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A quantitative analysis of cardiac myocyte relaxation: a simulation study

S. A. Niederer‚ P. J. Hunter and N. P. Smith

Abstract

The determinants of relaxation in cardiac muscle are poorly understood, yet compromised relaxation accompanies various pathologies and impaired pump function. In this study, we develop a model of active contraction to elucidate the relative importance of the [Ca2+]i transient magnitude, the unbinding of Ca2+ from troponin C (TnC), and the length-dependence of tension and Ca2+ sensitivity on relaxation. Using the framework proposed by one of our researchers, we extensively reviewed experimental literature, to quantitatively characterize the binding of Ca2+ to TnC, the kinetics of tropomyosin, the availability of binding sites, and the kinetics of crossbridge binding after perturbations in sarcomere length. Model parameters were determined from multiple experimental results and modalities (skinned and intact preparations) and model results were validated against data from length step, caged Ca2+, isometric twitches, and the half-time to relaxation with increasing sarcomere length experiments. A factorial analysis found that the [Ca2+]i transient and the unbinding of Ca2+ from TnC were the primary determinants of relaxation, with a fivefold greater effect than that of length-dependent maximum tension and twice the effect of tension-dependent binding of Ca2+ to TnC and length-dependent Ca2+ sensitivity. The affects of the [Ca2+]i transient and the unbinding rate of Ca2+ from TnC were tightly coupled with the effect of increasing either factor, depending on the reference [Ca2+]i transient and unbinding rate.

Journal
Biophys J
Keywords
Animals Calcium/*metabolism Calcium Signaling/*physiology Cells‚ Cultured Computer Simulation Elasticity Humans Isometric Contraction/physiology *Models‚ Biological Myocardial Contraction/*physiology Myocytes‚ Cardiac/*physiology Protein Binding Sarcomeres/*physiology Stress‚ Mechanical Troponin C/*metabolism
Note
United Kingdom Wellcome Trust Journal Article Research Support‚ Non−U.S. Gov't United States
Number
5
Pages
1697−722
Volume
90
Year
2006