PAC1 in Signaling Apoptosis and Tumor Suppression

PAC1 在信号凋亡和肿瘤抑制中的作用

• 批准号: 7237286
• 负责人: YUXIN YIN
• 金额: $ 31.48万
• 依托单位: COLUMBIA UNIVERSITY HEALTH SCIENCES
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-08-01 至 2009-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7237286
• 关键词: Acetylation; Achievement; Address; Animal Model; Apoptosis; Apoptotic; Applications Grants; Binding; Cell Cycle Arrest; Cell Cycle Regulation; Cell Death; Cell Survival; Complement component C1s; Condition; DNA Repair; Development; E2F1 gene; Gene Targeting; Genes; Genetic Transcription; Genotoxic Stress; Goals; Grant; Homologous Gene; Human; Lead; Luciferases; MAP Kinase Gene; Malignant Neoplasms; Mammalian Cell; Mediating; Mediator of activation protein; Mitogen-Activated Protein Kinases; Modification; Molecular; Mutation; Normal Cell; Numbers; Oxidative Stress; P1 Bacteriophage Artificial Chromosomes; Pathway interactions; Phosphoric Monoester Hydrolases; Phosphorylation; Play; Post-Translational Protein Processing; Predisposition; Principal Investigator; Protein Dephosphorylation; Protein Overexpression; Protein Tyrosine Phosphatase; Regulation; Reporter; Reporting; Role; Series; Signal Transduction; Signal Transduction Pathway; Stress; Substrate Specificity; System; TP53 gene; Testing; Threonine; Time; Transcription Coactivator; Transcriptional Regulation; Tumor Suppression; Tumor Suppressor Proteins; Tumorigenicity; Yin; base; cancer therapy; cell growth; cell injury; cell suicide; cisplatin/cyclophosphamide/doxorubicin protocol; gene therapy; inhibitor/antagonist; irradiation; mitogen-activated protein kinase phosphatase MKP6; paralogous gene; programs; promoter; response; transcription factor; tumor; tumorigenesis

DESCRIPTION (provided by applicant): Transcription factors p53 and E2F-1 coordinate and mediate apoptosis in response to genotoxic stress. However, the mechanism whereby p53 and E2F-1 mediate apoptosis is unclear. We have recently reported that p53 is a direct transcriptional regulator of PAC1, a dual-specific threonine and tyrosine phosphatase with stringent substrate specificity for MAP kinase. We also found that E2F-1 regulates PAC1 at the transcriptional level. PAC1 has been shown as a potent inhibitor of MAP kinase activity through dephosphorylation of MAPK, In our p53 inducible system, PAC1 is greatly upregulated upon activation of p53 that leads to apoptosis. The expression of PAC1 in normal cells is significant increased following oxidative stress in a p53-dependent manner. We show that p53 binds to a palindromic motif in the PAC1 promoter and activates the PAC1 promoter, leading to the expression of PAC1. Importantly, PAC1 is induced only under the stress conditions that cause apoptosis but not the conditions that lead to cell cycle arrest, suggesting that p53 may be modified following apoptotic stresses. E2F-1 also stimulates the activity of the PAC1 promoter luciferase reporter. We further demonstrate that overexpression of E2F-1 elevates the levels of PAC1 transcription and that E2F-1 is required for full induction of PAC1 in response to oxidative stress. Finally, overexpression of PAC1 greatly increases cellular susceptibility to apoptosis. Our findings indicate that p53 and E2F-1 are transcriptional regulators of PAC1 and that PAC1 is a cell death mediator in the p53 and E2F-1 pathways. This is the first evidence that p53 and E2F-1 share a common target gene in signaling apoptosis. In this grant application, we propose a series of experimental approaches to demonstrate how p53 modifications influence its choice of binding to the palindromic motif and of selectively regulating PAC1. We will determine how PAC1 is regulated by E2F1. We will also determine whether and how p73, a p53 paralog tumor suppressor, regulates PAC1 and we will demonstrate the importance of PAC1 in tumorigenesis. Successful achievement of our specific aims will provide strong evidence for how p53, p73 and E2F-1 cooperatively regulate a dual-specific phosphatase that in turn inactivates MAP kinase, a signal transduction pathway for cell growth and proliferation. This grant may reveal a new target for gene therapy or lead to effective chemotherapeutical strategies in cancer treatment.

描述(由申请人提供)：转录因子P53和E2F-1协调和介导细胞凋亡，以应对遗传毒性压力。然而，P53和E2F-1介导细胞凋亡的机制尚不清楚。我们最近报道，P53是PAC1的直接转录调节因子，PAC1是一种苏氨酸和酪氨酸磷酸酶，具有严格的底物特异性。我们还发现，E2F-1在转录水平上调节PAC1。PAC1是一种通过去磷酸化MAPK抑制MAPK活性的有效抑制剂，在我们的P53诱导系统中，PAC1在P53激活后显著上调，从而导致细胞凋亡。氧化应激后，PAC1在正常细胞中的表达显著增加，且依赖于P53。我们发现P53与PAC1启动子中的回文基序结合并激活PAC1启动子，导致PAC1的表达。重要的是，PAC1只在导致细胞凋亡的应激条件下被诱导，而不是在导致细胞周期停滞的条件下被诱导，这表明在凋亡应激之后P53可能被修饰。E2F-1还能刺激PAC1启动子荧光素酶报告基因的活性。我们进一步证明，E2F-1的过表达提高了PAC1的转录水平，并且E2F-1是完全诱导PAC1响应氧化应激所必需的。最后，PAC1的过度表达极大地增加了细胞对凋亡的敏感性。我们的研究结果表明，P53和E2F-1是PAC1的转录调节因子，而PAC1是P53和E2F-1通路中的细胞死亡介质。这是首次有证据表明P53和E2F-1在信号转导细胞凋亡方面具有共同的靶基因。在这项拨款申请中，我们提出了一系列实验方法来展示p53修饰如何影响其与回文基序的结合和选择性调节PAC1的选择。我们将确定E2F1如何调控PAC1。我们还将确定P73是否以及如何调节PAC1，我们将证明PAC1在肿瘤发生中的重要性。我们的特定目标的成功实现将为p53、p73和E2F-1如何协同调节双特异性磷酸酶提供强有力的证据，该双特异性磷酸酶反过来抑制细胞生长和增殖的信号转导途径MAPK。这笔赠款可能会揭示基因治疗的新靶点，或者导致癌症治疗中有效的化疗策略。