Shen Y T, Wiedmann R T, Greenland B D, Lynch J J, Grossman W
Department of Pharmacology, Merck Research Laboratories, West Point, Pennsylvania 19486, USA.
Cardiovasc Res. 1998 Aug;39(2):413-22. doi: 10.1016/s0008-6363(98)00117-5.
The goal of this study was to determine if the hemodynamic effects of the combined administration of an angiotensin converting enzyme (ACE) inhibitor and angiotensin II type 1 (AT1) receptor antagonist are greater than those produced by either of these agents administered individually during heart failure.
Ten farm pigs were chronically instrumented with aortic, left atrial and right atrial catheters, a left ventricular (LV) pressure gauge, LV dimension crystals, coronary occluders, an ascending aortic flow probe and pacing leads. Heart failure was induced by serial myocardial infarctions followed by repeated rapid ventricular pacing.
Heart failure was manifested by significant (p < 0.01) decreases in LV dP/dt (-38 +/- 5%, from 2943 +/- 107 mmHg/s) and cardiac output (-27 +/- 4%, from 4.1 +/- 0.2 l/min) and increases in left atrial pressure (+18 +/- 1 mmHg, from 4 +/- 1 mmHg) and total peripheral resistance (TPR)(+40 +/- 8%, from 23 +/- 2 mmHg/l/min). The effects of an ACE inhibitor (enalaprilat) and an AT1 receptor antagonist (L-158,809), administered in maximally effective doses, either individually or concomitantly, were examined on different days in conscious pigs with heart failure. There were no differences in any of the baseline hemodynamic measurements among the groups studied. Thirty minutes after administration, enalaprilat (4 mg/kg i.v.) increased (p < 0.05) cardiac output by 8 +/- 2% and reduced (p < 0.05) mean arterial pressure and TPR by 5 +/- 1 and 12 +/- 1%, respectively, while the changes in LV dP/dt (0 +/- 2%), LV fractional shortening (+4 +/- 3%) and heart rate (+1 +/- 1%) were not statistically significant. Similarly, L-158,809 (4 mg/kg, i.v.) increased cardiac output by 9 +/- 2% and reduced mean arterial pressure and TPR by 4 +/- 1 and 11 +/- 3%, respectively, while the changes in LV dP/dt (+3 +/- 3%), LV fractional shortening (+3 +/- 1%) and heart rate (0 +/- 1%) were not significant. However, enalaprilat (1 mg/kg, i.v.) and L-158,809 (1 mg/kg, i.v.), administered concomitantly, reduced TPR by 21 +/- 3%, an effect greater (p < 0.05) than when either of these agents was administered individually at a dose of 4 mg/kg, i.v. The changes in mean arterial pressure (-9 +/- 2%), cardiac output (+15 +/- 4%) and LV fractional shortening (+11 +/- 3%) also tended to be greater with concomitant administration. In addition, in a sequential dosing protocol, when L-158,809 (1 mg/kg, i.v.) was administered 30 min after enalaprilat (1 mg/kg, i.v.), TPR was reduced by 20 +/- 4% compared to only a 6 +/- 3% reduction (p < 0.05) when the enalaprilat was followed 30 min later by a second dose of enalaprilat (1 mg/kg, i.v.). The changes in mean arterial pressure and cardiac output for the combined treatment group also tended to be greater than those for the group given two sequential doses of enalaprilat.
In conscious pigs with heart failure, the combined vasodilatory effects of an ACE inhibitor and AT1 receptor antagonist are greater than those produced when only one of these agents is administered, suggesting that independent mechanisms of ACE inhibition and AT1 receptor antagonism could be partly responsible for the improved vascular dynamics during heart failure.
本研究的目的是确定在心力衰竭期间,联合使用血管紧张素转换酶(ACE)抑制剂和1型血管紧张素II(AT1)受体拮抗剂的血流动力学效应是否大于单独使用这两种药物中的任何一种所产生的效应。
十头农场猪长期植入主动脉、左心房和右心房导管、左心室(LV)压力计、LV尺寸晶体、冠状动脉闭塞器、升主动脉血流探头和起搏导线。通过连续心肌梗死随后反复快速心室起搏诱导心力衰竭。
心力衰竭表现为LV dP/dt显著降低(p < 0.01)(从2943 ± 107 mmHg/s降至-38 ± 5%)、心输出量显著降低(p < 0.01)(从4.1 ± 0.2 l/min降至-27 ± 4%)、左心房压力升高(从4 ± 1 mmHg升至+18 ± 1 mmHg)和总外周阻力(TPR)升高(从23 ± 2 mmHg/l/min升至+40 ± 8%)。在不同日期,对清醒的心力衰竭猪分别或联合给予最大有效剂量的ACE抑制剂(依那普利拉)和AT1受体拮抗剂(L-158,809),并观察其效应。研究的各组之间在任何基线血流动力学测量方面均无差异。给药后30分钟,依那普利拉(4 mg/kg静脉注射)使心输出量增加(p < 0.05)8 ± 2%,使平均动脉压和TPR分别降低(p < 0.05)5 ± 1%和12 ± 1%,而LV dP/dt的变化(0 ± 2%)、LV缩短分数(+4 ± 3%)和心率(+1 ± 1%)无统计学意义。同样,L-158,809(4 mg/kg静脉注射)使心输出量增加9 ± 2%,使平均动脉压和TPR分别降低4 ± 1%和11 ± 3%,而LV dP/dt的变化(+3 ± 3%)、LV缩短分数(+3 ± 1%)和心率(0 ± 1%)无统计学意义。然而,联合给予依那普利拉(1 mg/kg静脉注射)和L-158,809(1 mg/kg静脉注射)可使TPR降低21 ± 3%,该效应大于单独给予这两种药物中任何一种4 mg/kg静脉注射时的效应(p < 0.05)。联合给药时平均动脉压(-9 ± 2%)、心输出量(+15 ± 4%)和LV缩短分数(+11 ± 3%)的变化也往往更大。此外,在序贯给药方案中,在依那普利拉(1 mg/kg静脉注射)后30分钟给予L-158,809(1 mg/kg静脉注射),TPR降低20 ± 4%,而在依那普利拉后30分钟给予第二剂依那普利拉(1 mg/kg静脉注射)时TPR仅降低6 ± 3%(p < 0.05)。联合治疗组的平均动脉压和心输出量变化也往往大于给予两剂依那普利拉序贯治疗组。
在清醒的心力衰竭猪中,ACE抑制剂和AT1受体拮抗剂的联合血管舒张作用大于仅使用其中一种药物时产生的作用,这表明ACE抑制和AT1受体拮抗的独立机制可能部分负责心力衰竭期间血管动力学的改善。
