Cheng E Y, Mazzeo A J, Bosnjak Z J, Coon R L, Kampine J P
Department of Anesthesiology, Medical College of Wisconsin, Milwaukee 53226, USA.
Anesth Analg. 1996 Jul;83(1):162-8. doi: 10.1097/00000539-199607000-00028.
Ketamine, at concentrations achieved with the usual clinical doses, has a direct relaxant effect on airway smooth muscle (ASM). This study investigates the dose-dependent direct relaxation effects of midazolam and propofol on both proximal and distal ASM compared with ketamine. The proximal and distal airways were dissected from eight mongrel dogs and cut into 2-mm rings. The rings were attached to pressure transducers and equilibrated in a Krebs-Ringer bicarbonate bath kept at 37 degrees C, pH 7.4, CO2 37 mm Hg, and PaO2 > 100 mm Hg. Optimal length was determined, a dose-response curve to acetylcholine was established, and the 50% effective dose (ED50) of acetylcholine was calculated. Ketamine, midazolam, or propofol were given in random order to each ring preconstricted with ED50 of acetylcholine in cumulative log incremental doses from 10(-6) to 10(-4) M. Relaxation response was the tension during anesthetic equilibrium, expressed as a percentage of the tension from ED50 of acetylcholine. The drug vehicles were tested for their effects on the ASM. No bronchorelaxation was seen with any of the intravenous anesthetics at 10(-6) M. Ketamine 10(-5) M produced at 17.9% +/- 2.1% relaxation in the distal ASM but had no effect on the proximal ASM. Neither propofol nor midazolam affected the ASM at 10(-5) M. The distal ASM was significantly (P < 0.005) more sensitive to 10(-4) M of all three drugs compared with the proximal ASM. In the proximal ASM, 10(-4) M of ketamine, midazolam and propofol reduced ASM tension by 14.9% +/- 4.4%, 19.0% +/-8.8%, and 14.7% +/- 5.5%, respectively, versus 36.4% +/- 3.2%, 58.6% +/- 6.1%, and 64.4% +/- 9.0% in the distal ASM. The drug vehicles had no effect on the ASM. We conclude that ketamine, midazolam, and propofol have direct relaxant effects on ASM. All three intravenous anesthetics have a greater direct relaxant effect on distal ASM than on proximal ASM. Only ketamine showed significant direct bronchorelaxing effects at concentrations that are likely to be achieved with the usual clinical dosing patterns.
氯胺酮在常规临床剂量所达到的浓度下,对气道平滑肌(ASM)具有直接的松弛作用。本研究调查了与氯胺酮相比,咪达唑仑和丙泊酚对近端和远端ASM的剂量依赖性直接松弛作用。从8只杂种犬身上分离出近端和远端气道,并切成2毫米的环。将这些环连接到压力传感器上,并在温度为37℃、pH值为7.4、二氧化碳分压为37毫米汞柱且动脉血氧分压>100毫米汞柱的 Krebs-Ringer 碳酸氢盐浴中平衡。确定最佳长度,建立对乙酰胆碱的剂量反应曲线,并计算乙酰胆碱的50%有效剂量(ED50)。将氯胺酮、咪达唑仑或丙泊酚以随机顺序给予每个预先用乙酰胆碱的ED50预收缩的环,剂量以对数递增,从10(-6) 到10(-4) M。松弛反应是麻醉平衡期间的张力,以乙酰胆碱ED50引起的张力的百分比表示。测试了药物载体对ASM的影响。在10(-6) M时,任何一种静脉麻醉剂均未观察到支气管舒张作用。10(-5) M的氯胺酮使远端ASM产生17.9%±2.1%的松弛,但对近端ASM无影响。在10(-5) M时,丙泊酚和咪达唑仑均未影响ASM。与近端ASM相比,远端ASM对所有三种药物的10(-4) M浓度均更敏感(P<0.005)。在近端ASM中,10(-4) M的氯胺酮、咪达唑仑和丙泊酚分别使ASM张力降低14.9%±4.4%、19.0%±8.8%和14.7%±5.5%,而在远端ASM中分别为36.4%±3.2%、58.6%±6.1%和64.4%±9.0%。药物载体对ASM无影响。我们得出结论,氯胺酮、咪达唑仑和丙泊酚对ASM具有直接的松弛作用。所有三种静脉麻醉剂对远端ASM的直接松弛作用均大于对近端ASM的作用。只有氯胺酮在常规临床给药模式可能达到的浓度下显示出显著的直接支气管舒张作用。
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