Mechanisms of length history-dependent tension in an ionic model of the cardiac myocyte

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MODELING IN PHYSIOLOGY
Mechanisms of length history-dependent tension in an ionic model of the cardiac myocyte

Wolfgang F. Bluhm¹, Wilbur Y. W. Lew¹^,², Alan Garfinkel³, and Andrew D. McCulloch⁴

Departments of ¹ Medicine and ⁴ Bioengineering, University of California, San Diego, La Jolla 92093; ² Cardiology Division, Department of Veterans Affairs Medical Center, San Diego 92161; and ³ Departments of Physiological Science and Medicine (Cardiology), University of California, Los Angeles, Los Angeles, California 90024

The ionic model of the ventricular myocyte developed by Luo and Rudy (Circ. Res. 74: 1071-1096, 1994) was used to investigatepotential mechanisms of the slow changes in stress (SCS) thatfollow step changes in muscle length. A step change in myofilamentsensitivity alone caused an immediate increase in active tension,but no SCS. The effects of additional step changes in the parametersof sarcolemmal ion fluxes were examined for each ion flux in themodel. Changes in the coefficients of Ca²⁺ or K⁺ channels did not produce SCS. SCS was produced by step changesin parameters of the Na⁺-K⁺ pump or the Na⁺ leak current. This simulated mechanism was mediated through aslow increase in intracellular Na⁺ concentration and a resulting increase in systolic Ca²⁺ entry through the Na⁺/Ca²⁺ exchanger. The model reproduced the effects of several experimentalinterventions such as sarcoplasmic reticulum Ca²⁺ depletion, "diastolic" length changes, and changes in extracellularCa²⁺. Thus SCS in cardiac muscle may be caused by length-induced changesin sarcolemmal Na⁺ fluxes.

myocardial contraction; calcium; sodium

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MODELING IN PHYSIOLOGY Mechanisms of length history-dependent tension in an ionic model of the cardiac myocyte

MODELING IN PHYSIOLOGY
Mechanisms of length history-dependent tension in an ionic model of the cardiac myocyte