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磷酸二酯酶III抑制剂:长期风险与短期益处

Phosphodiesterase III inhibitors: long-term risks and short-term benefits.

作者信息

Cruickshank J M

机构信息

Royal Brompton National Heart and Lung Hospital, London, UK.

出版信息

Cardiovasc Drugs Ther. 1993 Aug;7(4):655-60. doi: 10.1007/BF00877818.

Abstract

Heart failure is now viewed as a disorder of the circulation, not merely the heart, which becomes manifest only when certain compensatory mechanisms break down. After treatment with diuretics, the two main strategies in treating heart failure involve decreasing the work of the heart by vasodilatation or increasing ventricular contractility by positive inotropic agents. It is now apparent, however, that the resulting hemodynamic benefit need not equate with long-term clinical improvement or increased longevity; indeed, the reverse can be true. Inhibitors of phosphodiesterase III, which is specific for the breakdown of cyclic adenosine monophosphate (cAMP), produce useful hemodynamic effects following intravenous and oral dosing, but have not fulfilled their initial promise in the chronic oral treatment of heart failure patients. The reason for reduced survival in the long-term studies of milrinone is not clear, but cardiac arrhythmias, possibly resulting from the increased intracellular levels of cAMP, may be responsible. However, intravenous usage may not suffer from the same limitations as chronic oral dosing. Short-term intravenous administration produces the expected beneficial hemodynamic effects of positive inotropism and vasodilatation. Though infusions of milrinone have been shown to enhance atrioventricular conduction in some, but not all, studies, there appears to be no significant increase in ventricular premature contractions, or ventricular or sustained tachyarrhythmias. Because milrinone does not have a significant adverse effect on His-Purkinje conduction, its use should be well tolerated in patients with intraventricular conduction disturbances. However, accurate assessment of the mortality risk and benefit of short-term intravenous treatment remains to be made in sufficiently powerful prospective, randomized controlled studies.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

心力衰竭现在被视为一种循环系统疾病,而不仅仅是心脏疾病,只有当某些代偿机制失效时才会显现出来。使用利尿剂治疗后,治疗心力衰竭的两种主要策略包括通过血管扩张减少心脏做功,或使用正性肌力药物增加心室收缩力。然而,现在很明显,由此产生的血流动力学益处不一定等同于长期临床改善或延长寿命;事实上,情况可能相反。磷酸二酯酶III特异性负责环磷酸腺苷(cAMP)的分解,其抑制剂在静脉和口服给药后可产生有益的血流动力学效应,但在心力衰竭患者的长期口服治疗中并未达到最初的预期。米力农长期研究中生存率降低的原因尚不清楚,但可能由细胞内cAMP水平升高导致的心律失常可能是原因所在。然而,静脉使用可能不会受到与长期口服给药相同的限制。短期静脉给药可产生预期的有益血流动力学效应,即正性肌力作用和血管扩张。尽管在一些(但不是所有)研究中,米力农输注已被证明可增强房室传导,但室性早搏、室性或持续性快速心律失常似乎没有显著增加。由于米力农对希氏-浦肯野传导没有显著不良影响,因此在有室内传导障碍的患者中使用应能很好耐受。然而,仍有待在足够有力的前瞻性随机对照研究中对短期静脉治疗的死亡风险和益处进行准确评估。(摘要截选至250字)

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