IFNARI SIGNALING THROUGH STAT3, PI 3 KINASE

通过 STAT3、PI 3 激酶的 IFNARI 信号传导

• 批准号: 2837730
• 负责人: LAWRENCE MARC PFEFFER
• 金额: $ 28.29万
• 依托单位: UNIVERSITY OF TENNESSEE HEALTH SCI CTR
• 依托单位国家: 美国
• 财政年份: 1997
• 资助国家: 美国
• 起止时间: 1997-12-02 至 2002-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/2837730
• 关键词: DNA binding protein; SDS polyacrylamide gel electrophoresis; antiviral agents; apoptosis; biological response modifiers; biological signal transduction; cell growth regulation; densitometry; gene expression; immunoprecipitation; interferon alpha; northern blottings; nuclear factor kappa beta; nuclear runoff assay; phosphatidylinositol 3 kinase; phosphorylation; protein kinase C; protein structure function; receptor binding; receptor coupling; tissue /cell culture; transcription factor; western blottings

Interferon-alpha (IFNalpha) is a multifunctional cytokine, which is clinically effective in the treatment of human malignancies, viral infections and auto-immune diseases. IFNalpha elicits pleiotropic biological effects by regulating gene expression through signals generated upon its binding to a surface receptor on target cells (IFNalphaR). The first cloned subunit of the IFNalphaR, IFNAR1, plays a decisive role as a IFN signal transducing subunit but does not directly bind IFNalpha. The IFNalpha-induced tyrosine phosphorylation of STAT transcription factors is crucial in activated protein kinase (ERK2) also contribute to IFNalpha action. Based on the applicant's recent studies, the hypothesis to be tested is that via the IFNalpha-induced binding of STAT3 to the IFNalphaR, STAT3 (a transcription factor regulation the acute phase response genes), couples IFNalphaR signaling to pathways involving PI-3 kinase (phosphatidylinositol-3' kinase, an upstream element in a serine kinase transduction cascade), NF-kappaB (nuclear factor-kappaB, a transcription factor for genes important in inflammation and preventing apoptosis), and serine kinases (PKC subspecies and ERK2). In Specific Aim 1, how STAT3 acts as an adapter to couple IFNalpha signaling pathways will be characterized. To be determined is if STAT3 activation (specifically via the docking domain in STAT3 for the p85 subunit of PI-3 kinase) is required for IFNalpha-induced: PI-3 kinase activation, PKC activation, ERK2 activation, gene expression, anti-viral action, and the anti- proliferative action. In Specific Aim 2, the role of PI-3 kinase arm of the STAT3-signaling pathway in IFNalpha action will be defined. The effect of expressing dominant negative and constitutively active PI-3 kinase constructs will be examined on IFNalpha-induced: serine phosphorylation of cellular substrates, PKC activation, ERK2 activation, DNA-binding activity, gene expression, anti-viral action, anti-proliferative action, and inhibition of programmed cell death. In specific Aim 3, the role of the NF-kappaB component of the STAT3-signaling pathway in IFNalpha action will be defined. To be determine are the mechanism for NF-kappaB activation, the interaction of STAT3 with NF-kappaB proteins, and the role of NF-kappaB activation on IFNalpha-induced: gene expression, anti-viral activity, anti-proliferative activity, inhibition of programmed cell death. The overall goal of these studies to determine how the activation of STAT3, PI-3 kinase and NF-kappaB are linked, and to determine their roles in effecting IFN's biological actions.

干扰素- α (ifn - α)是一种多功能细胞因子