Stimulus interval-dependent differences in Ca2+ transients and contractile responses of diabetic rat cardiomyocytes

doi:10.1016/S0008-6363(00)00062-6

Cardiovascular Research 2000 46(3):450-462; doi:10.1016/S0008-6363(00)00062-6
© 2000 by European Society of Cardiology

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Stimulus interval-dependent differences in Ca²⁺ transients and contractile responses of diabetic rat cardiomyocytes

George Kotsanas^a^,*, Leanne MD Delbridge^b and Igor R Wendt^a

^aDepartment of Physiology, Monash University, Clayton, Victoria 3168, Australia
^bDepartment of Physiology, University of Melbourne, Parkville, Victoria 3052, Australia

^* Corresponding author. Fax: +61-3-9905-2547 george.kotsanas{at}med.monash.edu.au

Objective: The aim of this study was to gain further insightsinto the consequences of insulin-dependent diabetes mellituson cardiomyocyte calcium handling. Methods: The effects of steadystate and transient changes in stimulus frequency on the intracellularCa²⁺ transient and cell shortening were examined in left ventricularcardiomyocytes isolated from the hearts of control and streptozotocin-induceddiabetic rats. Results: During steady state stimulation diabeticrat cardiomyocytes displayed a slower decay of the Ca²⁺ transientand longer times for maximum cell shortening and re-lengthening.At 1.5 mM extracellular [Ca²⁺], increasing stimulus frequencyover the range 0.2–1.0 Hz led to an increase in restingand peak [Ca²⁺]_i as well as the amplitude of the transient inboth the control and diabetic groups. At frequencies greaterthan 0.4 Hz the amplitude of the transient was significantlydepressed in diabetic rat cells and this was not normalizedby increasing extracellular [Ca²⁺] to 2.5 mM. Recovery of sarcoplasmicreticulum (SR) Ca²⁺ release was measured from the time courseof restitution of the intracellular Ca²⁺ transient. In bothcontrol and diabetic rat cardiomyocytes recovery of the transientoccurred in two phases. In diabetic rat myocytes, the initialrapid phase of restitution at intervals <1 s was markedlyslowed. The fraction of Ca²⁺ recirculating between the SR andthe cytosol was estimated from the decline in amplitude of transientsfollowing post-rest potentiation. There was no difference inthis fraction between control and diabetic rat cells eitherat 1.5 or 2.5 mM extracellular [Ca²⁺]. Conclusion: The bluntedfrequency response of diabetic rat cardiomyocytes at frequenciesgreater than 0.4 Hz is consistent with reduced SR Ca²⁺ uptakeleading to reduced SR Ca²⁺ content and subsequent release. Atstimulus intervals greater than 1 Hz this is likely to be exacerbatedby slower recovery of SR Ca²⁺ release. Despite the evidencefor depressed SR Ca²⁺ uptake, the relative amount of Ca²⁺ recirculatingwithin diabetic rat cardiomyocytes remains unaltered. This ismost likely due to an accompanying reduction in Ca²⁺ effluxfrom the cell due either to depressed Na⁺/Ca²⁺ exchanger activity,or an elevation in intracellular Na⁺ levels.

KEYWORDS Diabetes; Calcium (cellular); Myocytes

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