Abstract

In vitro contractile dysfunction is a result of cardiac hypertrophy that is caused by a pressure overload of the ventricular myocardium. This abnormal function occurs whether the pressure overload is from a chronic progressive or an acute overload. In contrast volume overload induced hypertrophy does not result in in vitro contractile dysfunction. In the case of the pressure overload induced hypertrophy, if this process is reversed then the contractile function returns to normal. We have studied an early stage of acute pressure overload right ventricular hypertrophy and found that there is an increase in the connective tissue components of the ventricular myocardium and a change in myocyte size and external sarcolemma surface area/ cell volume ratio. The change in connective tissue associated with pressure overload hypertrophy could contribute directly to compromised contractile performance by altering the elastic properties of the ventricle. The change in myocyte size and shape could contribute indirectly by altering the basic control systems for the contractile apparatus.
The SPECIFIC AIM of this proposal is to determine whether these structural effects or other structural modifications that are found in this pathophysiological model are causally related to the impaired contractile function and therefore have etiologic significance for the eventual changes found in this model. Since the chronic progressive pressure overload model does not cause myocardial injury a comparison to the tissue from the acute pressure overload model will determine if the changes seen are a result of the myocardial injury produced by acute pressure overload. Then a comparison of the pressure overload hypertrophied right ventricular myocardium to the volume overload hypertrophied myocardium will identify those structural alterations associated with the abnormal contractile function and those associated with the hypertrophy process in general. Those alterations unique to the myocardium with contractile dysfunction should return to normal when the hypertrophy process is reversed. This will be examined in the reversed chronic progressive pressure overload model. Morphometric ultrastructural studies are used to compare and contrast the right ventricular myocardium under these different hemodynamic conditions. These studies relate to our long-term objectives which are to determine myocardial alterations that result in abnormal function and ultimately heart failure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL029351-02
Application #
3340455
Study Section
Cardiovascular Study Section (CVA)
Project Start
1984-04-01
Project End
1987-03-31
Budget Start
1985-04-01
Budget End
1986-03-31
Support Year
2
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Temple University
Department
Type
Schools of Medicine
DUNS #
City
Philadelphia
State
PA
Country
United States
Zip Code
19122

  Publications

Marino, T A; Cao, W; Lee, J et al. (1996) Localization of proliferating cell nuclear antigen in the developing and mature rat heart cell. Anat Rec 245:677-84
Reiss, K; Kajstura, J; Capasso, J M et al. (1993) Impairment of myocyte contractility following coronary artery narrowing is associated with activation of the myocyte IGF1 autocrine system, enhanced expression of late growth related genes, DNA synthesis, and myocyte nuclear mitotic division in rats. Exp Cell Res 207:348-60
Marino, T A; Cassidy, M; Marino, D R et al. (1991) Norepinephrine-induced cardiac hypertrophy of the cat heart. Anat Rec 229:505-10
Marino, T A; Haldar, S; Williamson, E C et al. (1991) Proliferating cell nuclear antigen in developing and adult rat cardiac muscle cells. Circ Res 69:1353-60
Pollack, P S; Carson, N L; Nuss, H B et al. (1991) Mechanical properties of adult feline ventricular myocytes in culture. Am J Physiol 260:H234-41
Marino, T A; Walter, R A; Cobb, E et al. (1990) Effects of norepinephrine on neonatal rat cardiocyte growth and differentiation. In Vitro Cell Dev Biol 26:229-36
Marino, T A; Walter, R A; D'Ambra, K et al. (1989) Effects of catecholamines on fetal rat cardiocytes in vitro. Am J Anat 186:127-32
Marino, T A; Kuseryk, L; Lauva, I K (1987) Role of contraction in the structure and growth of neonatal rat cardiocytes. Am J Physiol 253:H1391-9
Cooper 4th, G (1987) Cardiocyte adaptation to chronically altered load. Annu Rev Physiol 49:501-18
Cooper 4th, G; Mercer, W E; Hoober, J K et al. (1986) Load regulation of the properties of adult feline cardiocytes. The role of substrate adhesion. Circ Res 58:692-705

Showing the most recent 10 out of 16 publications