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冠状动脉内和静脉注射硝苯地平对心脏和外周血管的直接作用

Direct cardiac and peripheral vascular effects of intracoronary and intravenous nifedipine.

作者信息

Terris S, Bourdillon P D, Cheng D T, Pitt B

出版信息

Am J Cardiol. 1986 Jul 1;58(1):25-30. doi: 10.1016/0002-9149(86)90235-3.

Abstract

The hemodynamic effects of a new parenteral formulation of nifedipine administered by the intravenous (1 mg) and intracoronary (IC) (0.1 and 0.2 mg) routes were studied in 10 patients with symptomatic coronary artery disease undergoing diagnostic right- and left-sided cardiac catheterization. Intravenous nifedipine (1 mg) reduced systemic vascular resistance by 34% (p less than 0.01), increased cardiac output by 28% (p less than 0.01) and decreased mean arterial pressure by 10% (p less than 0.01). It had less effect on peak positive dP/dt (-8% p less than 0.025) and on peak negative dP/dt (-15% p less than 0.01). Coronary blood flow increased 20% (p less than 0.025). In contrast, IC nifedipine (0.2 mg) increased coronary blood flow 46% (p less than 0.025), depressed contractility as assessed by peak positive dP/dt (-26% p less than 0.01) and prolonged diastolic relaxation time. The effect of 0.1 mg was similar but less pronounced. These data suggest that the primary therapeutic effect of nifedipine administered systemically to patients at rest results from an increase in coronary blood flow and, to a lesser extent, from afterload reduction; its myocardial depressant effects are small, transient and masked by reflex catecholamine release. IC nifedipine increases coronary blood flow, has a transient negative inotropic effect and prolongs relaxation. The relative importance of these myocardial effects in preventing myocardial ischemia is not known.

摘要

对10例有症状的冠心病患者在进行诊断性左右心导管插入术时,研究了通过静脉(1毫克)和冠状动脉内(IC)(0.1毫克和0.2毫克)途径给予硝苯地平新的肠胃外制剂的血流动力学效应。静脉注射硝苯地平(1毫克)使全身血管阻力降低34%(p<0.01),心输出量增加28%(p<0.01),平均动脉压降低10%(p<0.01)。它对峰值正dP/dt(-8%,p<0.025)和峰值负dP/dt(-15%,p<0.01)的影响较小。冠状动脉血流量增加20%(p<0.025)。相比之下,冠状动脉内注射硝苯地平(0.2毫克)使冠状动脉血流量增加46%(p<0.025),通过峰值正dP/dt评估的收缩力降低(-26%,p<0.01),舒张期松弛时间延长。0.1毫克的效果相似但不太明显。这些数据表明,对静息患者全身给予硝苯地平的主要治疗作用源于冠状动脉血流量增加,在较小程度上源于后负荷降低;其心肌抑制作用较小、短暂且被反射性儿茶酚胺释放所掩盖。冠状动脉内注射硝苯地平增加冠状动脉血流量,有短暂的负性肌力作用并延长舒张期。这些心肌效应在预防心肌缺血中的相对重要性尚不清楚。

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