Differentiation of calcium antagonists with respect to their effects in normal and skinned taenia caeci preparations

Author:

Cortijo J1,Foster R W2,Small R C2

Affiliation:

1. Departmento de Farmacologia, Facultad de Medicina, Universidad de Valencia, Espana

2. Department of Pharmacology, Materia Medica and Therapeutics, University of Manchester, Oxford Road, Manchester M13 9PT, UK

Abstract

Abstract In taenia preparations, depolarized by a K+-rich medium, Ca2+ caused contraction and cinnarizine (0.4–100 μM), trifluoperazine (2–100 μM) and verapamil (0.02–10 μM) caused concentration-dependent antagonism of Ca2+, displacing the Ca2+ log concentration-effect curve to the right and depressing the maximal response. Equieffective (IC75) antispasmogenic concentrations were selected. The antispasmogenic effects of verapamil were readily offset by removing the drug from the bathing fluid but those of the other drugs were not. The calcium antagonists (antispasmogenic IC75) were then tested for spasmolytic activity in tissues generating tension in response to the EC80 of Ca2+. Verapamil was more effective in producing spasmolysis than cinnarazine or trifluoperazine. In skinned taenia preparations, verapamil (100 μM) did not inhibit Ca2+-induced contractions. High concentrations of cinnarizine (100 μM) and trifluoperazine (100 μM) inhibited Ca2+-induced activation of the contractile proteins. However, antispasmogenic IC75s from intact taenia were not able to produce this effect on skinned preparations. It is concluded that there are differences between calcium antagonists. The action of verapamil on intact taenia is mainly exerted on the plasma membrane. Cinnarizine and trifluoperazine act both on the plasma membrane and upon the intracellular contractile machinery.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

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