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冠状动脉逆行灌注的药代动力学分析:以美托洛尔为示踪剂与冠状动脉顺行给药的比较。

Pharmacokinetic analysis of coronary venous retroinfusion: a comparison with anterograde coronary artery drug administration using metoprolol as a tracer.

作者信息

Rydén L, Tadokoro H, Sjöquist P O, Regardh C, Kobayashi S, Corday E, Drury J K

机构信息

Department of Medicine, Cedars-Sinai Medical Center, Los Angeles, California.

出版信息

J Am Coll Cardiol. 1991 Aug;18(2):603-12. doi: 10.1016/0735-1097(91)90620-o.

Abstract

Plasma and myocardial tissue concentrations of metoprolol were studied in ischemic and nonischemic areas of 22 pigs after 90 (n = 19) and 16 (n = 3) min of left anterior descending coronary artery occlusion. Group A (n = 6) received simultaneous intravenous metoprolol (0.2 mg/kg body weight) and tritium-labeled (3H)-metoprolol (0.2 mg/kg) retrogradely into the coronary vein. In group B (n = 5), metoprolol and 3H-metoprolol were administered in the same way, but at half the volume to study the influence of derived coronary venous pressure on the myocardial concentration of drug. In group C (n = 3), metoprolol was given retrogradely and saline solution was infused into the left anterior descending artery before induced death to wash out metoprolol from the coronary veins. To rule out a possible influence of the development of myocardial necrosis on drug distribution, metoprolol was retroinfused after 1 min of arterial occlusion in three pigs (group D). In group E (n = 5), metoprolol (0.2 mg/kg) was infused anterogradely into the left anterior descending artery. Peak plasma concentration was significantly higher after intravenous infusion of metoprolol (1,188 +/- 503 nmol/liter) than after coronary venous infusion (417 +/- 155 nmol/liter; p less than 0.001). In groups A and B, the nonischemic myocardial concentration of metoprolol was 250 to 300 pmol/g, whether the drug was infused intravenously or into the coronary vein. Coronary venous retroinfusion, however, resulted in a substantial accumulation of metoprolol in the ischemic myocardium. In group A pigs, subendocardial myocardial concentration was 16,800 +/- 7,774, mid-myocardial 39,590 +/- 18,043 and subepicardial 57,143 +/- 29,030 pmol/g (mean +/- SE). The ischemic myocardial concentration in pigs from group B was somewhat less pronounced, probably secondary to a lower coronary venous pressure (15 +/- 3 mm Hg) with the lower volume of infusion (6.1 +/- 0.3 ml) in group B compared with 32 +/- 5 mm Hg with a 14 +/- 1 ml infusion in group A. Coronary artery anterograde administration resulted in myocardial ischemic and nonischemic zone drug concentrations similar to those observed after retroinfusion into the coronary vein. With both modes of administration, there was a transmyocardial gradient from a somewhat lower drug concentration in the subendocardium, toward an increasing level in the mid-myocardium, to the highest concentration in the subepicardial zone of the ischemic myocardium. Coronary venous retroinfusion resulted in pronounced drug accumulation in the ischemic myocardium. The derived coronary venous pressure during infusion influenced the concentration of drug.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在22头猪的左前降支冠状动脉闭塞90分钟(n = 19)和16分钟(n = 3)后,研究了美托洛尔在缺血和非缺血区域的血浆及心肌组织浓度。A组(n = 6)同时静脉注射美托洛尔(0.2 mg/kg体重)和将氚标记的(³H)-美托洛尔(0.2 mg/kg)逆行注入冠状静脉。B组(n = 5)以相同方式给药,但体积减半,以研究冠状静脉衍生压力对心肌药物浓度的影响。C组(n = 3)在诱导死亡前将美托洛尔逆行注入,同时将生理盐水注入左前降支动脉以从冠状静脉中冲洗出美托洛尔。为排除心肌坏死发展对药物分布的可能影响,在3头猪(D组)动脉闭塞1分钟后逆行注入美托洛尔。E组(n = 5)将美托洛尔(0.2 mg/kg)顺行注入左前降支动脉。静脉注射美托洛尔后的血浆峰值浓度(1,188 ± 503 nmol/升)显著高于冠状静脉注射后的浓度(417 ± 155 nmol/升;p < 0.001)。在A组和B组中,无论药物是静脉注射还是注入冠状静脉,美托洛尔在非缺血心肌中的浓度均为250至300 pmol/g。然而,冠状静脉逆行注入导致美托洛尔在缺血心肌中大量蓄积。在A组猪中,心内膜下心肌浓度为16,800 ± 7,774、心肌中层为39,590 ± 18,043、心外膜下为57,143 ± 29,030 pmol/g(均值 ± 标准误)。B组猪的缺血心肌浓度稍低,可能是由于B组较低的冠状静脉压力(15 ± 3 mmHg)以及较低的注入体积(6.1 ± 0.3 ml),而A组的压力为32 ± 5 mmHg,注入体积为14 ± 1 ml。冠状动脉顺行给药导致心肌缺血和非缺血区域的药物浓度与冠状静脉逆行注入后观察到的相似。两种给药方式下,均存在跨心肌梯度,即心内膜下药物浓度略低,心肌中层浓度逐渐升高,至缺血心肌心外膜下区域浓度最高。冠状静脉逆行注入导致美托洛尔在缺血心肌中显著蓄积。注入过程中衍生的冠状静脉压力影响药物浓度。(摘要截断于400字)

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