LOCALIZATION OF CALCIUM CHANNELS OF THE L-TYPE IN HUMAN EPICARDIAL ARTERIES - A LIGHT-MICROSCOPE AUTORADIOGRAPHIC STUDY

被引:2
|
作者
FERRANTE, F
CADONI, A
ZACCHEO, D
AMENTA, F
机构
[1] UNIV CAMERINO,IST FARMACOL,SEZ ANAT UMANA,I-62032 CAMERINO,ITALY
[2] UNIV ROMA LA SAPIENZA,DIPARTIMENTO SCI CARDIOVASC & RESP,ROME,ITALY
[3] UNIV GENOA,IST ANAT UMANA,GENOA,ITALY
关键词
EPICARDIAL ARTERIES; HUMANS; AUTORADIOGRAPHY; L-TYPE CA2+ CHANNELS; H-3] NICARDIPINE;
D O I
10.3109/10641969509033642
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The anatomical localization of Ca2+ channels of the L-type was analyzed in sections of the human right and anterior interventricular coronary arteries by using in vitro light microscope autoradiography associated with radioligand binding techniques. [H-3]Nicardipine was utilised as a ligand. Binding of the radioligand to sections of the two coronary arteries was time-, temperature- and concentration-dependent. Analysis of binding isotherms revealed a dissociation constant value of about 0.5 nM in the two arteries and maximum binding capacities of 139 +/- 6.4 fmol/mg tissue for the right coronary artery and of 173 +/- 9.5 for the anterior interventricular branch. The pharmacological profile of [H-3]nicardipine binding to sections of human coronary arteries was consistent;with the labelling of Ca2+ channels of the L-type. Dihydropyridine derivatives were the most powerful competitors of [H-3]nicardipine binding, whereas phenylalkilamines, benzothiazepine or non-selective channel modulators were weak competitors or ineffective. Light microscope autoradiography revealed the highest density of [3H]nicardipine binding sites in the tunica media of the coronary arteries. In this layer Ca2+ channels of the L-type are located within smooth muscle cells. A lower accumulation of the radioligand occurred in the tunica adventitia, whereas no specific binding was found in the tunica intima. Study of the localization of Ca2+ channels in sections of human coronary arteries may contribute to a better understanding of the mechanism of the marked coronary dilatory activity elicited by Ca2+ antagonists demonstrable in both in vitro preparations and in vivo.
引用
收藏
页码:895 / 912
页数:18
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