Abstract

Myocardial contractility is enhanced with development. The proposed studies will test whether increases in cytosolic calcium(Cai) and in the sensitivity of the myofilaments to Ca underlie this enhancement, whether the immature cell depends relatively more on extracellular calcium(Cao), and whether changes in troponin T (TnT) isoform expression with development are correlated with changes in the sensitivity of the myofilaments to Ca. Three preparations obtained from rabbit ventricles at different stages of development will be studied: Calcium-tolerant intact single cells, chemically-skinned single cells, and chemically-skinned multicellular bundles. The membrane-intact isolated cell will be loaded with the fura-2 AM> Sarcomere shortening and changes in the 340/380 fluorescence ration will be measured at various stimulus patterns and perturbations that will allow us to examine the effects of changes in Cai and of different Cao, Nao, and Nao/Cao ratios, with and without the use of a calcium channel blocker. The fluorescence data will be calibrated by measuring the minimum and maximum fluorescence ratios, Rmin and Rmax, of the cell. The effects of age on Cai and extent of it modulation, and their relationship to developmental changes in sarcomere shortening will be examined. Sarcomere shortening waveforms will be recorded from intact cells: the cells will then be chemically skinned and the force-pCa relation determined and compared with that obtained from the multicellular preparation. The effects of development on the relation and on Cai will be studied. The force-pCa relation of chemically-skinned multicellular bundles will be measured and analyzed. Polyacrylamide gel electrophoresis will be used to examine the protein profile of the bundle. The proportion of TnT isoforms expressed in each bundle will be obtained from the gel and will be compared to the force-pCa characteristics of the preparation, pCa50 and the Hill constant. The effect of TnT isoform expression and its changes with development on the force-pCa relation will be analyzed. The proposed studies will provide new data that will allow us to test hypotheses that relate the control of Cai, the Ca sensitivity of the myofilaments, and the troponin T isoforms to the maturational increase in contractility.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL020749-14
Application #
3336240
Study Section
Cardiovascular and Pulmonary Research A Study Section (CVA)
Project Start
1988-12-01
Project End
1993-11-30
Budget Start
1992-12-01
Budget End
1993-11-30
Support Year
14
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Duke University
Department
Type
Schools of Medicine
DUNS #
071723621
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

McCall, Shannon J; Nassar, Rashid; Malouf, Nadia N et al. (2006) Development and cardiac contractility: cardiac troponin T isoforms and cytosolic calcium in rabbit. Pediatr Res 60:276-81
Peterson, J N; Nassar, R; Anderson, P A et al. (2001) Altered cross-bridge characteristics following haemodynamic overload in rabbit hearts expressing V3 myosin. J Physiol 536:569-82
Malouf, N N; Coleman, W B; Grisham, J W et al. (2001) Adult-derived stem cells from the liver become myocytes in the heart in vivo. Am J Pathol 158:1929-35
Chai, P J; Nassar, R; Oakeley, A E et al. (2000) Soluble complement receptor-1 protects heart, lung, and cardiac myofilament function from cardiopulmonary bypass damage. Circulation 101:541-6
Margossian, S S; Anderson, P A; Chantler, P D et al. (1999) Calcium regulation in the human myocardium affected by dilated cardiomyopathy: a structural basis for impaired Ca2+-sensitivity. Mol Cell Biochem 194:301-13
Ricchiuti, V; Voss, E M; Ney, A et al. (1998) Cardiac troponin T isoforms expressed in renal diseased skeletal muscle will not cause false-positive results by the second generation cardiac troponin T assay by Boehringer Mannheim. Clin Chem 44:1919-24
Bodor, G S; Oakeley, A E; Allen, P D et al. (1997) Troponin I phosphorylation in the normal and failing adult human heart. Circulation 96:1495-500
Saba, Z; Nassar, R; Ungerleider, R M et al. (1996) Cardiac troponin T isoform expression correlates with pathophysiological descriptors in patients who underwent corrective surgery for congenital heart disease. Circulation 94:472-6
Anderson, P A; Greig, A; Mark, T M et al. (1995) Molecular basis of human cardiac troponin T isoforms expressed in the developing, adult, and failing heart. Circ Res 76:681-6
Anderson, P A; Fair, E C; Nassar, R et al. (1994) A hemodynamic excitatory response to veratridine in the in utero lamb. Pediatr Res 35:550-4

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