Hypertension, Vol 8, 526-532, Copyright © 1986 by American Heart Association
EE Soltis and FP Field
This study investigated the effects of altered extracellular Ca2+ on in
vitro femoral arterial smooth muscle responsiveness in deoxycorticosterone
acetate (DOCA)-salt hypertensive rats. Compared with controls, femoral
arteries from DOCA-salt rats showed a significant increase in sensitivity
to KCl and norepinephrine in normal Ca2+ (2.5 mM). Although no difference
in maximal contractile response to KCl was observed between groups, there
was a significant difference in maximal response to norepinephrine.
Dose-response curves in low Ca2+ (0.25 mM) resulted in a significant
decrease in the sensitivity of femoral arteries from DOCA-salt rats to KCl
and NE so that the responses were similar to those of controls. Relaxation
of femoral arteries from DOCA-salt rats after washout of the KCl
contraction was significantly slower than that of controls in both low and
normal Ca2+. Isoproterenol-induced relaxation of femoral arteries from
DOCA-salt rats was significantly attenuated in normal Ca2+. Sensitivity of
femoral arteries from DOCA-salt rats to isoproterenol increased in low
Ca2+, but maximal relaxation was unaltered. Whereas no difference in
maximal relaxation to NaNO2 was seen in femoral arteries from either group
in normal Ca2+, a significant decrease in sensitivity to NaNO2 was observed
in femoral arteries from DOCA-salt rats. In low Ca2+ the response of
femoral arteries from DOCA-salt rats to NaNO2 was similar to that of
controls. These results suggest that the increased vascular smooth muscle
responsiveness to KCl and norepinephrine seen in DOCA- salt hypertension is
due to increased sensitivity of the vascular smooth muscle to Ca2+.
Extracellular Ca2+, however, plays only a minor role in the decreased
vasodilator responsiveness seen in this form of hypertension.
ARTICLES
Extracellular calcium and altered vascular responsiveness in the deoxycorticosterone acetate-salt rat