Circulatory effects of tolazoline and prostacyclin (PGI2) in chronically instrumented lambs.

W H Drummond, B J Williams, I B Webb
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Abstract

We used chronically instrumented, unanesthetized lambs to study the circulatory response to tolazoline and prostacyclin. During normoxia, tolazoline given in ten incremental doses from .01 to 6 mg/kg increased heart rate beginning at 1.1 mg/kg, cardiac output, and PVR/SVR. Systemic vascular resistance (SVR) fell, and pulmonary vascular resistance (PVR) did not change. Tolazoline given during hypoxemia, when basal PVR and heart rate were increased, caused SVR to fall at both 3.3 and 6.6 mg/kg doses, while PVR fell only at 6.6 mg/kg. During hypoxemia, even .01 mg/kg of tolazoline caused tachycardia, but cardiac output rose insignificantly, due to high variability. Prostacyclin given during normoxia caused SVR to fall without change in PVR. A significantly greater fall in SVR occurred when 6.6 micrograms/kg of PGI2 was the first dose given than when the same dose was given later in an incremental titration. Thus, neither drug is a selective pulmonary vasodilator in unanesthetized lambs. Dosing protocol may be important in determining the overall circulatory response to a given drug dose.

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长期使用托唑啉和前列环素(PGI2)对羔羊循环的影响。
我们使用长期使用仪器,未麻醉的羔羊来研究对托唑啉和前列环素的循环反应。在正常缺氧期间,从0.01至6mg /kg的10次增量剂量给药的托唑啉增加了从1.1 mg/kg开始的心率、心输出量和PVR/SVR。全身血管阻力(SVR)下降,肺血管阻力(PVR)无变化。在低氧血症期间,当基础PVR和心率增加时,给予Tolazoline导致3.3和6.6 mg/kg剂量的SVR下降,而PVR仅在6.6 mg/kg时下降。在低氧血症时,即使0.01 mg/kg的托唑啉也会引起心动过速,但心输出量升高不显著,这是由于其高变异性。常氧条件下给予前列环素导致SVR下降,但PVR无变化。当首次给药6.6微克/千克PGI2时,SVR的下降幅度明显大于随后以增量方式给予相同剂量时。因此,这两种药物在未麻醉的羔羊中都不是选择性肺血管扩张剂。给药方案在确定对给定药物剂量的总体循环反应方面可能是重要的。
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