Mager G, Klocke R K, Kux A, Höpp H W, Hilger H H
Klinik III für Innere Medizin, Universität zu Köln, Federal Republic of Germany.
Am Heart J. 1991 Jun;121(6 Pt 2):1974-83. doi: 10.1016/0002-8703(91)90834-5.
High levels of endogenous plasma catecholamines in patients with severe congestive heart failure induce a down-regulation of the myocardial beta-adrenoreceptors and thus cause adrenoreceptor agonists, such as dobutamine, to be less effective in the treatment of these patients. Phosphodiesterase III inhibitors work independent of adrenoreceptor activity and plasma catecholamine levels; thus these agents are likely to be more effective in the treatment of severe heart failure. The present study compares both the initial and late hemodynamic effects of dobutamine and milrinone during sequentially administered 24-hour infusions. Twenty patients with severe heart failure (New York Heart Association class III, n = 4; New York Heart Association class IV, n = 16) were investigated. Dobutamine could be administered at the prescribed maximum dose of 15 micrograms/kg/min for 24 hours in only 15 of 20 patients. In three patients the dose was reduced or dobutamine infusion completely stopped because of a drug-related increase in heart rate greater than 140 beats/min. Another 2 of 20 patients showed no hemodynamic improvement over 3 hours at the maximum dose of 15 micrograms/kg/min. Dobutamine administration was also discontinued in these patients on account of the existing unfavorable hemodynamic condition, and therapy with intravenous milrinone was started. All 20 patients responded to milrinone without side effects, although comparison of the hemodynamic effects during a 24-hour infusion was possible in only 15 patients. The 15 patients studied over both observation periods experienced an increase in heart rate from 88.8 to 105.6 beats/min (+ 1 hour; p less than or equal to 0.001) when receiving dobutamine but had no increase with milrinone. Stroke volume increased during dobutamine infusion from 19.3 to 28.9 ml/m2 (+49.6%) after 1 hour and then fell continuously to 25.2 ml/m2 after 12 hours; during milrinone therapy, stroke volume increased from 18.8 to 31.2 ml/m2 (+66%; p less than or equal to 0.001) and remained at this level until the end of the infusion (30.2 ml/m2). Pulmonary capillary wedge pressure (PCWP) decreased (p less than or equal to 0.001) immediately during milrinone therapy from 26.5 to 16.2 mm Hg after 30 minutes and stabilized at 20.1 mm Hg after 24 hours. During dobutamine infusion PCWP showed a delayed decrease from 27.8 to 19.0 mm Hg after 6 hours and subsequently rose to 22.7 mm Hg after 24 hours.(ABSTRACT TRUNCATED AT 400 WORDS)
重度充血性心力衰竭患者体内高水平的内源性血浆儿茶酚胺会导致心肌β - 肾上腺素能受体下调,从而使肾上腺素能受体激动剂(如多巴酚丁胺)在治疗这些患者时效果降低。磷酸二酯酶III抑制剂的作用独立于肾上腺素能受体活性和血浆儿茶酚胺水平;因此,这些药物在治疗重度心力衰竭时可能更有效。本研究比较了多巴酚丁胺和米力农在连续24小时输注过程中的初始和晚期血流动力学效应。对20例重度心力衰竭患者(纽约心脏协会III级,4例;纽约心脏协会IV级,16例)进行了研究。20例患者中只有15例能够以规定的最大剂量15微克/千克/分钟给予多巴酚丁胺24小时。3例患者因药物相关的心率增加超过140次/分钟而减少剂量或完全停止多巴酚丁胺输注。另外20例患者中有2例在最大剂量15微克/千克/分钟下3小时内血流动力学无改善。由于存在不利的血流动力学状况,这些患者也停止了多巴酚丁胺治疗,并开始静脉注射米力农治疗。所有20例患者对米力农均有反应且无副作用,尽管仅15例患者能够进行24小时输注期间的血流动力学效应比较。在两个观察期均接受研究的15例患者在接受多巴酚丁胺时心率从88.8次/分钟增加到105.6次/分钟(+1小时;p≤0.001),而接受米力农时心率无增加。多巴酚丁胺输注期间,每搏量在1小时后从19.3毫升/平方米增加到28.9毫升/平方米(+49.6%),然后在12小时后持续下降至25.2毫升/平方米;在米力农治疗期间,每搏量从18.8毫升/平方米增加到31.2毫升/平方米(+66%;p≤0.001),并在输注结束时(30.2毫升/平方米)保持在该水平。米力农治疗期间,肺毛细血管楔压(PCWP)在30分钟后立即从26.5毫米汞柱降至16.2毫米汞柱(p≤0.001),并在24小时后稳定在20.1毫米汞柱。多巴酚丁胺输注期间,PCWP在6小时后延迟从27.8毫米汞柱降至19.0毫米汞柱,随后在24小时后升至22.7毫米汞柱。(摘要截取自400字)
