Abstract

Human heart failure is characterized by profound catecholamine desensitization, in vivo, accompanied by alterations in beta-adrenergic signaling, in vitro, e.g., decreases in cardiac beta-adrenergic receptors, increases in Gialpha, and reductions in adenylyl cyclase activity. Our recent studies in dogs with chronic ventricular denervation and heart failure demonstrate marked attenuation of catecholamine desensitization. The first hypothesis to be tested is that in the absence of cardiac nerves, beta-adrenergic receptor signaling is present during the development of heart failure, e.g., by suppressing beta-adrenergic receptor kinase levels or maintaining the catalytic unit of adenylyl cyclase. This will be studied in dogs with and without selective ventricular denervation with chronic rapid ventricular pacing-induced heart failure. The first goal of this proposal is to define the cellular mechanisms responsible for the preserved catecholamine responsiveness. In vitro, the adrenergic receptor-G-protein-adenylyl cyclase signal transduction system will be studied. The second hypothesis to be tested is that differences in beta-adrenergic signaling in animals with ventricular denervation and heart failure may be affected by hemodynamics and cardiac geometry. To address this, isolated myocytes will be studied, first in terms of contraction and relaxation in both endo- and epicardial layers in response to isoproterenol, norepinephrine, forskolin and calcium. Secondly, studies of beta-adrenergic receptors, adenylyl cyclase and G-proteins will be examined in sarcolemmal preparations from the isolated myocytes. Thus, the current proposal contains two unique features. This proposal will provide the first data on altered catecholamine desensitization mechanisms in heart failure due to interruption of cardiac nerves. This part of the proposal has obvious significance not only for patients with transplanted hearts, which are denervated, but also for understanding basic mechanisms involved in autonomic regulation in heart failure. This becomes particularly important in view of recent clinical studies showing beneficial effects in patients in heart failure. Secondly, no study has systematically examined catecholamine desensitization mechanisms using a combination of in vivo studies and isolated myocytes for transmural physiology, biochemistry and molecular biology.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
7R01HL065183-02
Application #
6185199
Study Section
Experimental Cardiovascular Sciences Study Section (ECS)
Project Start
1999-09-30
Project End
2003-08-31
Budget Start
2000-09-01
Budget End
2001-08-31
Support Year
2
Fiscal Year
2000
Total Cost
$247,418
Indirect Cost

  Institution

Name
University of Medicine & Dentistry of NJ
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
605799469
City
Newark
State
NJ
Country
United States
Zip Code
07107

  Publications

Ho, David; Yan, Lin; Iwatsubo, Kousaku et al. (2010) Modulation of beta-adrenergic receptor signaling in heart failure and longevity: targeting adenylyl cyclase type 5. Heart Fail Rev 15:495-512
Yan, Lin; Vatner, Dorothy E; O'Connor, J Patrick et al. (2007) Type 5 adenylyl cyclase disruption increases longevity and protects against stress. Cell 130:247-58
Peter, Pallavi S; Brady, Jennifer E; Yan, Lin et al. (2007) Inhibition of p38 alpha MAPK rescues cardiomyopathy induced by overexpressed beta 2-adrenergic receptor, but not beta 1-adrenergic receptor. J Clin Invest 117:1335-43
Liu, Jing; Sadoshima, Junichi; Zhai, Peiyong et al. (2006) Pressure overload induces greater hypertrophy and mortality in female mice with p38alpha MAPK inhibition. J Mol Cell Cardiol 41:680-8
Yatani, A; Shen, Y-T; Yan, L et al. (2006) Down regulation of the L-type Ca2+ channel, GRK2, and phosphorylated phospholamban: protective mechanisms for the denervated failing heart. J Mol Cell Cardiol 40:619-28
Depre, Christophe; Wang, Qian; Yan, Lin et al. (2006) Activation of the cardiac proteasome during pressure overload promotes ventricular hypertrophy. Circulation 114:1821-8
Yan, Lin; Sadoshima, Junichi; Vatner, Dorothy E et al. (2006) Autophagy: a novel protective mechanism in chronic ischemia. Cell Cycle 5:1175-7
Yan, Lin; Vatner, Dorothy E; Kim, Song-Jung et al. (2005) Autophagy in chronically ischemic myocardium. Proc Natl Acad Sci U S A 102:13807-12
Hase, Makoto; Depre, Christophe; Vatner, Stephen F et al. (2005) H11 has dose-dependent and dual hypertrophic and proapoptotic functions in cardiac myocytes. Biochem J 388:475-83
Song, Long-Sheng; Pi, Yeqing; Kim, Song-Jung et al. (2005) Paradoxical cellular Ca2+ signaling in severe but compensated canine left ventricular hypertrophy. Circ Res 97:457-64

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