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静脉注射依诺昔酮的临床药理学:心力衰竭患者的药效学和药代动力学

Clinical pharmacology of intravenous enoximone: pharmacodynamics and pharmacokinetics in patients with heart failure.

作者信息

Smith N A, Kates R E, Lebsack C, Ruder M A, Mead R H, Bekele T, Okerholm R A, Rubin G M, Winkle R A

机构信息

Cardiovascular Medicine, Sequoia Hospital, Redwood City, CA.

出版信息

Am Heart J. 1991 Sep;122(3 Pt 1):755-63. doi: 10.1016/0002-8703(91)90522-j.

Abstract

Twenty-one patients with heart failure (New York Heart Association [NYHA] class II to IV) received a 24-hour infusion of enoximone followed by a 12-hour washout period. Patients were randomly assigned to one of four treatment groups. Groups I to III received an 0.5 mg/kg bolus, followed by a maintenance infusion of 2.5, 5.0, or 10.0 micrograms/kg/min. Group IV patients received a maintenance infusion of 5.0 micrograms/kg/min without a loading dose. Serial assessment of hemodynamics, plasma levels of enoximone and enoximone sulfoxide, and ventricular ectopy were performed. Enoximone produced a clinically significant increase in cardiac index, and a decrease in mean pulmonary artery wedge pressure and systemic vascular resistance in all groups. Enoximone mildly increased heart rate, and had a minimal effect on mean arterial pressure. There was no statistically significant change in ventricular ectopy during the infusion. Significant hemodynamic improvement was noted at even the lowest infusion rate, and did not increase in linear fashion at higher infusion rates. In patients who did not receive an initial loading bolus of 0.5 mg/kg, the increase in cardiac index was delayed by approximately 1 hour. Plasma concentrations of both enoximone and its major metabolite continued to rise throughout the 24-hour infusion in group III (10.0 micrograms/kg/min), rather than reaching steady state as predicted by the terminal exponential half-lives of these compounds. This is suggestive of nonlinear pharmacokinetics and indicates a potential for excessive accumulation of enoximone and its metabolite during prolonged infusion. These findings may have important implications in guiding the intravenous administration of enoximone.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

21例心力衰竭患者(纽约心脏协会[NYHA] II至IV级)接受依诺昔酮24小时静脉输注,随后有12小时的洗脱期。患者被随机分配到四个治疗组之一。第一组至第三组先给予0.5mg/kg的负荷剂量,随后分别以2.5、5.0或10.0微克/千克/分钟的速度持续输注。第四组患者不给予负荷剂量,仅以5.0微克/千克/分钟的速度持续输注。对血流动力学、依诺昔酮和依诺昔酮亚砜的血浆水平以及室性异位搏动进行了连续评估。依诺昔酮使所有组的心脏指数出现临床上显著升高,平均肺动脉楔压和全身血管阻力降低。依诺昔酮使心率轻度增加,对平均动脉压影响极小。输注期间室性异位搏动无统计学显著变化。即使在最低输注速度下也观察到显著的血流动力学改善,且在较高输注速度下并非呈线性增加。未接受0.5mg/kg初始负荷剂量的患者,心脏指数的增加延迟约1小时。在第三组(10.0微克/千克/分钟)中,依诺昔酮及其主要代谢产物的血浆浓度在24小时输注过程中持续升高,而非如这些化合物的终末指数半衰期所预测的那样达到稳态。这提示存在非线性药代动力学,表明依诺昔酮及其代谢产物在长时间输注期间可能过度蓄积。这些发现可能对指导依诺昔酮的静脉给药具有重要意义。(摘要截选至250字)

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