A Paradoxical Fall in Urine Dopamine Output When Patients with Essential Hypertension Are Given Added Dietary Salt

Harvey, Jeremy N.; Casson, Ian; Clayden, A D; Cope, Georgina; Perkins, C. M.; Lee, M. R.

doi:10.1042/cs0670083

Cited by 50 publications

(22 citation statements)

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“…43 White subjects with essential hypertension have also been reported to exhibit lower levels of DA excretion compared with normotensive whites in response to increasing dietary salt intake. 24 -" Gill et al 25 observed no increase in urinary DA in salt-sensitive and salt-resistant hypertensive subjects with normal renin in contrast to the rise in urinary DA in normotensive subjects on changing from a low to a high salt intake; although not specified, it is presumed that these patients were white. In line with these data demonstrating decreased urinary excretion of DA with salt loading is the observation that hypertensive whites appear to be more sensitive to the natriuretic and hypotensive effects of DA and DA agonists than normotensive subjects.…”

Section: Discussionmentioning

confidence: 99%

“…13 -22 That the dietary salt or saline-mediated natriuresis is causally linked to renal DA excretion is supported by the observation that administration of carbidopa, the peripheral inhibitor of the enzyme dopa decarboxylase, prevents the increases in urinary sodium in response to dietary salt 23 and saline infusion. 14 - 15 However, there is evidence that salt loading does not appropriately increase urinary DA excretion in hypertensive patients, 24 -M suggesting that decreased renal DA production in response to a salt load may play a role in the pathogenesis and maintenance of hypertension. Data from a recent report by Gill et al 23 suggested that salt sensitivity in hypertensive patients with normal renin may be related in part to decreased urinary DA to norepinephrine ratios, particularly with high salt intake.…”

Section: H Ypertension In American Blacks Asmentioning

confidence: 99%

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Salt sensitivity in blacks. Salt intake and natriuretic substances.

Sowers

Zemel

et al. 1988

Hypertension

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SUMMARY Accumulating evidence suggests that hypertension hi blacks is manifested hi part by impaired renal excretion of salt. Consequently, this study was performed to determine if hypertensive and normotensive black subjects differ hi their ability to generate known natriuretic substances. Fourteen normotensive and 11 hypertensive blacks were maintained on constant metabolic diets containing either 40 or 180 mmol of salt per day for 14 days each. During the last 4 days of each salt intake period, urine was collected for measurement of sodium, dopamine, and norepinephrine. On the last day of each 14-day dietary period, blood pressures were measured, blood was collected for measurement of plasma atrial natriuretic factor (ANF) and aldosterone, and urine was collected over 2 hours for measurement of prostaglandin E 2 (PGE 2 ). Both the normotensive and the hypertensive groups manifested salt sensitivity; then-mean arterial pressure rose by 7 ± 0.2 and 6 ± 0.2%, respectively, when salt intake was increased from 40 to 180 mmoJ/day. The hypertensive group exhibited decreased (p < 0.05) dopamme excretion as compared with the normotensive group for both dietary salt intakes. Plasma ANF levels increased (p < 0.05) in the hypertensive group, but not in the normotensive group, with increasing dietary salt. Plasma aldosterone and urinary norepinephrine and PGE 2 were comparable in the two groups for both dietary salt Intakes. These data suggest that salt sensitivity is not unique to hypertensive blacks but occurs hi normotensive blacks as well. Decreased renal production of dopamme may be a pathogenic factor hi the development and maintenance of hypertension in blacks. compared with hypertension in whites, is characterized by a higher incidence of salt sensitivity '-4 in spite of the apparent lack of differences in sodium and salt intakes between the two populations. 5 The mechanisms involved in the relatively high incidence of salt-sensitive hypertension in blacks are poorly understood. However, an impaired natriuretic response to a salt load in hypertensive blacks could result from a reduced ability to generate natriuretic substances such as dopamine (DA), prostaglandin E? (PGE2), and atrial natriuretic factor (ANF).There is a considerable body of evidence suggesting a relationship between renal production of DA and the ability of the kidney to excrete a salt load. 6 -21 Enhanced dietary salt intake or infusion of saline results in an increase in urinary DA excretion and a decrease in norepinephrine excretion. 13 -22 That the dietary salt or saline-mediated natriuresis is causally linked to renal DA excretion is supported by the observation that administration of carbidopa, the peripheral inhibitor of the enzyme dopa decarboxylase, prevents the increases in urinary sodium in response to dietary salt 23 and saline infusion. 14 -15 However, there is evidence that salt loading does not appropriately increase urinary DA excretion in hypertensive patients, 24 -M suggesting that decreased renal DA production in response to...

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Section: Discussionmentioning

confidence: 99%

Section: H Ypertension In American Blacks Asmentioning

confidence: 99%

Salt sensitivity in blacks. Salt intake and natriuretic substances.

