Regulation of Cell Survival and Tumor Progression by Akt

Akt 对细胞存活和肿瘤进展的调节

• 批准号: 6964934
• 负责人: Vivek M Rangnekar
• 金额: $ 26.01万
• 依托单位: UNIVERSITY OF KENTUCKY
• 依托单位国家: 美国
• 财政年份: 2005
• 资助国家: 美国
• 起止时间: 2005-08-01 至 2010-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6964934
• 关键词: SDS polyacrylamide gel electrophoresis; apoptosis; athymic mouse; biological signal transduction; cell growth regulation; cell line; immunoprecipitation; molecular oncology; neoplastic growth; phosphorylation; polymerase chain reaction; prostate neoplasms; protein isoforms; protein protein interaction; protein structure function; serine threonine protein kinase; tumor suppressor proteins

DESCRIPTION (provided by applicant): Akt is the focal point of a number of signaling pathways that regulate cell survival and tumor progression. Akt interacts with, and modifies via phosphorylation, many substrates involved in these cellular events. Owing to its anti-apoptotic properties, Akt plays a key role in promoting human cancer. Thus, the identification of molecules that interact with Akt may lead to a better understanding of the role of Akt in various local signaling networks and enable the development of strategies for specifically blocking signaling pathways involved in cancer development and progression. Par-4 is a leucine zipper domain protein that, when ectopically expressed, induces apoptosis in cancer cells but not in normal or immortalized cells. Apoptosis by ectopic Par-4 occurs by inhibition of NF-kappaB activity. As cancer cells contain reasonable levels of endogenous Par-4, we sought to determine whether Par-4 exists in an inactive form. Our Preliminary Studies reveal that Akt1 binds and inactivates endogenous Par-4, rendering it ineffective in apoptosis-induction. Moreover, inactivation of Akt1 releases Par-4 to induce apoptosis, implying that endogenous Par-4 is functionally active in the absence of Akt1. In view of the pro-survival functions of Akt1 and the pro-apoptotic functions of Par-4, the objective of this proposal is to study the molecular basis and functional relevance of the interaction between Akt1 and Par-4 in prostate cancer cell survival and tumor progression. Toward this end, we propose the following specific aims: Aim 1, elucidate the molecular basis for the isoform-specific effects of Akt on Par-4; Aim 2, determine the mechanism for cytoplasmic retention and inactivation of Par-4 by Akt1; and Aim 3, determine the downstream effects and functional relevance of Par-4 inhibition by Akt1 in tumor growth. Because PTEN loss is a well defined genetic lesion that elevates Akt activity and neutralizes the apoptotic pathway in the prostate, and contributes to prostate tumors in mouse models, this study will focus on the prostate cancer cell background to study the Akt1-Par-4 interaction. However, as the Akt1-Par-4 interaction occurs in diverse tumor cell types, we anticipate that the findings of this study will have broad implications in cancer. The findings will be further developed in future studies to design therapeutic strategies that can prevent Par-4 binding to Akt1 and induce apoptosis and tumor growth regression.

描述（由申请人提供）：Akt是调节细胞存活和肿瘤进展的许多信号通路的焦点。Akt与参与这些细胞事件的许多底物相互作用，并通过磷酸化修饰。由于其抗凋亡特性，Akt在促进人类癌症中起着关键作用。因此，与Akt相互作用的分子的鉴定可能导致更好地理解Akt在各种局部信号网络中的作用，并能够开发用于特异性阻断参与癌症发展和进展的信号通路的策略。 Par-4是一种亮氨酸拉链结构域蛋白，当异位表达时，其诱导癌细胞凋亡，但不诱导正常细胞或永生化细胞凋亡。异位Par-4的凋亡通过抑制NF-κ B活性而发生。由于癌细胞含有合理水平的内源性Par-4，我们试图确定Par-4是否以无活性形式存在。我们的初步研究表明，Akt 1结合和失活内源性Par-4，使其无效的骨化诱导。此外，Akt 1的失活释放Par-4以诱导细胞凋亡，这意味着内源性Par-4在Akt 1不存在的情况下具有功能活性。鉴于Akt 1的促生存功能和Par-4的促凋亡功能，本提案的目的是研究Akt 1和Par-4在前列腺癌细胞存活和肿瘤进展中相互作用的分子基础和功能相关性。为此，我们提出了以下具体目标：目标1，阐明Par-4的Akt的异构体特异性作用的分子基础;目标2，确定Par-4的细胞质滞留和Akt 1的失活机制;目标3，确定Par-4的下游效应和功能相关性的抑制Akt 1在肿瘤生长。由于PTEN缺失是一种明确的遗传病变，可提高Akt活性并中和前列腺中的凋亡途径，并有助于小鼠模型中的前列腺肿瘤，因此本研究将重点关注前列腺癌细胞背景以研究Akt 1-Par-4相互作用。然而，由于Akt 1-Par-4相互作用发生在不同的肿瘤细胞类型中，我们预计这项研究的发现将对癌症产生广泛的影响。这些发现将在未来的研究中进一步发展，以设计可以阻止Par-4与Akt 1结合并诱导细胞凋亡和肿瘤生长消退的治疗策略。