High throughput assay for novel pharmacological probes targeting cAMP signaling

针对 cAMP 信号传导的新型药理学探针的高通量测定

基本信息

批准号：
8477859
负责人：
XIAODONG CHENG
金额：
$ 3.83万
依托单位：
UNIVERSITY OF TEXAS MED BR GALVESTON
依托单位国家：
美国
项目类别：
财政年份：
2010
资助国家：
美国
起止时间：
2010-07-01 至 2013-06-30
项目状态：
已结题

项目摘要

DESCRIPTION (provided by applicant): cAMP-mediated cell signaling regulates a myriad of important biological processes under both physiological and pathological conditions, including diabetes, heart failure, and cancer. In eukaryotic cells, the effects of cAMP are transduced by two intracellular cAMP receptors, the classic protein kinase A/cAMP-dependent protein kinase (PKA/cAPK) and the recently discovered exchange protein directly activated by cAMP/cAMP-regulated guanine nucleotide exchange factor (Epac/cAMP-GEF). Like PKA, Epac contains a cAMP-binding domain, an evolutionally conserved structural motif that acts as a molecular switch for sensing intracellular second messenger cAMP levels. The discovery of Epac has opened a new dimension in studying the cAMP-mediated signaling as both PKA and Epac are ubiquitously expressed in all tissues. An increase in intracellular cAMP levels will lead to the activation of both PKA and Epac. Therefore, the net cellular effects of cAMP are not just dictated by PKA or Epac alone, but dependent upon the dynamic expression of Epac and PKA and their specific subcellular distribution in a particular tissue. Currently, the physiological functions of Epac are not clear. One of the major challenges within the research field is the lack of Epac-specific antagonists to dissect the specific physiological functions that Epac play in the overall cAMP-mediated signaling. The objective of this proposal is to develop a High Throughput Screening (HTS) assay for the discovery of novel molecular probes that are specific for Epac but not PKA. These Epac-specific probes will be powerful pharmacological tools for investigating the biological functions of Epac and molecular mechanism of cAMP signaling as well as, for promoting an understanding of disease mechanisms related to Epac/cAMP signaling. PUBLIC HEALTH RELEVANCE: The goal of our proposed research is to develop a High Throughput Screening assay for the discovery of novel target-specific pharmacological probes that can be used for elucidating the mechanism of signal transduction mediated by an important second messenger, cAMP. The medical and pharmacological implications of this research program are far-reaching. Novel pharmacological probes targeting specific cAMP signaling components can potentially lead to the identification of mechanism-based therapeutic strategies for diseases associated with cAMP signaling.

描述（由申请人提供）：在生理和病理状况（包括糖尿病，心力衰竭和癌症）下，CAMP介导的细胞信号传导调节了无数重要的生物学过程。在真核细胞中，cAMP的作用被两个细胞内cAMP受体转导，即经典蛋白激酶A/CAMP依赖性蛋白激酶（PKA/CAPK）和最近发现的cAMP/CAMP调节鸟嘌呤核苷酸交换因子直接激活的最近发现的交换蛋白（EPAC/CAMP-GEF）。像PKA一样，EPAC也包含一个营地结合域，这是一种进化保守的结构基序，它是一种分子开关，用于感应细胞内的第二信使camp水平。 EPAC的发现为研究CAMP介导的信号传导而开辟了一个新的维度，因为PKA和EPAC在所有组织中都普遍表达。细胞内营地水平的增加将导致PKA和EPAC的激活。因此，CAMP的净细胞效应不仅由PKA或EPAC决定，还取决于EPAC和PKA的动态表达及其在特定组织中的特定亚细胞分布。当前，EPAC的生理功能尚不清楚。研究领域中的主要挑战之一是缺乏EPAC特异性拮抗剂来剖析EPAC在整个CAMP介导的信号传导中发挥的特定生理功能。该提案的目的是开发高吞吐量筛选（HTS）测定法，以发现针对EPAC但不是PKA的新型分子探针。这些EPAC特异性探针将是研究EPAC和CAMP信号传导的生物学功能的强大药理工具，以及促进对与EPAC/CAMP信号相关的疾病机制的理解。公共卫生相关性：我们提出的研究的目的是开发高吞吐量筛选测定法，以发现新型目标特异性药理探针，该探针可用于阐明由重要的第二使者CAMP介导的信号转导机制。该研究计划的医学和药理意义是深远的。针对特定cAMP信号成分的新型药理学探针可能会导致与CAMP信号相关的疾病的基于机制的治疗策略鉴定。