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Adrenergic versus VIPergic control of cyclic AMP in human colonic crypts
Authors:N Boige  A Munck  M Laburthe
Institution:Unité de Recherches de Diabétologie et d''Etudes Radio-Immunologiques des Hormones Protéiques Equipe de Recherche sur le Mécanisme d''Action des Hormones et Neuropeptides Digestifs (INSERM U.55, CNRS ERA 494), Hôpital Saint-Antoine, 184, rue du Faubourg Saint-Antoine 75571 Paris Cedex 12, France
Abstract:The actions of catecholamines on VIP-induced cyclic AMP is studied in human colon. We show that: (1) Epinephrine in the 10(-7)-10(-3) M concentration range (ED50 = 11.10(-6) M) inhibits VIP-induced cyclic AMP rise in isolated colonic epithelial cells; the maximal inhibition reaches 30% of VIP effect; epinephrine alters the efficacy of the peptide and does not modify its potency; epinephrine also reduces the basal cyclic AMP level. (2) The inhibition is found with other alpha adrenergic agonists with the order of potencies epinephrine greater than norepinephrine greater than phenylephrine. Clonidine has a poor intrinsic activity but antagonizes the action of epinephrine. (3) The inhibition of VIP action by epinephrine is reversed by the alpha antagonists dihydroergotamine, phentolamine and the alpha 2 antagonist yohimbine, while unaffected by the beta antagonist propranolol and the alpha 1 antagonist prazosin, (4) Epinephrine inhibits VIP-stimulated adenylate cyclase activity in preparations of colonic plasma membranes. Thus catecholamines exert through an alpha 2 adrenoreceptor a negative control on basal and VIP-stimulated cyclic AMP formation in human colon. We suggest that colonic cyclic AMP metabolism undergoes a dual control: VIPergic, activator and adrenergic, inhibitor.
Keywords:Vasoactive intestinal peptide  Catecholamines  Cyclic AMP  Human  Colon
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