Impact of early T-bet on CD8 T cell effector responses

早期 T-bet 对 CD8 T 细胞效应反应的影响

• 批准号: 9301463
• 负责人: CHRISTOPHER A HUNTER
• 金额: $ 40.25万
• 依托单位: UNIVERSITY OF PENNSYLVANIA
• 依托单位国家: 美国
• 财政年份: 2016
• 资助国家: 美国
• 起止时间: 2016-06-21 至 2021-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9301463
• 关键词: Affect; Alpha Cell; Antigens; Biological; CCL3 gene; CD8-Positive T-Lymphocytes; Cell Adhesion Molecules; Cell Communication; Cell Cycle; Cells; Cellular Immunity; Cellular Immunology; Chemotactic Factors; Data; Development; Disease; Effector Cell; Event; GATA3 gene; Generations; Genetic Transcription; Grant; Hand; Immune; Immune system; Immunology; In Vitro; Infection; Inflammatory; Interferons; Interleukin-12; Knowledge; Laboratories; Lead; Link; Mediating; Memory; Modeling; Mus; Parasites; Pathway interactions; Phase; Phenotype; Physiological; Population; Predisposition; Process; Production; Proliferating; Publishing; Reporter; Research Personnel; Resistance; Resistance to infection; Role; Signal Transduction; Site; System; T cell response; T-Cell Activation; T-Cell Development; T-Lymphocyte; Testing; Toxoplasma; Toxoplasma gondii; Transcriptional Regulation; Transgenic Organisms; Up-Regulation; Vaccines; Work; cell behavior; cellular imaging; comparative; cytokine; experimental study; imaging approach; imaging study; in vivo; interest; intravital imaging; long term memory; novel; pathogen; polarized cell; promoter; response; tool; transcriptome sequencing

Project Summary Understanding the transcriptional regulation of polarized T cell responses and their link to inflammatory conditions and resistance to infection has been a major theme in immunology for the last 20 years and has led to the identification of T-bet, GATA3 and RoRt as “master regulators” of the development of Th1, Th2 and Th17 type responses, respectively. As such, the ability of T-bet to promote IFN- production has dominated our appreciation of how T-bet contributes to T cell responses in the setting of infection. This is reinforced by the increased susceptibility of T-bet-/- mice to various intracellular infections, including the opportunistic parasite Toxoplasma gondii. In CD4+ and CD8+ T cells there is good evidence that T cell activation is accompanied by two waves of T-bet expression (the T-bet two step) and that the initial TCR- mediated induction of T-bet sensitizes T cells for polarizing signals provided by cytokines such as IL-12 that reinforce further T-bet expression and commitment to differentiation. However, our recent published and preliminary studies indicate that in CD8+ T cells T-bet may have an unanticipated role in controlling a myriad of early T cell activation induced events including upregulation of adhesion molecules and chemoattractants and entry of CD8+ T cells into cell cycle. These results have led to the novel hypothesis that the early induction of T-bet optimizes the interactions between recently activated T and DC populations to promote entry into the cell cycle, optimize expansion and the acquisition of effector functions. To test this hypothesis we will combine transcriptional profiling to identify early targets of T-bet with state of the art cellular immunology and imaging approaches to understand the role of T-bet and in hand candidates in the initial events that are essential for the generation of effector responses required for resistance to an intracellular pathogen.

项目摘要 了解极化T细胞反应的转录调控及其与炎症的联系 在过去的20年里，条件和对感染的抵抗力一直是免疫学的一个主要主题， 导致T-bet、GATA 3和RoR β t被鉴定为Th 1、Th 2和Th 3的发展的“主调节因子”。 和Th 17型应答。因此，T-bet促进IFN-γ产生的能力已经被证实。 主导了我们对T-bet如何在感染环境中促进T细胞应答的理解。这是 T-bet-/-小鼠对各种细胞内感染的易感性增加，包括 机会寄生虫弓形虫。在CD 4+和CD 8 + T细胞中，有很好的证据表明T细胞 活化伴随着T-bet表达的两个波（T-bet两步），并且初始TCR-γ表达的两个波（T-bet两步）是T-bet表达的两个波（T-bet两步）。 T-bet介导的诱导使T细胞对由细胞因子如IL-12提供的极化信号敏感 这进一步增强了T-bet表达和分化的承诺。然而，我们最近出版的 初步研究表明，在CD 8 + T细胞中，T-bet可能在控制免疫应答中发挥意想不到的作用。 大量早期T细胞活化诱导的事件，包括粘附分子的上调， 化学引诱物和CD 8 + T细胞进入细胞周期。这些结果导致了一个新的假设 T-bet的早期诱导优化了最近激活的T和DC群体之间的相互作用， 以促进进入细胞周期、优化扩增和获得效应子功能。 为了验证这一假设，我们将结合联合收割机转录谱来鉴定T-bet的早期靶点， 本领域的细胞免疫学和成像方法来理解T-bet的作用， 初始事件中的候选者对于产生所需的效应器响应是必要的， 对细胞内病原体的抵抗力。