Insulin Resistance Clinical Trial
Official title:
The Influence of Rosiglitazone on the Diuretic Effect of Furosemide and Amiloride. A Double-blind Placebo Controlled Cross Over Study.
Thiazolidinedione derivates (TZD's) are Peroxisome-Proliferator-Activated-Receptor-γ
agonists (PPARγ-agonists) and enhance insulin sensitivity. One of the side effects, however,
is the fact that subjects treated with these drugs seem to be more prone to fluid retention.
The precise mechanism of rosiglitazone-related fluid retention is unknown, but it is clear
that either primary or secondary renal sodium retention is part of the mechanism.
Furthermore in observational studies, TZD-related oedema seems to be resistant to loop
diuretic therapy. The recent finding that rosiglitazone induces upregulation of the
epithelial sodium channel (ENaC) in the kidney could be the explanation for TZD-related
fluid retention and the observed resistance to loop diuretics. In the present human in-vivo
study the following hypothesis will be tested:
Rosiglitazone treatment stimulates the activity of ENaC in the distal nephron, which
enhances the natriuretic effect of amiloride and decreases the natriuretic effect of
furosemide in parallel.
This is a randomized, placebo-controlled, double-blind, single-centre, cross-over study with
4 weeks of wash out comparing placebo with rosiglitazone 4 mg bid for 9 weeks treatment
periods. Randomization of the treatment sequence will be computer-generated, with a
sequentially driven allocation. Randomization and blinding will be performed at the
department of Clinical Pharmacy. After 8 (furosemide) and 9 (amiloride) weeks in each period
the end-point experiments will be performed. During all visits (week 0, 4, 8, 9) of each
period, adverse events and pill compliance will be recorded. In addition, physical
examination, foot volume and bio-impedance measurements will be performed and safety
chemical, and hematological profiles will be determined. Only at start and at 8 weeks in
each period, glucose, insulin and HbA1c are measured. All visits and interventions will be
performed at the Clinical Research Center Nijmegen (CRCN).
Furosemide end-point experiment Each participant will attend the hospital at 8 a.m. after an
overnight fast and abstinence of alcohol and caffeine for 20 hours, delivering a 24-hour
urine collection and the present morning voiding. The previous three days each participant
will adhere to an individualized diet containing 150 mmol of sodium and 80 mmol of potassium
prescribed by a dietician. First, blood will be collected to measure fasting glucose and
insulin concentrations. Then the subject will be given an individualized breakfast including
1 cup of water. Afterwards a brachial vein will be cannulated and connected to a Braunpump
(10 ml/hr NaCl 0.9%), followed by blood drawing for safety and vascular hormone measurements
(aldosterone, Atrial Natriuretic Peptide (ANP), Brain Natriuretic Peptide (BNP), Vascular
Endothelial Growth Factor (VEGF) and renin).
A bolus of furosemide (40 mg) will be injected through a small cannule in a vein of the
contra-lateral arm, just after bladder emptying. Venous blood samples will be drawn at 0,
15, 30, 45, 60, 90,120, 150, 180, 240, 300, 360, 420 and 480 minutes after bolus injection
to measure plasma furosemide levels. The participants will be asked to urinate regularly, at
least hourly. The exact time of voiding and the urine volume will be recorded. Two urine
samples will be taken. In one sample, sodium and creatinine concentrations will be measured
while the other sample will be light-protected and immediately frozen for measurement of
furosemide levels later on. To prevent dehydration each participant will be asked to drink
tap water equal to the volume of diuresis in the previous hour. During the test the
participant will be sitting on a bed. At noon the participant will be offered an
individualized lunch. After 8 hours each participant will leave the hospital with the
instruction to adhere to the diet without fluid restrictions and to collect the urine for up
to 24 hours after start of the experiment.
Amiloride end-point experiment Until amiloride infusion the procedures will be similar. At
time point 0, venous infusion of a loading dose of amiloride will be started (150 μg/kg in
60 minutes) followed by maintenance infusion (0.20 μg/kg/min) for 4 hours. Amiloride will be
obtained as a sterile powder in the form of amiloride HCl/2H2O . Directly before use, the
powder will be dissolved in NaCl 0,9% up to a concentration of 1 mg/ml and the solution was
filtered through a 0.22 μm Millipore filter. Venous blood for measurement of the amiloride
concentration will be sampled at 60, 180, 300 and 420 minutes. All the other procedures will
be similar to the furosemide experiment.
Pharmacokinetic considerations on the amiloride-dose The peak plasma levels 3-4 hours after
intake of 10 or 20 mg amiloride are 20 μg/L (32) and 38-40 μg/L respectively(33). These
concentrations are well below the half maximal inhibitory concentration (IC50) of amiloride
for Na+/H+ and Na+/Ca2+-transporters and the α1-receptor, but well above the IC50 for
ENaC(34). Using the pharmacokinetic characteristics of amiloride(35) we calculated the
required amiloride infusion in order to reach a steady-state concentration between 30-45
μg/L.
Exosome extraction:
Urinary exosomes will be isolated by ultracentrifugation and ENaC abundance will be measured
by immunoblotting as previously described (19;36) and normalized to urine creatinine levels.
4 µg of protein lysed in Laemmli buffer will be loaded on 8% SDS-PAGE. PAGE, blotting and
blocking of the PVDF membranes will be done as previously described. Membrane will be
incubated with 1:4000-diluted affinity-purified rabbit α-ENaC antibody (Rossier BC,
Lausanne, Switzerland), followed by 1:5,000-diluted goat anti-rabbit IgG's as secondary
antibody coupled to horseradish peroxidase. Blotting signals will be visualized using
enhanced chemiluminescence. The samples will be normalized for the expression level of
α-ENaC in placebo treatment and indicated as percentage.
;
Allocation: Randomized, Endpoint Classification: Pharmacokinetics/Dynamics Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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