Alpha2-adrenoceptors in platelets of spontaneously hypertensive rats

Abstract

Alpha₂-adrenoceptors were studied in platelets of stroke-prone spontaneously hypertensive rats (SpSHR) and of normotensive Wistar Kyoto control rats (WKY). In platelets of female SpSHR with established hypertension but not in those of normotensive WKY, specific binding of the α₂-adrenoreceptor ligand, [³H]yohimbine, was found. Compared with human platelets (K _D and B _max about 3 nM and 200 fmol/mg protein, respectively), [³H]yohimbine binding to SpSHR platelets was of lower affinity (K _D about 20 nM) and of lower capacity (B _max about 30 fmol/mg protein). The potency orders of α-adrenoceptor agonists (clonidine > adrenaline > phenylephrine) and antagonists (yohimbine ≧ phentolamine > prazosin) in competing with [³H]yohimbine indicated that the binding sites in SpSHR platelets are of the α₂-adrenoreceptor type. Similar data were obtained in platelets of 7–9 week old hypertensive rats without established hypertension. Furthermore, adrenaline inhibited SpSHR but not WKY platelet adenylate cyclase. This inhibition, which was smaller than in human platelets, was also found in platelets of 4 week old SpSHR but not in the corresponding control rats. The data show that in SpSHR α₂-adrenoreceptors can appear, which may play a significant role in the pathogenesis of hypertension.