Abstract

This renewal application of our Program Project consists of four projects employing lipid bilayers, membrane vessicles and patches, perfused papillary muscles and intact in situ hearts which explore the causes of the electrical abnormalities underlying ischemia-induced ventricular fibrillation and sudden cardiac death. The projects are supported by an Animal/Laboratory Support core (A), a Technical Core (B), and an Administrative Core (C) and are also united by their use of common preparations and common technologies. The in situ pig heart with a carotid to left anterior descending (LAD) coronary artery shunt is used in Projects 1 to explore a unique model of reproducible ventricular fibrillation which occurs when the interruption of flow through the LAD shunt is preceded by the elevation of potassium in the LAD distribution. The project seeks to characterize and to determine the causes of the very slow conduction which invariably precedes ventricular fibrillation. It will also employ the intact perfused rabbit papillary muscle preparation used in Project 2 to test the hypothesis that CO2 diffusion at the border between ischemic and nonischemic tissues causes inhomogeneous changes in intracellular pH and calcium that result in inhomogeneous electrical changes, including very slow conduction. Project 3 uses lipid bilayers to determine the effects of changes in intracellular pH, calcium and magnesium on the voltage dependent L-type calcium channel in order to better understand the factors causing the rise in intracellular calcium that is thought to underlie many of the ischemia induced electrical events. The Technical Core provides electrode, electronic, and computer support. It takes advantage of unique interactions within and without the University of North Carolina to develop new capabilities which will be directly applied to the individual projects. Our program reflects a maturation of our concepts over the last five years and involves investigators from the Departments of Medicine, Biochemistry and Biophysics, Cell Biology and Anatomy, Pharmacology, Biomedical Engineering, and Biostatistics and includes extensive interaction and collaboration with investigators at Duke University, North Carolina State University, and the National Institutes for Environment Health Sciences, The Department of Experimental Cardiology at the University of Amsterdam, the Netherlands, and the Physiologisches Institut, University of Bern, Switzerland.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL027430-13
Application #
2216149
Study Section
Heart, Lung, and Blood Research Review Committee A (HLBA)
Project Start
1982-07-01
Project End
1997-11-30
Budget Start
1994-12-01
Budget End
1995-11-30
Support Year
13
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Cole, R T; Lucas, C L; Cascio, W E et al. (2005) A LabVIEW model incorporating an open-loop arterial impedance and a closed-loop circulatory system. Ann Biomed Eng 33:1555-73
Cascio, Wayne E; Yang, Hua; Muller-Borer, Barbara J et al. (2005) Ischemia-induced arrhythmia: the role of connexins, gap junctions, and attendant changes in impulse propagation. J Electrocardiol 38:55-9
Xu, Le; Meissner, Gerhard (2004) Mechanism of calmodulin inhibition of cardiac sarcoplasmic reticulum Ca2+ release channel (ryanodine receptor). Biophys J 86:797-804
Kim, Chang-Soo; Ufer, Stefan; Seagle, Christopher M et al. (2004) Use of micromachined probes for the recording of cardiac electrograms in isolated heart tissues. Biosens Bioelectron 19:1109-16
Graff, Ronald D; Kelley, Scott S; Lee, Greta M (2003) Role of pericellular matrix in development of a mechanically functional neocartilage. Biotechnol Bioeng 82:457-64
Stange, Mirko; Xu, Le; Balshaw, David et al. (2003) Characterization of recombinant skeletal muscle (Ser-2843) and cardiac muscle (Ser-2809) ryanodine receptor phosphorylation mutants. J Biol Chem 278:51693-702
Bidasee, Keshore R; Xu, Le; Meissner, Gerhard et al. (2003) Diketopyridylryanodine has three concentration-dependent effects on the cardiac calcium-release channel/ryanodine receptor. J Biol Chem 278:14237-48
Sun, Junhui; Xu, Le; Eu, Jerry P et al. (2003) Nitric oxide, NOC-12, and S-nitrosoglutathione modulate the skeletal muscle calcium release channel/ryanodine receptor by different mechanisms. An allosteric function for O2 in S-nitrosylation of the channel. J Biol Chem 278:8184-9
Yamaguchi, Naohiro; Xu, Le; Pasek, Daniel A et al. (2003) Molecular basis of calmodulin binding to cardiac muscle Ca(2+) release channel (ryanodine receptor). J Biol Chem 278:23480-6
Meissner, Gerhard (2002) Regulation of mammalian ryanodine receptors. Front Biosci 7:d2072-80

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