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New antiarrhythmic drugs for treatment of atrial fibrillation.

机译:新的抗心律失常药物治疗房颤。

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摘要

Inadequacies in current therapies for atrial fibrillation have made new drug development crucial. Conventional antiarrhythmic drugs increase the risk of ventricular proarrhythmia. In drug development, the focus has been on favourable multichannel-blocking profiles, atrial-specific ion-channels, and novel non-channel targets (upstream therapy). Molecular modification of the highly effective multichannel blocker, amiodarone, to improve safety and tolerability has produced promising analogues such as dronedarone, although this drug seems less effective than does amiodarone. Vernakalant, an atrial-selective drug with reduced proarrhythmic risk, might be useful for cardioversion in atrial fibrillation. Ranolazine, another atrial-selective agent initially developed as an antianginal, has efficacy for atrial fibrillation and is being tested in prospective clinical trials. So-called upstream therapy with angiotensin-converting enzyme and angiotensin-receptor inhibitors, statins, or omega-3 fatty acids and fish oil that target atrial remodelling could be effective, but need further clinical validation. We focus on the basic and clinical pharmacology of newly emerging antiarrhythmic drugs and non-traditional approaches such as upstream therapy for atrial fibrillation.
机译:目前房颤治疗的不足使新药开发变得至关重要。常规抗心律不齐药物会增加室性心律失常的风险。在药物开发中,重点一直放在有利的多通道阻滞曲线,心房特异性离子通道和新型非通道靶点(上游治疗)上。高效多通道阻滞剂胺碘酮的分子修饰可提高安全性和耐受性,产生了有前途的类似物,如决奈达隆,尽管这种药物似乎不如胺碘酮有效。 Vernakalant是一种降低心律失常风险的心房选择性药物,可能对房颤的心脏复律有用。雷诺嗪是另一种最初作为抗心绞痛药物开发的心房选择性药物,具有房颤有效的功效,目前正在前瞻性临床试验中进行测试。使用血管紧张素转换酶和血管紧张素受体抑制剂,他汀类药物或omega-3脂肪酸和鱼油靶向房重构的所谓上游疗法可能是有效的,但需要进一步的临床验证。我们专注于新兴抗心律不齐药物的基础和临床药理学以及非传统方法,例如房颤的上游治疗。

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  • 来源
    《The Lancet》 |2010年第9721期|共12页
  • 作者

    Dobrev D; Nattel S;

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