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缺血性心脏病的代谢管理:曲美他嗪的临床数据

Metabolic management of ischemic heart disease: clinical data with trimetazidine.

作者信息

Desideri A, Celegon L

机构信息

Coronary Care Unit and Cardiology Service, S. Giacomo General Hospital, Castelfranco Veneto, Italy.

出版信息

Am J Cardiol. 1998 Sep 3;82(5A):50K-53K. doi: 10.1016/s0002-9149(98)00537-2.

Abstract

The metabolic management of heart disease represents a promising new strategy for ischemic syndromes. This review focuses on the clinical studies performed with trimetazidine, a cellular anti-ischemic agent, either as monotherapy or in combination with other drugs. Acute and chronic administration of trimetazidine significantly increased total work, exercise duration, and time to 1-mm ST segment depression, without any change in heart rate, systolic blood pressure, or rate-pressure product at the same workload, as compared with placebo. Chronic administration studies have been performed comparing the anti-ischemic effects of trimetazidine with nifedipine or propranolol in patients with chronic stable angina. In these studies, the number of anginal attacks was significantly decreased in all groups. Ergometric results showed that trimetazidine increased duration of exercise, time to 1-mm ST segment depression, time to angina, and decreased ST segment depression at peak exercise similarly to propranolol or nifedipine treatment. Rate-pressure product at the same workload remained unchanged in the patients treated with trimetazidine in comparison with baseline treatment, suggesting no effect of the drug on oxygen demand, whereas it was decreased during treatment with nifedipine and propanolol, because of the hemodynamic activity of these drugs. The therapeutic value of adding trimetazidine to either calcium antagonists or beta blockers in patients with ischemic heart disease has also been demonstrated. Unlike classic anti-ischemic agents, treatment with trimetazidine is not accompanied by any modification in hemodynamic parameters, confirming the experimental data showing a unique mechanism of action via a direct effect on the ischemic myocardium.

摘要

心脏病的代谢管理是缺血综合征一种有前景的新策略。本综述聚焦于使用曲美他嗪(一种细胞抗缺血药物)进行的临床研究,该药物既可作为单一疗法,也可与其他药物联合使用。与安慰剂相比,急性和慢性给予曲美他嗪均显著增加了总功、运动持续时间以及出现1毫米ST段压低的时间,而在相同工作量下心率、收缩压或心率-血压乘积无任何变化。已开展慢性给药研究,比较曲美他嗪与硝苯地平或普萘洛尔对慢性稳定型心绞痛患者的抗缺血作用。在这些研究中,所有组的心绞痛发作次数均显著减少。测力计结果显示,曲美他嗪增加运动持续时间、出现1毫米ST段压低的时间、出现心绞痛的时间,并在运动峰值时降低ST段压低,与普萘洛尔或硝苯地平治疗相似。与基线治疗相比,接受曲美他嗪治疗的患者在相同工作量下的心率-血压乘积保持不变,表明该药物对氧需求无影响,而在用硝苯地平和普萘洛尔治疗期间该乘积降低,这是由于这些药物的血流动力学活性。在缺血性心脏病患者中,将曲美他嗪添加到钙拮抗剂或β受体阻滞剂中也已证明具有治疗价值。与经典抗缺血药物不同,曲美他嗪治疗不会伴随血流动力学参数的任何改变,这证实了实验数据显示其通过对缺血心肌的直接作用具有独特的作用机制。

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