Transcriptional regulation by TEF-1 in cardiac myocytes

TEF-1 在心肌细胞中的转录调控

• 批准号: 6822829
• 负责人: IAIN K FARRANCE
• 金额: $ 29.22万
• 依托单位: UNIVERSITY OF MARYLAND BALTIMORE
• 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 2008-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6822829
• 关键词: Adenoviridae; affinity chromatography; cardiac myocytes; cofactor; gene expression; laboratory rat; small interfering RNA; transcription factor; transfection /expression vector; ventricular hypertrophy

DESCRIPTION (provided by applicant): Cardiovascular diseases are the leading cause of death in developed countries, with a very poor prognosis for patients in advanced stages. Congestive heart failure, the end result of many cardiovascular problems is one of the most expensive health problems in the United States. Although there have been dramatic improvements in the treatment of cardiovascular diseases their continued poor prognosis makes the development of novel therapies necessary. During cardiac development, during normal life and during cardiovascular disease there are complex changes in gene expression controlled by multiple transcription factors and their cofactors (Nkx2, MEF2, NFAT, SRF, GATA, HDACs, HATs and TEF-1). It is known how the activity of some but not all of these factors, such as TEF-1 is regulated at a gross level. The research in this proposal will concentrate on determining the role of the TEF-1 gene family in transcriptional regulation in the heart. The studies will use rat neonatal cardiac myocytes, a well established in vitro model system of normal and diseased heart. The research in this grant will address the hypothesis that interactions between MCAT sites, TEF-1 proteins, their cofactors, and other cardiac transcription factors are key in generating the complex patterns of gene expression in normal and hypertrophic cardiac myocytes. The experiments will (1) determine if TEF-1 regulates endogenous cardiac gene expression in normal and hypertrophic cardiac myocytes (dominant negative proteins, siRNA), (2) determine if MCAT core sequence affects the activity of MCAT sites by influencing the interaction of TEF-1 with its cofactors, (3) isolate novel TEF-1 cofactors by state of the art MS/MS, and (4) study how the TEF-1 cofactors (YAP65, TAZ, CK2) and TEF-1 interact with each other and with other cardiac transcription factors to regulate gene expression in cardiac myocytes under normal and hypertrophic conditions. The approaches that will be used include expression of dominant negative TEF-1 proteins using adenoviral vectors. These analyses will detail the mechanisms of promoter response to specific signals in normal and diseased cardiac myocytes, leading to improved treatments for heart disease.

描述（申请人提供）：心血管疾病是发达国家的主要死亡原因，晚期患者预后极差。充血性心力衰竭是许多心血管疾病的最终结果，是美国最昂贵的健康问题之一。尽管在心血管疾病的治疗方面有了显著的改善，但其持续的不良预后使得开发新的治疗方法成为必要。在心脏发育、正常生活和心血管疾病期间，多种转录因子及其辅助因子（Nkx2、MEF2、NFAT、SRF、GATA、hdac、HATs和TEF-1）控制的基因表达发生复杂变化。目前已知的是，这些因子中的一些（但不是全部）的活性是如何在总体水平上受到调节的，比如TEF-1。本提案的研究将集中于确定TEF-1基因家族在心脏转录调控中的作用。该研究将使用大鼠新生儿心肌细胞，这是一种建立良好的正常和病变心脏体外模型系统。该基金的研究将解决MCAT位点、TEF-1蛋白、它们的辅助因子和其他心脏转录因子之间的相互作用是在正常和肥厚心肌细胞中产生复杂基因表达模式的关键这一假设。实验将(1)确定TEF-1是否调节内源性心脏基因在正常和肥厚心肌细胞中的表达（显性阴性蛋白，siRNA），(2)确定MCAT核心序列是否通过影响TEF-1与其辅助因子的相互作用来影响MCAT位点的活性，(3)通过最先进的MS/MS分离新的TEF-1辅助因子，(4)研究TEF-1辅助因子(YAP65， TAZ，CK2)和TEF-1相互作用，并与其他心脏转录因子相互作用，调节心肌细胞在正常和肥大状态下的基因表达。将使用的方法包括使用腺病毒载体表达显性阴性TEF-1蛋白。这些分析将详细说明启动子对正常和患病心肌细胞中特定信号的反应机制，从而改善心脏病的治疗。