Sowers

Zemel

et al. 1988

Hypertension

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show abstract

“…It seems likely to be effective in hypertension and congestive heart failure with perhaps less tendency to produce sodium retention than known vasodilators. Our group has produced evidence that renal dopamine mobilization on salt loading is deficient both in essential hypertension (Perkins et al, 1980;Harvey et al, 1984) and in chronic renal failure (Casson et al, 1983). Treatment with a peripheral dopamine receptor agonist may be particularly appropriate in both these clinical conditions.…”

Section: Discussionmentioning

confidence: 99%

The effect of oral fenoldopam (SKF 82526‐J), a peripheral dopamine receptor agonist, on blood pressure and renal function in normal man.

Harvey¹,

Worth²,

Brown³

et al. 1985

Brit J Clinical Pharma

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1 The effect of a single oral dose of 100 mg of fenoldopam on renal function and blood pressure was investigated in seven healthy male subjects in a double-blind placebo controlled study. 2 Mean diastolic blood pressure fell by 10 mm Hg, 45 min after oral dosing and then gradually returned to baseline values. There was an increase in pulse rate and a delayed rise in systolic blood pressure. 3 Measured from 30 to 120 min after drug ingestion, mean effective renal plasma flow increased to 158% of the value observed after placebo; mean glomerular filtration rate rose to 109% of the placebo value. Measured from 120 to 210 min after administration of the drug, effective renal plasma flow and glomerular filtration rate had returned to baseline values. 4 Fenoldopam produced a small increase in the mean sodium excretion rate which was not significantly different from the fall after placebo. No change was detected in urine flow or potassium excretion rate. 5 Mean plasma renin activity increased three-fold 1 h after oral dosing. Plasma aldosterone did not show a parallel increase although the plasma concentration at 1 h was significantly higher than after placebo. 6 The results show a pronounced renal vasodilator effect lasting about 2 h. The findings are consistent with marked DA1 receptor agonist activity.Keywords fenoldopam (SKF 82526-J) dopamine renal blood flow blood pressure

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“…Many stud ies have shown that elevated dietary salt in take can elevate urinary DA excretion [3][4][5][6]. High salt diets do not appear to increase the activity of AAAD when compared to normal salt diets [47][48][49][50], but do result in increased AAAD activity when compared to low salt diets [49.50].…”

Section: Discussionmentioning

confidence: 99%

“…Therefore, it is of great importance to under stand the factors that are involved in the regu lation of the synthesis and release of DA in the kidney. Studies of human salt-dependent hy pertension have consistently reported that urinary DA excretion is attenuated in individ uals that are salt-sensitive and placed on high salt diets [3][4][5][6]. Furthermore, recent studies have suggested that defects exist in the cou pling of renal DA receptors to their effector systems in spontaneously hypertensive rats and may contribute to the development of hy pertension [7.…”

mentioning

confidence: 99%

Characterization of the Synthesis and Release of Dopamine in LLC-PK<sub>1</sub> Cells

Dawson¹,

Felheim²,

1994

Kidney Blood Press Res

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The ability of a renal epithelial cell line of porcine origin (LLC-PK₁) to synthesize dopamine (DA) from L-dopa and release DA into the culture media was studied. L-Dopa was rapidly taken up by LLC-PK₁ cells and converted to DA which was then released into the media. L-Dopa uptake and conversion to DA was competitively inhibited by other aromatic amino acids (Tyr and Phe). Studies were conducted to assess L-dopa uptake, DA synthesis and DA release in LLC-PK₁ cells in response to changes in the ionic composition of the Krebs-Ringer bicarbonate (KRB) buffer media and to various drugs known to alter renal transport function. Sodium chloride addition to KRB media resulted in enhanced DA release into the media that was significantly attenuated by both quinine (1 mM) and benzamil (0.1 mM). Other sodium salts (sodium acetate and sodium phosphate) also enhanced DA release from LLC-PK₁ cells. Salts containing chloride (LiCl, NH₄Cl, choline chloride) stimulated a greater efflux of DA from LLC-PK₁ cells than sodium salts at equimolar concentrations. Osmotic stimuli (sucrose, mannitol and dextran, 50-200 mM) also elicited increased DA release from LLC-PK₁cells into the media but not to the same extent as inorganic salts. DA release (secretion) from LLC-PK₁ cells was strongly inhibited (25-50%) by drugs known to be substrates for the renal cation transport system. These studies have characterized extensively the factors that govern and regulate the synthesis of DA from L-dopa and the transport system responsible for the secretion (release) of intracellular DA into the media.

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A Paradoxical Fall in Urine Dopamine Output When Patients with Essential Hypertension Are Given Added Dietary Salt

Cited by 50 publications

References 0 publications

Salt sensitivity in blacks. Salt intake and natriuretic substances.

Salt sensitivity in blacks. Salt intake and natriuretic substances.

The effect of oral fenoldopam (SKF 82526‐J), a peripheral dopamine receptor agonist, on blood pressure and renal function in normal man.

Characterization of the Synthesis and Release of Dopamine in LLC-PK<sub>1</sub> Cells

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