Abstract

OF WORK: Project 2 ? Dissecting GRK Function in the Heart Research over the last two decades has shown that increased G protein-coupled receptor (GPCR) kinase-2 (GRK2) expression and activity in the cardiomyocyte, which can occur after stress/injury, is pathological to the heart. Studies have shown that lowering GRK2 expression or inhibiting its activity in myocytes rescues several different animal models of heart failure (HF). Mechanistically, new data has revealed that GRK2-mediated myocardial pathology can occur through both GPCR-dependent and GPCR-independent actions. Over the last funding cycle of this PPG, we found, using genetically engineered mice including a novel GRK2 knock-in mouse (GRK2-C340S) where endogenous GRK2 can no longer be regulated via nitric oxide (NO) bioavailability (through S-nitrosylation), that GRK2 can induce cardiac injury through disruption of the normal nitroso-redox balance of the myocyte. More recent data demonstrates that increased GRK2 can induce cellular reactive oxygen species (ROS) and this appears to be mitochondrial in origin, which is interesting since we have discovered GRK2 can reside in mitochondria. In this competitive renewal we are interested in delineating the mechanistic role of GRK2 on the oxidative state and nitroso-redox imbalance of the injured and stressed cardiomyoycte, especially during HF development. Importantly, since other components of GPCR signaling are also targets of S-nitrosylation, we have the unique opportunity through this PPG group to dissect GRK2/?-arrestin/GPCR mechanisms when NO bioavailability is altered. Finally, we have recently uncovered that the oxidative stress induced in the heart by the neurohormone aldosterone, which is implicated in human HF development through activation of its mineralocorticoid receptor, can also involve GRK2 and this will be explored herein. This project will specifically test the overall hypothesis that GRK2 is a key component of myocyte oxidative stress imbalance including through its inter-relationship with the NO signaling system and mitochondrial targeting. Moreover, we believe that GRK2 plays a key and novel role in promoting myocyte injury downstream of hyper-aldosteronism. These studies will also delineate new mechanisms supporting the therapeutic benefits of GRK2 lowering and inhibition in dysfunctional myocardium.
Specific Aims are: [1] To determine whether dynamic S-nitrosylation plays a role in GRK2-mediated pathology during HF development; [2] To determine the mitochondrial targets of GRK2 in the myocyte that play a mechanistic role in altering mitochondrial function including metabolism and ROS formation; and [3] To determine the role of GRK2 in aldosterone-mediated cardiac pathology.

Public Health Relevance

Project 2 ? Dissecting GRK Function in the Heart Heart failure (HF) is a major health problem and understanding molecular processes involved in its development can advance translation of novel therapies. We have found that GRK2 plays a key role in chronic HF through classical effects and also novel effects. This inlcudes regulation of this enzyme by nitric oxide. Continued research in this area, as described in this proposal, can lead to new HF strategies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
2P01HL075443-11
Application #
8932314
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
Project End
Budget Start
2015-08-01
Budget End
2016-05-31
Support Year
11
Fiscal Year
2015
Total Cost
$340,804
Indirect Cost
$14,750

  Institution

Name
Duke University
Department
Type
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Kim, Jihee; Grotegut, Chad A; Wisler, James W et al. (2018) ?-arrestin 1 regulates ?2-adrenergic receptor-mediated skeletal muscle hypertrophy and contractility. Skelet Muscle 8:39
Zhou, Hua-Lin; Stomberski, Colin T; Stamler, Jonathan S (2018) Cross Talk Between S-Nitrosylation and Phosphorylation Involving Kinases and Nitrosylases. Circ Res 122:1485-1487
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
de Lucia, Claudio; Eguchi, Akito; Koch, Walter J (2018) New Insights in Cardiac ?-Adrenergic Signaling During Heart Failure and Aging. Front Pharmacol 9:904
Wang, Jialu; Hanada, Kenji; Gareri, Clarice et al. (2018) Mechanoactivation of the angiotensin II type 1 receptor induces ?-arrestin-biased signaling through G?i coupling. J Cell Biochem 119:3586-3597
Hayashi, Hiroki; Hess, Douglas T; Zhang, Rongli et al. (2018) S-Nitrosylation of ?-Arrestins Biases Receptor Signaling and Confers Ligand Independence. Mol Cell 70:473-487.e6
Rizza, Salvatore; Cardaci, Simone; Montagna, Costanza et al. (2018) S-nitrosylation drives cell senescence and aging in mammals by controlling mitochondrial dynamics and mitophagy. Proc Natl Acad Sci U S A 115:E3388-E3397
Cannavo, Alessandro; Koch, Walter J (2018) GRK2 as negative modulator of NO bioavailability: Implications for cardiovascular disease. Cell Signal 41:33-40
Wang, Jialu; Gareri, Clarice; Rockman, Howard A (2018) G-Protein-Coupled Receptors in Heart Disease. Circ Res 123:716-735

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