急性静脉注射可卡因会使清醒犬先出现短暂的心脏功能抑制，随后左心室功能增强。

Acute intravenous cocaine causes transient depression followed by enhanced left ventricular function in conscious dogs.

作者信息

Stambler B S, Komamura K, Ihara T, Shannon R P

机构信息

Department of Medicine, Harvard Medical School, Beth Israel Hospital, Boston, Mass.

出版信息

Circulation. 1993 May;87(5):1687-97. doi: 10.1161/01.cir.87.5.1687.

DOI:10.1161/01.cir.87.5.1687

PMID:8491024

Abstract

BACKGROUND

Prior studies in experimental canine models have demonstrated that intravenous cocaine administration causes myocardial depression. The purpose of the present study was to establish the mechanisms of cocaine's actions on myocardial and left ventricular performance after single intravenous bolus doses in conscious, chronically instrumented dogs, in which the full autonomic influences of cocaine would be manifest.

METHODS AND RESULTS

In the intact state, cocaine (1 mg/kg) caused a transient decrease in left ventricular dP/dt (baseline; 3,086 +/- 107 mm Hg/sec; 2.5 minutes, 2,649 +/- 114 mm Hg; p < 0.05) followed by a 25 +/- 4% increase in left ventricular dP/dt that peaked at 15 minutes (left ventricular dP/dt, 3,751 +/- 127 mm Hg/sec, p < 0.01) and remained elevated during the 30-minute period of observation. Both the initial depression and the sustained increase in left ventricular contractile response were dose related. The increase in left ventricular dP/dt persisted under circumstances in which the responses were normalized for changes in heart rate and preload that accompanied cocaine administration. The positive inotropic effects were abolished by full autonomic or selective beta-adrenergic blockades. Finally, both cardiac output (baseline, 2,461 +/- 142 min/mL; peak [5 minutes], 3,434 +/- 218 mL/min; p < 0.05) and left ventricular stroke work (baseline, 39 +/- 5 g.m; peak, 49 +/- 6 g.m; p < 0.05) were increased at all times after cocaine administration, suggesting that pump performance was enhanced, despite early reductions in myocardial contractility. Similarly, indexes of early diastolic filling were enhanced despite transient early prolongation in isovolumic relaxation.

CONCLUSIONS

Acute intravenous cocaine administration (0.1-2 mg/kg) has a biphasic effect on myocardial and left ventricular function with a transient depression followed by significant sustained increases in left ventricular contractility. The results are in keeping with an early local effect followed by significant adrenergic stimulation, which may be obscured by anesthesia or masked by changes in loading conditions.

摘要

背景

先前在实验犬模型中的研究表明，静脉注射可卡因会导致心肌抑制。本研究的目的是确定在清醒、长期植入仪器的犬中单次静脉推注剂量后，可卡因对心肌和左心室功能作用的机制，在这些犬中可卡因的全部自主神经影响将得以体现。

方法与结果

在完整状态下，可卡因（1毫克/千克）导致左心室dp/dt短暂下降（基线值；3,086±107毫米汞柱/秒；2.5分钟时，2,649±114毫米汞柱；p<0.05），随后左心室dp/dt增加25±4%，在15分钟时达到峰值（左心室dp/dt，3,751±127毫米汞柱/秒，p<0.01），并在30分钟观察期内持续升高。左心室收缩反应的初始抑制和持续增加均与剂量相关。在对伴随可卡因给药出现的心率和前负荷变化进行反应标准化的情况下，左心室dp/dt的增加仍然持续。完全自主神经或选择性β-肾上腺素能阻滞消除了正性肌力作用。最后，可卡因给药后所有时间点的心输出量（基线值，2,461±142毫升/分钟；峰值[5分钟]，3,434±218毫升/分钟；p<0.05）和左心室每搏功（基线值，39±5克·米；峰值，49±6克·米；p<0.05）均增加，这表明尽管心肌收缩力早期降低，但泵功能得到增强。同样，尽管等容舒张期短暂早期延长，但早期舒张期充盈指标仍得到增强。