Hypertension Clinical Trial
Official title:
Effect of Gene Variants on Dopamine Receptor Natriuretic Responses (RMC033)
Hypothesis to be tested: Dopamine D1-like receptor-induced natriuresis is impaired in humans
with G protein-related kinase 4 gene variants.
Our research group has discovered a D1 receptor/adenylyl cyclase coupling defect in renal
PTCs from subjects with essential hypertension. We have found increased GRK-4 activity in
renal PTCs in human essential hypertension due to activating variants of GRK-4, an effect
that was reproduced in a transfected cell model. Preventing the translation of GRK-4
normalized the coupling of the D1 receptor to adenylyl cyclase in hypertension. Gene
variants of GRK-4 cause a ligand-independent serine-phosphorylation of the D1 receptor,
resulting in its uncoupling from the G-protein/effector complex. The desensitization of the
D1 receptor in the renal PTC is hypothesized to be the cause of the compromised natriuretic
effect of DA that eventually leads to Na+ retention and hypertension. The primary objective
of this protocol is to demonstrate that natriuresis engendered by D1-like receptor
activation with fenoldopam is blunted in subjects with 3 or more SNPs of GRK-4 compared with
responses in subjects with 0-2 SNPs.
Dopamine (DA) is an endogenous catecholamine, which serves as a biochemical precursor of
norepinephrine and epinephrine. DA is well known as a neurotransmitter in the central
nervous system. During the past decade, however, DA has been characterized as an important
modulator of BP, Na+ balance, renal and adrenal function through an independent peripheral
dopaminergic system. Evidence indicates that DA is synthesized locally within the kidney and
acts at adjacent cells in an autocrine or paracrine fashion to control renal Na+ excretion
(1,2).
The renin-angiotensin system (RAS) is a coordinated hormonal cascade, the principal effector
of which is angiotensin II (ANG II). All of the components of the RAS are present within the
kidney and intrarenal formation of ANG II provides major regulation of renal hemodynamic and
tubule function via a self-contained intrarenal RAS (3,4). We propose to study the
interaction of the renal dopaminergic and renin-angiotensin systems in the regulation of Na+
balance and Na+ sensitivity of blood pressure (BP) and in the pathophysiology of essential
hypertension in man.
Our group has discovered a D1 receptor/adenylyl cyclase coupling defect in renal PTCs from
subjects with essential hypertension. We have found increased GRK activity in renal PTCs in
human essential hypertension due to activating variants of GRK-4, an effect that was
reproduced in a transfected cell model. Preventing the translation of GRK-4 normalized the
coupling of the D1 receptor to adenylyl cyclase in hypertension. The variants of GRK-4 cause
a ligand-independent serine-phosphorylation of the D1 receptor, resulting in its uncoupling
from the G-protein/effector complex. The desensitization of the D1 receptor in the renal PTC
may be the cause of the compromised natriuretic effect of DA that eventually leads to Na+
retention and hypertension. Therefore, a primary objective of the entire Program Project
Grant, of which this protocol is one part, is to identify humans with salt-sensitive
hypertension and resistance to the inhibitory effect of D1-like receptor agonist fenoldopam
on renal proximal Na+ reabsorption and determine whether these individuals have the
activating polymorphisms of GRK-4 alone or in combination with polymorphisms of genes of the
RAS.
Subjects are selected (on the basis of their GRK-4 genotype) from the pool of subjects that
have already been genetically screened under IRB-HSR # 11494.
Subjects will be prepared and will be studied in approximate metabolic balance at 150 meq
Na+/d. After approximate metabolic balance is achieved (estimated 5 days), subjects will
receive either fenoldopam infusion or vehicle infusion on Day 6 and the opposite agent
(fenoldopam or vehicle) will be infused on Day 7. The order of infusion will be randomized
and the study will be conducted in double-blind fashion. Vehicle will be D5W and will be
infused during the control period using the same rate as the post control period. At 1100 h
on study Day 6, an i.v. infusion of fenoldopam or vehicle will be initiated and continued
for 3h. The fenoldopam infusion rate will be 0.05 μg/kg/min. This infusion rate of
fenoldopam has resulted in a greater than 2-fold increase in UNaV without alteration of
systemic hemodynamic function in normal subjects (30). Plasma fenoldopam levels will be
monitored to document delivery of this agent into the circulation. BP and heart rate will be
measured in duplicate every 10 min during the experimental period (1100-1400h). The
experimental period will be followed by a 2-hour post-control period (1400h-1600h) during
which vehicle will be infused. Blood and urine samples will be obtained every 30 min and
will be analyzed for Na+, K+, lithium and creatinine concentrations and osmolality. In
addition, blood samples will be analyzed for PRA, cyclic AMP (blood and urine), plasma ANG
II and aldosterone concentrations at 1045, 1215, 1345 and 1545 h. After completion of a
post-control period at 1600h, the subjects will be allowed to be out of bed but remain as
inpatients and receive the same diet as previously. No food is given after 2400h on Day 6.
On Day 7, the identical protocol as on Day 6 will be repeated except that the opposite agent
(fenoldopam or vehicle) will be infused. The subjects will be discharged from the GCRC on
their previous diet.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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