Autor: |
KATZ, ARNOLD M., REPKE, DORIS I., TADA, MICHIHIKO, CORKEDALE, SUSAN |
Zdroj: |
Cardiovascular Research; Jul1974, Vol. 8 Issue 4, p541-549, 9p |
Abstrakt: |
Both cardiac microsomal Ca-binding and Ca-uptake were inhibited by propranolol. Both 1-propranolol (which has β-blocking and local anaesthetic actions) and d-propranolol (which lacks the former action) inhibited Ca-binding and Ca-uptake; sensitivity to the 1-isomer being slightly greater than that to the d-isomer. Inhibition of Ca-binding by propranolol could be reversed by Ca2+; kinetic analysis indicated the existence of competitive inhibition between Ca2+ and the drug. Inhibition of Ca-uptake by propranolol was also partially reversed by Ca2+, although kinetic analysis to define competition could not be carried out because Ca-uptake in the range of Ca2+ concentration < 3 x 10"6 M does not exhibit saturation kinetics. Isoproterenol in concentrations equal to or greater than those of propranolol did not reverse inhibition of either Ca-binding or Ca-uptake. Cardiac microsomal adenylate cyclase was not inhibited by concentrations of d,l-propranolol that inhibit Ca-binding and Ca-uptake but the stimulation of adenylate cyclase by 10"4 M epinephrine was abolished by an equimolar concentration of d,l-propranolol. Inhibition of cardiac microsomal Ca-binding and Ca-uptake cannot, therefore, be attributed to a direct β-blocking action of propranolol upon calcium transport by the sarcoplasmic reticulum. [ABSTRACT FROM PUBLISHER] |
Databáze: |
Complementary Index |
Externí odkaz: |
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