Hypertension, Vol 18, 614-621, Copyright © 1991 by American Heart Association
JR Gill Jr, E Grossman and DS Goldstein
Dopamine in urine is derived substantially from renal uptake and
decarboxylation of 3,4-dihydroxyphenylalanine (dopa), and increases in
excretion of dopa normally parallel increases in excretion of dopamine
during salt loading. Since patients with salt-sensitive hypertension may
have decreased urinary excretion of dopamine during dietary salt loading,
the present study was designed to evaluate the response of dopa to salt
loading. Sixteen inpatients with normal-renin essential hypertension ate a
constant metabolic diet containing 9 mmol/day sodium for 7 days, followed
by the same diet but containing 249 mmol/day sodium for 7 days. Salt
sensitivity was defined as an increase in mean arterial pressure of 8 mm Hg
between the diets; on this basis, nine patients were salt-sensitive and
seven, salt-resistant. The rate of urinary dopa excretion was significantly
higher in the salt-sensitive patients throughout the study (mean rates 132
+/- 13 nmol/day in the salt-sensitive group and 78 +/- 9 nmol/day in the
salt-resistant group for the 14 days of observation, p less than 0.01).
When dietary sodium intake was increased to 249 mmol/day, urinary dopa
excretion increased significantly more in salt-sensitive patients than
salt-resistant patients. At the end of the high salt diet, dopamine
excretion was significantly attenuated in the salt-sensitive patients,
despite higher rates of dopa excretion. Thus, the urinary ratio of dopamine
to dopa was decreased in salt-sensitive patients, regardless of salt
intake.(ABSTRACT TRUNCATED AT 250 WORDS)
ARTICLES
High urinary dopa and low urinary dopamine-to-dopa ratio in salt- sensitive hypertension
Hypertension-Endocrine Branch, National Heart, Lung, and Blood Institute, Bethesda, Md 20892.
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