Hypertension, Vol 8, 662-668, Copyright © 1986 by American Heart Association
TJ Resink, E Burgisser and FR Buhler
Platelets provide an accessible and homogeneous cellular system for
investigative studies on hypertension. Hypertension-associated
abnormalities of cyclic adenosine 3',5'-monophosphate (AMP) metabolism were
studied in human platelets. Platelets from hypertensive subjects had an
enhanced cyclic AMP accumulation response to prostaglandin E1 (twofold
increase in prostaglandin E1 sensitivity). The degree of adenylate cyclase
activation in response to both prostaglandin E1 (receptor-mediated) and
forskolin (non-receptor-mediated) was greater in hypertensive than
normotensive subjects, and prostaglandin E1- stimulated and
forskolin-stimulated adenylate cyclase activity correlated directly (r =
0.71, p less than 0.001, n = 26). This finding suggests that the catalytic
subunit of the enzyme is the rate-limiting step of this hormonal
information transduction. Platelets from hypertensive subjects were more
sensitive to epinephrine-induced inhibition of the stimulatory effects of
prostaglandin E1 on both cyclic AMP accumulation (fourfold) and activation
of cyclic AMP- dependent protein kinase. These findings suggest that the
enhanced cyclic AMP metabolic response to prostaglandin E1 in platelets
from subjects with established essential hypertension may function as a
negative feedback mechanism to protect the cells against calcium overload
and to reduce their stimulated participation in hemostatic and thrombotic
processes.
ARTICLES
Enhanced platelet cyclic AMP response to prostaglandin E1 in essential hypertension