par Chatelain, Pierre 
;Waelbroeck, Magali ;Camus, Jean Claude ;De Neef, Philippe ;Robberecht, Patrick ;Roba, Joseph ;Christophe, Jean
Référence European journal of pharmacology, 72, 1, page (17-25)
Publication Publié, 1981-06
;Waelbroeck, Magali ;Camus, Jean Claude ;De Neef, Philippe ;Robberecht, Patrick ;Roba, Joseph ;Christophe, Jean Référence European journal of pharmacology, 72, 1, page (17-25)
Publication Publié, 1981-06
Article révisé par les pairs
| Résumé : | Normotensive (WKY) and spontaneously hypertensive (SHR) male rats were treated orally, one week after weaning and for 9 weeks, with alpha-methyldopa (100 mg/kg per day), propranolol (30 mg/kg per day) or hydralazine (10 mg/kg per day). Untreated WKY and SHR rats served as controls. The development of hypertension in SHR rats were attenuated by treatment but none of the drugs was able to restore the impairment in isoproterenol, secretin and glucagon responsiveness of cardiac adenylate cyclase activity which is characteristic of these animals. In heart membranes from both WKY and SHR rats, alpha-methyldopa treatment increased the number of beta-adrenoceptors by 20-32% and the maximal response of adenylate cyclase activity to isoproterenol and glucagon by 20-34%. By contrast, the beta-blocker propranolol was ineffective on these parameters. The results obtained are consistent with the hypothesis that the change in adenylate cyclase seen in SHR rats is genetic in origin and is not a consequence of hypertension. |
