MECHANISM OF ACTION OF CLENTIAZEM ON HUMAN CORONARY-ARTERY AND MYOCARDIUM

被引:14
|
作者
NARITA, H [1 ]
ZERA, PH [1 ]
GINSBURG, R [1 ]
机构
[1] STANFORD MED CTR,DIV CARDIOL,STANFORD,CA 94305
来源
CARDIOVASCULAR DRUGS AND THERAPY | 1990年 / 4卷 / 04期
关键词
calcium antagonist; clentiazem; coronary vasorelaxation; diltiazem; negative inotropic action; nifedipine;
D O I
10.1007/BF01856505
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
We evaluated the pharmacologic action of clentiazem, a new diltiazem derivative, on isolated human coronary artery and right ventricular trabeculae. In addition to its Ca2+ blocking action, clentiazem demonstrated both vasorelaxing and negative inotropic actions, similar to our reference Ca2+ antagonists. The coronary vasorelaxing action of clentiazem on the tonic KCl contraction (EC50=2.21×10-7M) was 3.1 times more potent than diltiazem (EC50=6.94×10-7M) and 28.8 times less potent than nifedipine (EC50=7.67×10-9 M). The negative inotropic action of clentiazem (IC50=8.78×10-6 M) was similar to diltiazem (IC50=7.18×10-6M) and was 21.1 times less potent than nifedipine (IC50=3.98×10-7 M). Selectivity ratios, comparing the effectiveness in cardiac muscle to coronary artery, were nifedipine (51.9)>clentiazem (39.7)>diltiazem (10.3), when calculated from the EC50 and the IC50, and clentiazem (24.2)>nifedipine (15.9)>diltiazem (9.3), when calculated from the EC20 and the IC20. In conclusion, clentiazem is a Ca2+ antagonist and demonstrates comparable vasoselectivity to the 1,4-dihydropyridine derivative, nifedipine. Moreover, it has longer lasting áction than diltiazem. © 1990 Kluwer Academic Publishers.
引用
收藏
页码:1097 / 1104
页数:8
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