Abstract

G protein-coupled receptors (GPCRs) are key regulators of cell physiology, controlling processes that range from the sensation of light to the contractility of the heart. GPCR kinases (GRKs) phosphorylate active GPCRs at sites in their cytoplasmic loops and C-terminal tails, thereby promoting uncoupling of these receptors from heterotrimeric G proteins and ultimately their internalization. Although GRKs allow cells to adapt to changes in their environment and protect against damage incurred by sustained signaling, aberrant GRK activity is strongly associated with diseases such as heart failure and cardiac hypertrophy. Furthermore, inhibition of GRK activity is expected to enhance the action of many drugs that promote GPCR signaling. During and since the last funding cycle, our lab has made substantial advances in the identification and development of GRK selective small molecule inhibitors. We determined the crystal structure of GRK2 in complex with a selective RNA aptamer, and then used this macromolecule as a tool to identify the FDA-approved drug paroxetine as a selective inhibitor of GRK2 activity in vitro and in vivo that improves outcome in myocardial infarcted mice. Furthermore, we conducted several ligand-induced thermal stability screens that identified additional chemical scaffolds that potently and selectivity inhibits GRK2 and GRK5. Subsequent rational design based on crystal structures of these leads in complex with various GRKs led to the development of more potent compounds, one of which assisted us in determining the atomic structure of GRK5. In the first aim, we will further develop and characterize hybrid inhibitors of GRK2 based on the two most promising scaffolds.
The second aim i s devoted to testing how these compounds affect GRK2 recruitment to membranes and receptors and how they perform in cell-based and whole animal models relevant to human disease. In the third aim, we will use our inhibitors to help investigate how GRK5 interacts with membranes and Ca2+*CaM, which together regulate the entry of GRK5 into the nucleus where it promotes the expression of genes that cause cardiac hypertrophy. Collectively, these studies are designed to create a chemical tool box that can be used to help decipher the function of specific GRKs in living cells and disease states, to take a significant step closer towards development of new therapeutic agents for the treatment of heart disease, and to achieve a better understanding of how GRKs interact with their cellular targets.

Public Health Relevance

G protein-coupled receptor (GPCR) kinases (GRKs) regulate the activity of most of the ~800 GPCRs in the human genome and play an adaptive role in cells. Some GRKs are also overexpressed in pathophysiological conditions. For example, GRK2 and GRK5 are strongly implicated in the progression of heart failure and cardiac hypertrophy, respectively. This proposal seeks to develop chemical probes that selectively inhibit GRKs in cells. These probes could also serve as therapeutic leads for the treatment of heart disease and as useful tools to further investigate how GRKs interact with their cellular targets.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
7R01HL071818-14
Application #
9553163
Study Section
Molecular and Integrative Signal Transduction Study Section (MIST)
Program Officer
Balijepalli, Ravi C
Project Start
2004-01-01
Project End
2019-06-30
Budget Start
2017-09-01
Budget End
2018-06-30
Support Year
14
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Purdue University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
072051394
City
West Lafayette
State
IN
Country
United States
Zip Code
47907

  Publications

Beyett, Tyler S; Gan, Xinmin; Reilly, Shannon M et al. (2018) Carboxylic Acid Derivatives of Amlexanox Display Enhanced Potency toward TBK1 and IKK? and Reveal Mechanisms for Selective Inhibition. Mol Pharmacol 94:1210-1219
Sakr, Moustafa; Li, Xiao-Yan; Sabeh, Farideh et al. (2018) Tracking the Cartoon mouse phenotype: Hemopexin domain-dependent regulation of MT1-MMP pericellular collagenolytic activity. J Biol Chem 293:8113-8127
Cannavo, Alessandro; Koch, Walter J (2018) GRK2 as negative modulator of NO bioavailability: Implications for cardiovascular disease. Cell Signal 41:33-40
Hinkovska-Galcheva, Vania; Kelly, Robert; Manthei, Kelly A et al. (2018) Determinants of pH profile and acyl chain selectivity in lysosomal phospholipase A2. J Lipid Res 59:1205-1218
de Lucia, Claudio; Gambino, Giuseppina; Petraglia, Laura et al. (2018) Long-Term Caloric Restriction Improves Cardiac Function, Remodeling, Adrenergic Responsiveness, and Sympathetic Innervation in a Model of Postischemic Heart Failure. Circ Heart Fail 11:e004153
Grisanti, Laurel A; Schumacher, Sarah M; Tilley, Douglas G et al. (2018) Designer Approaches for G Protein-Coupled Receptor Modulation for Cardiovascular Disease. JACC Basic Transl Sci 3:550-562
Waldschmidt, Helen V; Bouley, Renee; Kirchhoff, Paul D et al. (2018) Utilizing a structure-based docking approach to develop potent G protein-coupled receptor kinase (GRK) 2 and 5 inhibitors. Bioorg Med Chem Lett 28:1507-1515
Beyett, Tyler S; Gan, Xinmin; Reilly, Shannon M et al. (2018) Design, synthesis, and biological activity of substituted 2-amino-5-oxo-5H-chromeno[2,3-b]pyridine-3-carboxylic acid derivatives as inhibitors of the inflammatory kinases TBK1 and IKK? for the treatment of obesity. Bioorg Med Chem 26:5443-5461
Bouley, Renee; Waldschmidt, Helen V; Cato, M Claire et al. (2017) Structural Determinants Influencing the Potency and Selectivity of Indazole-Paroxetine Hybrid G Protein-Coupled Receptor Kinase 2 Inhibitors. Mol Pharmacol 92:707-717
Yao, Xin-Qiu; Cato, M Claire; Labudde, Emily et al. (2017) Navigating the conformational landscape of G protein-coupled receptor kinases during allosteric activation. J Biol Chem 292:16032-16043

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