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β受体阻滞剂在慢性心力衰竭管理中的应用。该疾病神经激素模型概念演变中的又一步。

Beta-blockade in the management of chronic heart failure. Another step in the conceptual evolution of a neurohormonal model of the disease.

作者信息

Packer M

机构信息

Division of Circulatory Physiology, Columbia University, College of Physicians and Surgeons, New York, NY, USA.

出版信息

Eur Heart J. 1996 Apr;17 Suppl B:21-3. doi: 10.1093/eurheartj/17.suppl_b.21.

Abstract

Although heart failure has been viewed primarily as a haemodynamic disorder, the development of pharmacologic agents that address the haemodynamic derangements has not proved to be a successful approach to its management. Consequently, attention in recent years has shifted to the development of neurohormonal antagonists in the hope that prolonged interference with the renin-angiotensin system and the sympathetic nervous system would have favourable effects on the natural history of heart failure. Both converting-enzyme inhibitors and beta-adrenergic blockers have been shown to produce long-term haemodynamic and clinical benefits in patients with left ventricular systolic dysfunction in controlled clinical trials. For both classes of drugs, the improvement evolves gradually over several months, although initiation of therapy may be accompanied by undesirable (but usually transient) haemodynamic effects. This pattern of response contrasts sharply with the response pattern seen with direct-acting vasodilators that stimulate neurohormonal systems (e.g. flosequinan). Initiation of treatment with flosequinan produces immediate clinical benefits due to the haemodynamic actions of the drug, but this improvement may disappear within weeks as a result of neurohormonal activation, which also may contribute to the increased risk of death seen during long-term administration of the drug. Recognition of the prognostic importance of neurohormonal activation has led to the hope that long-term treatment with beta-blockers might reduce mortality in heart failure in a manner similar to that seen with converting-enzyme inhibitors. Large-scale, long-term studies are being planned to evaluate this possibility.

摘要

尽管心力衰竭主要被视为一种血流动力学紊乱疾病,但旨在解决血流动力学紊乱问题的药物研发并未被证明是治疗心力衰竭的成功方法。因此,近年来人们的注意力已转向神经激素拮抗剂的研发,希望长期干扰肾素 - 血管紧张素系统和交感神经系统会对心力衰竭的自然病程产生有利影响。在对照临床试验中,血管紧张素转换酶抑制剂和β - 肾上腺素能阻滞剂均已显示对左心室收缩功能障碍患者产生长期血流动力学和临床益处。对于这两类药物,改善效果会在数月内逐渐显现,尽管开始治疗时可能会伴有不良(但通常是短暂的)血流动力学效应。这种反应模式与刺激神经激素系统的直接作用血管扩张剂(如氟司喹南)的反应模式形成鲜明对比。使用氟司喹南开始治疗时,由于药物的血流动力学作用会立即产生临床益处,但这种改善可能会在数周内消失,原因是神经激素激活,这也可能导致长期使用该药物期间死亡风险增加。认识到神经激素激活对预后的重要性,人们希望β受体阻滞剂长期治疗可能会像血管紧张素转换酶抑制剂那样降低心力衰竭患者的死亡率。正在计划进行大规模、长期研究以评估这种可能性。

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