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A Combined Approach Using Patch-Clamp Study and Computer Simulation Study for Understanding Long QT Syndrome and TdP in Women

机译:运用膜片钳研究和计算机模拟研究相结合的方法来理解女性的长QT综合征和TdP

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摘要

Female sex is an independent risk factor for development of torsade de pointes (TdP)-type arrhythmias in both congenital and acquired long QT syndrome (LQTS). In females, QTc interval and TdP risk vary during the menstrual cycle and around delivery. Biological experiments including single-cell current recordings with the patch-clamp technique and biochemical experiments show that progesterone modulates cardiac K+ current and Ca2+ current via the non-genomic pathway of the progesterone receptor, and thus the cardiac repolarization duration, in a concentration-dependent manner. Incorporation of these biological findings into a computer model of single-cell and coupled-cell cardiomyocytes simulates fluctuations in QTc interval during the menstrual cycle with reasonable accuracy. Based on this model, progesterone is predicted to have protective effects against sympathetic nervous system-induced arrhythmias in congenital LQTS and drug-induced TdP in acquired LQTS. A combined biological and computational approach may provide a powerful means to risk stratify TdP risk in women.
机译:在先天性和后天性长QT综合征(LQTS)中,女性性行为是发生扭转性足尖(TdP)型心律失常的独立危险因素。在女性中,QTc间隔和TdP风险在月经周期和分娩前后有所不同。包括膜片钳技术的单细胞电流记录和生化实验在内的生物学实验表明,孕酮通过非基因组途径调节心脏K + 电流和Ca 2 + 电流孕酮受体的浓度,从而以浓度依赖的方式影响心脏复极化的持续时间。将这些生物学发现整合到单细胞和耦合细胞心肌细胞的计算机模型中,可以以合理的准确性模拟月经周期中QTc间隔的波动。基于该模型,黄体酮有望对先天性LQTS中交感神经系统引起的心律不齐和获得性LQTS中药物引起的TdP具有保护作用。生物学和计算机学相结合的方法可能为将女性的TdP风险分层提供强有力的手段。

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