Abstract

Calcium channels in the surface membrane of heart cells play a central role in excitation-contraction coupling, in normal pacemaker acitivity and in arrhythmogenesis. As the major pathway for Ca influx into the cell, Ca channels help determine the free intracellular Ca concentration, (Ca2+)i. Several lines of evidence indicate that (Ca2+)i in turn exerts feedback control on the availability of Ca channels. An increase in (Ca2+)i has been implicated in the decay of Ca current during depolarization (""""""""inactivation""""""""), as in a number of other preparations. An increase in (Ca2+)i is also believed to exert opposing positive feedback effects on ICa under certain conditions, such as during digitalis inotropy in the heart and during C kinase activation in Aplysia neurones. This project proposes to investigate the basic mechanism(s) of Ca channel regulation by (Ca+)i, under normal conditions and during """"""""Ca overload"""""""" states associated with triggered arrhythmias. Membrane currents will be measured using several variants of the gigaseal (""""""""patch"""""""") voltage clamp technique in single mammalian ventricular cells. Whole-cell Ca current (ICa) recordings will be used to test simple kinetic schemes for Ca-dependent inactivation. Ensemble fluctuation analysis of whole-cell currents will determine whether or not changes in (Ca2+)i affect the number of functional channels. Single channel recordings will enable characterization of the changes in gating behavior underlying positive and negative regulation. Direct simultaneous measurements of (Ca2+)i and ICa will establish quantitatively the relationship between these two variables, and will provide direct evidence regarding the relative roles of positive regulation and Ca-dependent inactivation. Finally, measurements of (Ca2+)i during the recovery from inactivation of ICa will help establish the basis of the oscillatory restitution that occurs during Ca overload. Ca-regulation of Ca channels, while ubiquitous, remains poorly characterized at the most basic level. A clearer understanding of the regulation of Ca channels, as sought by the proposed project, will be of fundamental importance. Such understanding also promises to help elucidate the mechanism of arrhythmias associated with Ca overload states.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Modified Research Career Development Award (K04)
Project #
5K04HL001872-05
Application #
3074134
Study Section
Physiology Study Section (PHY)
Project Start
1986-08-01
Project End
1991-07-31
Budget Start
1990-08-01
Budget End
1991-07-31
Support Year
5
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Kusuoka, H; Marban, E (1992) Cellular mechanisms of myocardial stunning. Annu Rev Physiol 54:243-56
Lawrence, J H; Yue, D T; Rose, W C et al. (1991) Sodium channel inactivation from resting states in guinea-pig ventricular myocytes. J Physiol 443:629-50
Marban, E (1991) Myocardial stunning and hibernation. The physiology behind the colloquialisms. Circulation 83:681-8
Corretti, M C; Koretsune, Y; Kusuoka, H et al. (1991) Glycolytic inhibition and calcium overload as consequences of exogenously generated free radicals in rabbit hearts. J Clin Invest 88:1014-25
Marban, E (1991) Pathogenetic role for calcium in stunning? Cardiovasc Drugs Ther 5:891-3
Koretsune, Y; Corretti, M C; Kusuoka, H et al. (1991) Mechanism of early ischemic contractile failure. Inexcitability, metabolite accumulation, or vascular collapse? Circ Res 68:255-62
Marban, E; Kitakaze, M; Koretsune, Y et al. (1990) Quantification of [Ca2+]i in perfused hearts. Critical evaluation of the 5F-BAPTA and nuclear magnetic resonance method as applied to the study of ischemia and reperfusion. Circ Res 66:1255-67
Cingolani, H E; Koretsune, Y; Marban, E (1990) Recovery of contractility and pHi during respiratory acidosis in ferret hearts: role of Na(+)-H+ exchange. Am J Physiol 259:H843-8
Marban, E; Koretsune, Y (1990) Cell calcium, oncogenes, and hypertrophy. Hypertension 15:652-8
Koretsune, Y; Marban, E (1990) Relative roles of Ca2(+)-dependent and Ca2(+)-independent mechanisms in hypoxic contractile dysfunction. Circulation 82:528-35

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