Abstract

The major goal of this proposal is to use a multidisciplinary approach to identify the factors that may convert the initial adaptive phase of cardiac hypertrophy to the terminal phase of myocardial failure and death. A second and related goal is to investigate the pathophysiologic basis for the mechanical, structural, and electrical dysfunction associated with cardiac hypertrophy itself. To achieve these goals the Program is comprised of nine research projects designed to investigate various aspects of a pathophysiologic sequence of events we have formulated on the basis of previous experimental work in models of myocardial disease: (1) Hypertrophy induced by pressure overload; (2) Reactive hypertrophy after myocardial infarction; (3) Acquired cardiomyopathy induced by combined pressure overload hypertrophy and diabetes; (4) Genetic cardiomyopathy. Tissue from failing human hearts removed prior to transplantation also will be studied. A variety of experimental techniques will be used: voltage clamp studies in isolated single cardiac cells; assessment of myocardial mechanics and sarcomere dynamics by light diffraction in isolated cells and intact muscles; characterization of intrinsic connective tissue by special staining techniques, immuno-localization, and scanning electron microscopy; biochemical analysis of myosin isoenzymes, protease activity and sarcolemmal composition; investigation of vascular architecture and distribution; morphometric analysis of infarct size; use of recombinant DNA techniques to isolate and characterize the genes associated with myosin heavy chains and other contractile proteins; measurements of transmittal flow and hemodynamic parameters in the intact heart. The importance of elucidating the mechanisms responsible for causing the evolution of adaptive hypertrophy to cardiac failure is emphasized by the fact that despite palliation of symptoms, no presently available therapeutic interventions have been shown to improve the survival of patients with congestive cardiomyopathy and heart failure. Furthermore, many patients with cardiac failure die suddenly without evidence of hemodynamic deterioration; sudden death in those patients is believed to be due to arrhythmias. We believe that the results of the proposed studies will provide a better understanding of the pathophysiologic processes that ultimately lead to cardiac failure, lethal arrhythmias, and death in patients with heart disease. We anticipate that elucidation of such pathophysiologic processes should improve our ability to prevent the often fatal outcome of patients with cardiac failure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL037412-02
Application #
3098572
Study Section
Heart, Lung, and Blood Research Review Committee A (HLBA)
Project Start
1988-09-30
Project End
1993-09-29
Budget Start
1989-09-30
Budget End
1990-09-29
Support Year
2
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Type
Schools of Medicine
DUNS #
009095365
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Takahashi, S; Geenen, D; Nieves, E et al. (1999) Collagenase degrades collagen in vivo in the ischemic heart. Biochim Biophys Acta 1428:251-9
Nordin, C (1997) Computer model of electrophysiological instability in very small heterogeneous ventricular syncytia. Am J Physiol 272:H1838-56
Nordin, C (1996) Response of Ca(2+)-loaded, depolarized guinea pig myocytes to critically timed premature stimulations. Am J Physiol 270:H447-65
Malhotra, A; Lopez, M C; Nakouzi, A (1995) Troponin subunits contribute to altered myosin ATPase activity in diabetic cardiomyopathy. Mol Cell Biochem 151:165-72
Nordin, C; Ming, Z (1995) Computer model of current-induced early afterdepolarizations in guinea pig ventricular myocytes. Am J Physiol 268:H2440-59
Nikolic, S D; Feneley, M P; Pajaro, O E et al. (1995) Origin of regional pressure gradients in the left ventricle during early diastole. Am J Physiol 268:H550-7
Akella, A B; Ding, X L; Cheng, R et al. (1995) Diminished Ca2+ sensitivity of skinned cardiac muscle contractility coincident with troponin T-band shifts in the diabetic rat. Circ Res 76:600-6
De Leon, J R; Buttrick, P M; Fishman, G I (1994) Functional analysis of the connexin43 gene promoter in vivo and in vitro. J Mol Cell Cardiol 26:379-89
Straceski, A J; Nakouzi, A S; Malhotra, A (1994) Expression of regulated cardiac troponin I in Escherichia coli. J Mol Cell Cardiol 26:1565-72
Lonn, E; Factor, S M; Van Hoeven, K H et al. (1994) Effects of oxygen free radicals and scavengers on the cardiac extracellular collagen matrix during ischemia-reperfusion. Can J Cardiol 10:203-13

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