Hypertension, Vol 22, 315-322, Copyright © 1993 by American Heart Association
K Sudhir, TW Kurtz, PG Yock, AJ Connolly and RC Morris Jr
It has recently been proposed that in rat models of genetic hypertension,
supplemental dietary potassium preserves release of endothelium-derived
relaxing factor independently of its capacity to either attenuate
hypertension or increase plasma potassium. To test this hypothesis in Dahl
salt-sensitive rats given sodium chloride (4%) for 3 weeks, we supplemented
dietary potassium (2.1%) with either KCl (n = 16) or KHCO3 (n = 16).
Compared with unsupplemented rats (n = 16), rats supplemented with either
potassium salt had a lower mean arterial pressure and a greater release of
endothelium-derived relaxing factor, as assessed from acetylcholine-induced
relaxation of precontracted aortic rings. However, the maximum relaxation
response to acetylcholine correlated inversely with blood pressure (r =
-.82, P < .001), not only in the KCl (r = -.68, P < .002) and KHCO3
(r = -.77, P < .001) groups but also in unsupplemented rats (r = -.86, P
< .001). With potassium supplementation, plasma potassium concentrations
measured between 4 and 6 PM did not increase, but those measured between 4
and 6 AM did increase (P < .05). In isolated ring segments, aortic
compliance was greater in both the KCl and KHCO3 groups than in
unsupplemented rats (0.015 and 0.017 vs 0.009 mm2/mm Hg) (P < .01). This
greater compliance could not be related to differences in blood pressure,
plasma potassium, or collagen or elastin content of the aortic
wall.(ABSTRACT TRUNCATED AT 250 WORDS)
ARTICLES
Potassium preserves endothelial function and enhances aortic compliance in Dahl rats
Department of Medicine, University of California, San Francisco 94143- 0126.
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