Abstract

The long-term objective of this application is to identify whether oxidative stress is responsible for the introduction of the phenotypic characteristics of the failing heart and whether interventions capable of interfering with the formation of reactive O2 modify the course of cardiac decompensation. Oxidative damage, mediated by activation of the local renin-angiotensin system (RAS) and enhanced by the reduction of nitric oxide (NO) in the stressed heart, may promote apoptotic and necrotic death of myocytes, endothelial cells, smooth muscle cells and fibroblasts. High levels of oxidative challenge trigger cell necrosis and lower levels induce apoptosis. Cardiac cell death results in loss of muscle, coronary arterioles and capillaries, which coupled with cavitary dilation and wall thinning, lead to defects in myocardial perfusion, ventricular dysfunction and ultimately heart failure (HF). Similar mechanisms may be operative in the diseased human heart during its evolution from moderate to severe decompensation and terminal failure, or in the aging mouse heart in which deletion of the eNOS gene should potentiate the effects of oxidative damage on cardiac cell death. Therefore, production of oxygen radicals may be the common denominator of several pathologic states of the heart including the development of the aging myopathy and HF in the elderly. Conversely, recovery from HF with removal of the inciting stimulus may initiate reactive growth restoring myocytes and vascular structures. Synthesis of NO, reduction of oxidative stress, downregulation of the cellular RAS, decreased cell death and attenuation of Ang II-induced myocyte hypertrophy may all contribute to the recovery process. It is postulated that significant regeneration of functioning myocardium is needed for regression of HF. Myocyte proliferation may be critical for the acute reconstitution of ventricular mass and, thereby, telomere length. Rapidly dividing cells may undergo progressive telomeric shortening, loss of DNA, terminal differentiation and growth arrest. These hypotheses will be tested in a model of HF associated with rapid ventricular pacing in dogs, in human hearts with idiopathic dilated cardiomyopathy in class I-IV NYHA and in an aging mouse model with ablation of the eNOS gene and greater potential for oxidative DNA damage and cardiac cell death.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
2P01HL043023-11
Application #
6493621
Study Section
Project Start
1991-01-01
Project End
2006-07-31
Budget Start
Budget End
Support Year
11
Fiscal Year
2001
Total Cost
Indirect Cost

  Institution

Name
New York Medical College
Department
Type
DUNS #
City
Valhalla
State
NY
Country
United States
Zip Code
10595

  Publications

Szekeres, Mária; Nádasy, György L; Dörnyei, Gabriella et al. (2018) Remodeling of Wall Mechanics and the Myogenic Mechanism of Rat Intramural Coronary Arterioles in Response to a Short-Term Daily Exercise Program: Role of Endothelial Factors. J Vasc Res 55:87-97
Alhawaj, Raed; Patel, Dhara; Kelly, Melissa R et al. (2015) Heme biosynthesis modulation via ?-aminolevulinic acid administration attenuates chronic hypoxia-induced pulmonary hypertension. Am J Physiol Lung Cell Mol Physiol 308:L719-28
Song, Su; Kertowidjojo, Elizabeth; Ojaimi, Caroline et al. (2015) Long-term methionine-diet induced mild hyperhomocysteinemia associated cardiac metabolic dysfunction in multiparous rats. Physiol Rep 3:
Huang, An; Pinto, John T; Froogh, Ghezal et al. (2015) Role of homocysteinylation of ACE in endothelial dysfunction of arteries. Am J Physiol Heart Circ Physiol 308:H92-100
Patel, Dhara; Alhawaj, Raed; Wolin, Michael S (2014) Exposure of mice to chronic hypoxia attenuates pulmonary arterial contractile responses to acute hypoxia by increases in extracellular hydrogen peroxide. Am J Physiol Regul Integr Comp Physiol 307:R426-33
Patel, Dhara; Kandhi, Sharath; Kelly, Melissa et al. (2014) Dehydroepiandrosterone promotes pulmonary artery relaxation by NADPH oxidation-elicited subunit dimerization of protein kinase G 1?. Am J Physiol Lung Cell Mol Physiol 306:L383-91
Laurent, D; Mathew, J E; Mitry, M et al. (2014) Chronic ethanol consumption increases myocardial mitochondrial DNA mutations: a potential contribution by mitochondrial topoisomerases. Alcohol Alcohol 49:381-9
Signore, Sergio; Sorrentino, Andrea; Ferreira-Martins, João et al. (2014) Response to letter regarding article ""Inositol 1,4,5-trisphosphate receptors and human left ventricular myocytes"". Circulation 129:e510-1
Neo, Boon Hwa; Patel, Dhara; Kandhi, Sharath et al. (2013) Roles for cytosolic NADPH redox in regulating pulmonary artery relaxation by thiol oxidation-elicited subunit dimerization of protein kinase G1?. Am J Physiol Heart Circ Physiol 305:H330-43
Hicks, S; Labinskyy, N; Piteo, B et al. (2013) Type II diabetes increases mitochondrial DNA mutations in the left ventricle of the Goto-Kakizaki diabetic rat. Am J Physiol Heart Circ Physiol 304:H903-15

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