Hypertension, Vol 12, 562-567, Copyright © 1988 by American Heart Association
L Raij, TF Luscher and PM Vanhoutte
Endothelium-dependent relaxations are reduced in hypertensive rats. High
dietary potassium supplementation reduces the incidence of strokes in Dahl
rats independently of blood pressure, thereby suggesting a direct
protective effect of the diet. Endothelium-dependent relaxations and aortic
vascular architecture were studied in Dahl salt-sensitive rats fed 8% NaCl,
0.1% NaCl, or 8% NaCl plus 3.6% potassium citrate for 8 weeks. Rats fed 8%
NaCl or 8% NaCl plus 3.6% potassium citrate became hypertensive, while
those fed 0.1% NaCl did not. Aortic rings with and without endothelium were
suspended in organ chambers filled with physiological salt solution (37
degrees C) and aerated with 95% O2, 5% CO2. In rings contracted with
norepinephrine, acetylcholine and adenosine 5'-diphosphate caused
endothelium-dependent relaxations that were significantly reduced in rats
fed 8% NaCl as compared with those fed 0.1% NaCl. Potassium supplementation
(8% NaCl/3.6% potassium citrate) significantly enhanced relaxations to
acetylcholine in salt- sensitive rats, while those to adenosine
5'-diphosphate and thrombin were either minimally affected or unchanged.
Relaxations to sodium nitroprusside were similar in rats with or without
potassium supplementation. Hypertension significantly increased aortic
medial and intimal thickness. Dietary potassium had no significant effect
on the vascular architecture. These results suggest that high potassium
diet enhances endothelium-dependent relaxations in Dahl rats at least in
part independently of changes in blood pressure. Thus, potassium may be
important for its protective effect against stroke and renal damage in this
animal model of hypertension.
ARTICLES
High potassium diet augments endothelium-dependent relaxations in the Dahl rat
Renal Section, Veterans Administration Hospital, Minneapolis, Minnesota.
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