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Potent vasodilatory with minor cardiodepressant actions of mibefradil in human cardiac tissue

机译:在人心脏组织中有效的舒张血管舒张性舒张作用

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摘要

The present study compared the cardiovascular effects of mibefradil (MIB), a novel Ca2+-channel antagonist with high selectivity for T-type Ca2+-channels to the effect of the L-type Ca2+-channel-antagonists nifedipine (NIF) and diltiazem (DIL) in left ventricular myocardium and coronary arteries of hearts obtained from patients suffering from dilated cardiomyopathy (NYHA IV). Right atrial myocardium from patients undergoing aortocoronary bypass surgery without signs of cardiac failure was studied as well.NIF and DIL (100 μmol l−1) completely depressed force of contraction (FOC) in electrically driven left ventricular myocardium (NIF 6.5±1.4% and DIL 7.1±1.2% of control), whereas a similar concentration of MIB only reduced force of contraction to 55.1±4.0% of the basal FOC. The negative inotropic potency as measured by the concentration needed to reduce basal FOC for 25% was NIF (0.0095 μmol l−1)>DIL (0.041 μmol l−1)>MIB (9.47 μmol l−1).All three Ca2+-channel antagonists were more potent in human atrial compared to human left ventricular myocardium to reduce FOC.The rank order of Ca2+-antagonistic moiety as measured by the decrease of the intracellular Ca2+-transient (fura-2 ratio method) was NIF>DIL>MIB.All Ca2+-channel antagonists completely relaxed human coronary arteries (% of papaverine effect: MIB 81.7±5.5%, DIL 91.3±0.9%, NIF 96.4±3.7%) precontracted with PGF2α (0.3 μmol l−1). The rank order of vasodilatory potency was NIF (EC50; 0.02 μmol l−1)>DIL (0.13 μmol l−1)>MIB (2.05 μmol l−1).The vasoselectivity measured by the ratio of the concentration needed to achieve a 25% decrease in force and the concentration needed for 25% vasodilatation was 316 for MIB, 1.5 for NIF and 1.0 for DIL.The present study provides evidence that blockade of T-type Ca2+-channels (e.g. mibefradil) results in potent vasodilatory properties with only minor cardiodepressant effects.
机译:本研究比较了米贝拉地尔(MIB)(一种对T型Ca2 +通道具有高选择性的新型Ca2 +通道拮抗剂)与L型Ca2 +通道拮抗剂硝苯地平(NIF)和地尔硫卓(DIL)的心血管作用。 )从患有扩张型心肌病(NYHA IV)的患者获得的左心室心肌和心脏的冠状动脉中。还研究了无心衰征象的主动脉冠状动脉搭桥手术患者的右心房心肌.NIF和DIL(100μμmol·l-1)完全抑制了电动左心室心肌的收缩力(FOC)(NIF 6.5±1.4%和DIL为对照组的7.1±1.2%),而类似浓度的MIB仅将收缩力降低至基础FOC的55.1±4.0%。通过将基础FOC降低25%所需的浓度来测量的负性肌力强度为NIF(0.0095μmol-1)> DIL(0.041μmol-1)> MIB(9.47 mol -1)。所有三个Ca2 +通道与人左心室心肌相比,拮抗剂在人心房中对FOC的降低作用更强。通过细胞内Ca2 +瞬变的减少(fura-2比值法)测量,Ca2 +拮抗部分的等级顺序为NIF> DIL> MIB。所有的Ca2 +通道拮抗剂都完全放松了预先与PGF2α(0.3?μmol·l-1)签订合同的人冠状动脉(罂粟碱作用的百分比:MIB 81.7±5.5%,DIL 91.3±0.9%,NIF 96.4±3.7%)。血管舒张力的等级顺序为NIF(EC50;0.02μmol·l-1)> DIL(0.13μmol·l-1)> MIB(2.05μmol·l-1)。通过达到25所需的浓度比来测量血管选择性。力降低百分比,25%血管舒张所需的浓度对于MIB为316,对于NIF为1.5,对于DIL为1.0。本研究提供的证据表明,T型Ca2 +通道(例如米贝拉地尔)的阻断导致有效的血管舒张特性,仅轻微的抗抑郁作用。

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