Abstract

Excessive activation of G protein-coupled receptors and their target G proteins contributes to cardiovascular diseases such as hypertension, congestive heart failure, and vascular restenosis. Furthermore, mutations leading to constitutively active or """"""""runaway"""""""" receptors have been found which play a role in genetic diseases and are likely to contribute to complex polygenic disorders of the cardiovascular system. There are two ways to block excess G protein stimulation which are effective against both constitutively activated and ligand-activated receptors: 1) inverse agonists and 2) inhibition of the signal downstream of receptor such as at the receptor-G protein (or RG) interface. To date, the RG interface has not been fully exploited as a possible target of drug action though it has great potential. Knowledge of the structural basis of RG interactions would facilitate the development of practical inhibitors at this useful and potentially specific drug target. The diversity of G protein subunits provides a rich basis for specificity with numerous alpha (a), beta(b)and gamma (y) subunit subtypes. Understanding precisely where on the G protein surface the receptor binds will greatly facilitate the design of specific drugs targeting this site. Since the Gab or Gay interface includes structural determinants from both subunits, this would be an ideal location for designing uniquely specific drugs acting downstream of G protein coupled receptors. This project will use a multi-faceted approach to study the structure and function of the RG interface.
The specific aims of the present project are to utilize a genetic strategy to identify all functional contacts between receptor and G protein, to produce an atomic level molecular model of the receptor-G protein complex, to utilize biochemical cross-linking and functional studies to define the receptor G protein interface with emphasis on the contributions of G band y subunits, and to examine the changes in a2 adrenergic receptor-Gafty contacts that occur in different receptor and G protein conformational states. This work should greatly improve our understanding of the structural and mechanistic basis of RG coupling and should facilitate the design of drugs that target particular G protein subunit combinations.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL046417-12
Application #
6688264
Study Section
Special Emphasis Panel (ZRG1-PTHA (02))
Program Officer
Lin, Michael
Project Start
1992-02-01
Project End
2004-12-31
Budget Start
2004-01-01
Budget End
2004-12-31
Support Year
12
Fiscal Year
2004
Total Cost
$264,250
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Pharmacology
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Lim, William K; Kanelakis, Kimon C; Neubig, Richard R (2013) Regulation of G protein signaling by the 70kDa heat shock protein. Cell Signal 25:389-96
Myung, Chang-Seon; Lim, William K; DeFilippo, Joseph M et al. (2006) Regions in the G protein gamma subunit important for interaction with receptors and effectors. Mol Pharmacol 69:877-87
Chai, Biao-Xin; Pogozheva, Irina D; Lai, Yu-Mei et al. (2005) Receptor-antagonist interactions in the complexes of agouti and agouti-related protein with human melanocortin 1 and 4 receptors. Biochemistry 44:3418-31
Chai, Biao-Xin; Neubig, Richard R; Millhauser, Glenn L et al. (2003) Inverse agonist activity of agouti and agouti-related protein. Peptides 24:603-9
Simons, Peter C; Shi, Mei; Foutz, Terry et al. (2003) Ligand-receptor-G-protein molecular assemblies on beads for mechanistic studies and screening by flow cytometry. Mol Pharmacol 64:1227-38
Goubaeva, Farida; Ghosh, Mousumi; Malik, Sundeep et al. (2003) Stimulation of cellular signaling and G protein subunit dissociation by G protein betagamma subunit-binding peptides. J Biol Chem 278:19634-41
Soyer, Orkun S; Dimmic, Matthew W; Neubig, Richard R et al. (2003) Dimerization in aminergic G-protein-coupled receptors: application of a hidden-site class model of evolution. Biochemistry 42:14522-31
Chung, Duane A; Zuiderweg, Erik R P; Fowler, Carol B et al. (2002) NMR structure of the second intracellular loop of the alpha 2A adrenergic receptor: evidence for a novel cytoplasmic helix. Biochemistry 41:3596-604
Sarvazyan, Noune A; Lim, William K; Neubig, Richard R (2002) Fluorescence analysis of receptor-G protein interactions in cell membranes. Biochemistry 41:12858-67
Chung, Duane A; Wade, Susan M; Fowler, Carol B et al. (2002) Mutagenesis and peptide analysis of the DRY motif in the alpha2A adrenergic receptor: evidence for alternate mechanisms in G protein-coupled receptors. Biochem Biophys Res Commun 293:1233-41

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