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通过 I(f)-通道抑制来降低心率及其在射血分数降低和保留的心衰中的潜在作用。

Heart rate reduction by I(f)-channel inhibition and its potential role in heart failure with reduced and preserved ejection fraction.

机构信息

Klinik für Innere Medizin III, University of the Saarland, Homburg Saar, Germany.

出版信息

Trends Cardiovasc Med. 2009 Jul;19(5):152-7. doi: 10.1016/j.tcm.2009.09.002.

Abstract

Selective heart rate (HR) reduction by I(f)-channel inhibition is a recently developed pharmacological principle in cardiovascular therapy. Among these newly identified HR-lowering drugs, only ivabradine has now become approved for clinical use. I(f)-channel inhibition mainly reduces HR, thereby improving myocardial oxygen supply, energy balance, and cardiac function. Ivabradine was well tolerated and revealed a good safety profile in the investigated study populations. The guiding experimental and clinical results of I(f)-channel inhibition were compared to those of beta-blockade as a HR reducing principle as well as cornerstone of heart failure standard therapy. Beside its use in therapy of coronary artery disease, I(f)-channel inhibition potentially exhibits beneficial effects in systolic and diastolic heart failure as well. Therefore, hemodynamic effects of ivabradine and its limitations in heart failure together with the biological impact of HR reduction will be considered in this context. Because no clinical data with specific heart-rate-reducing agents are available in heart failure patients until now, the prospective significance of I(f)-channel inhibition can only be speculated on. However, the presented results and considerations are encouraging: ivabradine may play a therapeutic role in the future protecting left ventricular function and structure from early deterioration in heart failure with reduced and preserved ventricular ejection fraction.

摘要

选择性心率(HR)降低通过 I(f)通道抑制是心血管治疗中最近开发的药理学原则。在这些新鉴定的降低心率药物中,只有伊伐布雷定现已被批准用于临床使用。I(f)通道抑制主要降低心率,从而改善心肌供氧、能量平衡和心功能。伊伐布雷定在研究人群中具有良好的耐受性和安全性。I(f)通道抑制的指导实验和临床结果与β阻断作为降低心率的原则以及心力衰竭标准治疗的基石进行了比较。除了在冠状动脉疾病的治疗中使用外,I(f)通道抑制在收缩性和舒张性心力衰竭中也可能具有有益的作用。因此,将在此背景下考虑伊伐布雷定的血液动力学效应及其在心力衰竭中的局限性以及心率降低的生物学影响。由于迄今为止心力衰竭患者中尚无具有特定心率降低作用的药物的临床数据,因此只能推测 I(f)通道抑制的前瞻性意义。然而,所呈现的结果和考虑因素令人鼓舞:伊伐布雷定可能在未来发挥治疗作用,保护左心室功能和结构免受射血分数降低和保留的心力衰竭中早期恶化。

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