Clinical Pharmacology of If Current Inhibition

Heartdrug : excellence in cardiovascular trials Pub Date : 2005-02-07 DOI:10.1159/000083382

V. Benatar, G. Lerebours Pigeonnière, Patricia Nury-Philémon

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Abstract

Elevated resting heart rate is linked to an increase in both cardiovascular and all-cause mortality, and agents that reduce heart rate have obvious applications in improving the prognosis of coronary artery disease and heart failure. In this short review, we examine the pathophysiological grounds for the original clinical benefits of pure heart rate lowering through the development of a new class of heart-rate-reducing agents. Ivabradine, a novel selective and specific inhibitor of the If pacemaker current in the sinoatrial node cells, is the prototype of this pharmacological class. It has shown anti-ischemic and antianginal efficacy superior to placebo and comparable to β-blockers and calcium channel blockers. In early clinical pharmacological studies, ivabradine was shown to reduce heart rate in a dose-dependent manner without modifying other cardiac parameters such as conduction, contractility, and ventricular repolarization. Ivabradine improves myocardial oxygen delivery and decreases oxygen consumption. Together, these properties make ivabradine a valuable alternative to existing drug therapies for stable angina and other myocardial conditions.

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If电流抑制的临床药理学

静息心率升高与心血管和全因死亡率的增加有关，降低心率的药物在改善冠状动脉疾病和心力衰竭的预后方面有明显的应用。在这篇简短的综述中，我们通过开发一种新型的降心率药物来研究纯降心率最初的临床益处的病理生理学依据。伊伐布雷定是一种新型的选择性和特异性窦房结细胞If起搏器电流抑制剂，是这类药物的原型。它的抗缺血和抗心绞痛疗效优于安慰剂，与β受体阻滞剂和钙通道阻滞剂相当。在早期的临床药理学研究中，伊伐布雷定显示出以剂量依赖的方式降低心率，而不改变其他心脏参数，如传导、收缩力和心室复极。伊伐布雷定改善心肌供氧，减少耗氧量。总之，这些特性使伊伐布雷定成为稳定型心绞痛和其他心肌疾病的现有药物治疗的有价值的替代品。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Heartdrug : excellence in cardiovascular trials

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