between the United States and foreign countries.

描述（由申请人提供）：目前的HIV-AIDS和相关疾病研究合作（FIRCA）申请提出的研究将加强美国俄亥俄州立大学（Patrick Green博士）和意大利帕多瓦大学（Donna D'Agostino博士）两个高效研究小组之间新开发的合作。主要研究人员参加了2001年6月25日至29日在爱尔兰都柏林举行的“第十届人类逆转录病毒学：HTLV和相关病毒国际会议”之后，参与实验室之间出现了联合研究项目。会议期间讨论了以下提议所概述的联合项目。要使这些富有成效的交流继续下去，至关重要的是为美国研究人员提供资金，使合作得以成熟，并使意大利帕多瓦大学实验室的研究能力得以扩大。拟议的研究将把在每个机构建立的资源结合起来，用于双方参与者的集体利益。HIV和HTLV是复杂的逆转录病毒，其表达受病毒调节蛋白Tat和Rev （HIV）和Tax和Rex （HTLV）的控制。我们的研究实验室一起进行了基础研究，以确定每种病毒的调节蛋白的作用，并处于一个独特的位置，以确定这些类似的调节蛋白如何影响这些复杂逆转录病毒的基因表达和复制。Green博士的研究小组已经证明，Tax对于细胞转化是必不可少的，并且已经确定了一个新的调节Rex-2功能的磷酸化结构域。D'Agostino博士已经证明，通过选择性剪接，HTLV-2可能产生被称为x-III蛋白的Rex-2的截断形式，作为全长Rex-2的抑制因子。最近，她的团队证明了Rev中一个环区在功能上的重要性，该环区影响了蛋白质的几个特性，这些特性对其功能至关重要。我们提出的合作研究将解决的具体目标是：1)探索磷酸化在x-III蛋白活性中的作用，并检查其对HTLV-2复制的影响；2)研究蛋白激酶c介导的丝氨酸残基磷酸化和环区脯氨酸异构化对Rev构象和功能的控制。拟议的与艾滋病有关的FIRCA汇集的综合设施和专业知识是独特的，富有成效的，并履行福格蒂国际中心的使命，支持美国与外国之间的合作研究。