Abstract

The aim of this project is to define the course of the major physiological cations (calcium, sodium, potassium) from surface to interior of the myocardial cell as affected by binding and/or exchange at the glycocalyx, the sarcolemmal bilayer, the mitochondria and the sarcoplasmic reticulum. In addition the cationic binding and exchange characteristics will be related to the contractile properties of the myocardium. The experiments are designed to dissect current models of excitation-contraction coupling so that the various cellular organelles can be realistically placed in a comprehensive model for the role of the ions in control of the heart's function. The studies will utilize various specialized techniques which have been developed or are in the process of development in the PI's laboratory. These techniques are 1) the scintillator-disk flow cell for tissue culture, 2) the """"""""gas dissected"""""""" membrane from culture, 3) the arterially-perfused interventricular septum 4) the isolated, single cell from adult rat or rabbit heart (all developed in this laboratory and in routine use), 5) the isolated glycocalyx from culture and the 6) planar-oriented sarcolemma from adult heart (both under advanced development). The long term objective of the PI for the past 20 years has been definition of ionic exchange as it relates to myocardial function. The current proposal is designed to continue to pursue this objective through the use of sophisticated flux and radioisotopic techniques as enumerated above. The pursuit of the long term objective will involve experimentation in 6 areas of study. 1) Control of Ca permeability 2) Sarcolemmal-glycocalyx binding. 3) Transmembranous Ca flux via """"""""carrier"""""""" and """"""""channel"""""""". 4) Subcellular Ca compartmentalization. 5) Movement and compartmentalization of Na. 6) Identification of specific sites (and molecules) important in control of cation permeability. The techniques have been designed to minimize extrapolation from isolated experimental systems to the intact, functional cardiac cell as these areas of study are pursued. The proposed program is fundamental to the understanding of the basis of myocardial function. This understanding at the cellular level is crucial to further clinical advances.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL028539-05
Application #
3339909
Study Section
Cardiovascular Study Section (CVA)
Project Start
1982-05-01
Project End
1987-04-30
Budget Start
1986-05-01
Budget End
1987-04-30
Support Year
5
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
Schools of Medicine
DUNS #
119132785
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Ponce-Hornos, J E; Philipson, K D; Bonazzola, P et al. (1999) Energetics of Na(+)-Ca(2+) exchange in resting cardiac muscle. Biophys J 77:3319-27
Marengo, F D; Wang, S Y; Wang, B et al. (1998) Dependence of cardiac cell Ca2+ permeability on sialic acid-containing sarcolemmal gangliosides. J Mol Cell Cardiol 30:127-37
Korge, P; Langer, G A (1998) Mitochondrial Ca2+ uptake, efflux, and sarcolemmal damage in Ca2+-overloaded cultured rat cardiomyocytes. Am J Physiol 274:H2085-93
Marengo, F D; Wang, S Y; Langer, G A (1997) The effects of temperature upon calcium exchange in intact cultured cardiac myocytes. Cell Calcium 21:263-73
Langer, G A; Peskoff, A (1997) Role of the diadic cleft in myocardial contractile control. Circulation 96:3761-5
Barrigon, S; Wang, S Y; Ji, X et al. (1996) Characterization of the calcium overload in cultured neonatal rat cardiomyocytes under metabolic inhibition. J Mol Cell Cardiol 28:1329-37
Wang, S Y; Peskoff, A; Langer, G A (1996) Inner sarcolemmal leaflet Ca(2+) binding: its role in cardiac Na/Ca exchange. Biophys J 70:2266-74
Wang, S Y; Clague, J R; Langer, G A (1995) Increase in calcium leak channel activity by metabolic inhibition or hydrogen peroxide in rat ventricular myocytes and its inhibition by polycation. J Mol Cell Cardiol 27:211-22
Clague, J R; Langer, G A (1994) The pathogenesis of free radical-induced calcium leak in cultured rat cardiomyocytes. J Mol Cell Cardiol 26:11-21
Ji, S; Weiss, J N; Langer, G A (1993) Modulation of voltage-dependent sodium and potassium currents by charged amphiphiles in cardiac ventricular myocytes. Effects via modification of surface potential. J Gen Physiol 101:355-75

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