Mechanisms of beat-to-beat regulation of cardiac pacemaker cell function by Ca²⁺ cycling dynamics.
نویسندگان
چکیده
Whether intracellular Ca(2+) cycling dynamics regulate cardiac pacemaker cell function on a beat-to-beat basis remains unknown. Here we show that under physiological conditions, application of low concentrations of caffeine (2-4 mM) to isolated single rabbit sinoatrial node cells acutely reduces their spontaneous action potential cycle length (CL) and increases Ca(2+) transient amplitude for several cycles. Numerical simulations, using a modified Maltsev-Lakatta coupled-clock model, faithfully reproduced these effects, and also the effects of CL prolongation and dysrhythmic spontaneous beating (produced by cytosolic Ca(2+) buffering) and an acute CL reduction (produced by flash-induced Ca(2+) release from a caged Ca(2+) buffer), which we had reported previously. Three contemporary numerical models (including the original Maltsev-Lakatta model) failed to reproduce the experimental results. In our proposed new model, Ca(2+) releases acutely change the CL via activation of the Na(+)/Ca(2+) exchanger current. Time-dependent CL reductions after flash-induced Ca(2+) releases (the memory effect) are linked to changes in Ca(2+) available for pumping into sarcoplasmic reticulum which, in turn, changes the sarcoplasmic reticulum Ca(2+) load, diastolic Ca(2+) releases, and Na(+)/Ca(2+) exchanger current. These results support the idea that Ca(2+) regulates CL in cardiac pacemaker cells on a beat-to-beat basis, and suggest a more realistic numerical mechanism of this regulation.
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متن کاملLetter to the editor: “Validating the requirement for beat-to-beat coupling of the Ca clock and M clock in pacemaker cell normal automaticity”
TO THE EDITOR: A novel, general concept of a coupled-clock pacemaker cell system of surface membrane electrogenic proteins that function as a voltage oscillator (M clock) and of intracellular proteins that effect diastolic submembrane Ca oscillations (Ca clock) has been recently put forth (5). The essence of the “yin-yang”-type dynamic coupling of the clocks is based on, in part, several lines ...
متن کاملLetter to the editor: "Validating the requirement for beat-to-beat coupling of the Ca2+ clock and M clock in pacemaker cell normal automaticity".
TO THE EDITOR: A novel, general concept of a coupled-clock pacemaker cell system of surface membrane electrogenic proteins that function as a voltage oscillator (M clock) and of intracellular proteins that effect diastolic submembrane Ca oscillations (Ca clock) has been recently put forth (5). The essence of the “yin-yang”-type dynamic coupling of the clocks is based on, in part, several lines ...
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Cardiac electrical dynamics are governed by cellular-level properties, such as action potential duration (APD) restitution and intracellular calcium (Ca) handling, and tissue-level properties, including conduction velocity restitution and cell-cell coupling. Irregular dynamics at the cellular level can lead to instabilities in cardiac tissue, including alternans, a beat-to-beat alternation in t...
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عنوان ژورنال:
- Biophysical journal
دوره 105 7 شماره
صفحات -
تاریخ انتشار 2013