Cellular calcium handling and electrophysiology are modulated by chronic physiological pacing in human induced pluripotent stem cell-derived cardiomyocytes

电生理学 农奴 内科学 电流钳 舒张期 诱导多能干细胞 化学 膜片钳 医学 血压 胚胎干细胞 生物化学 基因 ATP酶
作者
Maria Knierim,Thea Bommer,Michael Paulus,Dominic Riedl,Sarah Fink,Arnold Pöppl,Florian Reetz,Peter Wang,Lars S. Maier,Niels Voigt,Matthias Nahrendorf,Samuel Sossalla,Katrin Streckfuß‐Bömeke,Steffen Pabel
出处
期刊:American Journal of Physiology-heart and Circulatory Physiology [American Physiological Society]
标识
DOI:10.1152/ajpheart.00536.2024
摘要

Electric pacing of human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CM) has been increasingly used to simulate cardiac arrhythmias in vitro and to enhance cardiomyocyte maturity. However, the impact of electric pacing on cellular electrophysiology and Ca 2+ -handling in differentiated hiPSC-CM is less characterized. Here we studied the effects of electric pacing for 24h or 7d at a physiological rate of 60 bpm on cellular electrophysiology and Ca 2+ -cycling in late-stage, differentiated hiPSC-CM (>90% troponin + , >60d post differentiation). Electric culture pacing for 7d did not influence cardiomyocyte cell size, apoptosis or generation of reactive oxygen species in differentiated hiPSC-CM compared to 24h pacing. However, epifluorescence measurements revealed that electric pacing for 7d improved systolic Ca 2+ -transient amplitude and Ca 2+ -transient upstroke, which could be explained by elevated sarcoplasmic reticulum Ca 2+ -load and SERCA activity. Diastolic Ca 2+ -leak was not changed in line-scanning confocal microscopy suggesting that the improvement in systolic Ca 2+ -release was not associated with a higher open probability of RyR2 during diastole. While bulk cytosolic Na + -concentration and NCX activity were not changed, patch-clamp studies revealed that chronic pacing caused a slight abbreviation of the action potential duration (APD) in hiPSC-CM. We found in whole-cell voltage-clamp measurements that chronic pacing for 7d led to a decrease in late Na + -current, which might explain the changes in APD. In conclusion, our results show that chronic pacing improves systolic Ca 2+ -handling and modulates the electrophysiology of late-stage, differentiated iPSC-CM. This study might help to understand the effects of electric pacing and its numerous applications in stem cell research including arrhythmia simulation.
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