Renal dysfunction, which comprises 10%-40% of acute heart failure patients (AHF), plays an important role in diuretic resistance mechanism. DR-AHF was designed to demonstrate the effectiveness of early tolvaptan (a vasopressin-2 receptor antagonist) add-on therapy in acute heart failure patients with renal dysfunction and clinical evidence of loop diuretic resistance.
This is a single-center, open-label, randomized controlled trial, which will enroll 128 patients hospitalized due to AHF. These patients with wet-warm phenotype whose estimated glomerular filtration rates at admission are above 15 and below 60 mL/min/1.73 m2, and cumulative urine output \<300 mL in 2 hours after the first dose of intravenous furosemide will be randomly assigned 1:1 to receive a standard care with uptitrating intravenous furosemide alone or a combination therapy with tolvaptan 15mg once daily for 2 days. The standard furosemide treatment will follow the modified 2019 Position Statement from the ESC Heart Failure Association. The primary endpoint is the cumulative urine output at 48 hour. Key secondary endpoints include the improvement of fractional excretion of sodium at 6 hour, the total dose of furosemide, the changes in the body weights, the net fluid loss, the lessening of diastolic dysfunction parameters on echocardiography, and the incidence of clinically relevant worsening renal function at 48 hour.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
128
vasopressin-2 receptor antagonist 15mg once daily is added-on to the conventional diuretic strategy
Cardiology Department
Ho Chi Minh City, Vietnam
RECRUITINGCumulative urine volume output at 48h after randomization
Urine volume in mL
Time frame: Hour 48
Cumulative dose of furosemide at 48h after randomization
Furosemide dose in mg
Time frame: Hour 48
Symptom of dyspnea by 7-point Likert scale at 24h and 48h after randomization
3: markedly better, 2: moderately better, 1: minimally better, 0: no change, -1: minimally worse, -2: moderately worse, -3: markedly worse
Time frame: Hour 24, Hour 48
Changes in body weight at 24h and 48h after randomization
weight in gram
Time frame: Hour 24, Hour 48
Incidence of clinically relevant worsening renal function at 24h and 48h after randomization
An increase in serum creatinine ≥ 0.3 mg/dL within 48 hours accompanying doubling the dose of furosemide according to the diuretic treatment protocol
Time frame: Hour 24, Hour 48
Changes in serum electrolytes measured at 12h, 24h and 48h after randomization
Changes in serum sodium (mmol/L), potassium (mmol/L), chloride (mmol/L)
Time frame: Hour 12, Hour 24, Hour 48
Changes in urine electrolyte excretion at 6h, 24h and 48h
Increase in sodium (mmol/L), potassium (mmol/L) and chloride (mmol/L) excretion adjusted for urine creatinine (umol/L)
Time frame: Hour 6, Hour 24, Hour 48
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Changes in NT-proBNP at 48h after randomization
Changes in NT-proBNP (pg/mL)
Time frame: Hour 0, Hour 48
Changes in mitral e' on echocardiography
Average of septal e' (cm/s) and lateral e' (cm/s) on tissue doppler imaging in apical 4-chamber view
Time frame: Hour 24, Hour 48
Changes in E/e' ratio on echocardiography
The ratio between mitral E (cm/s) and average e' (cm/s)
Time frame: Hour 24, Hour 48
Changes in left atrial volume on echocardiography
Average of left atrial volumes (ml) by Simpson's rule in apical 4-chamber and 2-chamber view
Time frame: Hour 24, Hour 48
Changes in tricuspid regurgitation maximal velocity on echocardiography
Tricuspid regurgitation maximal velocity (m/s) by continuous wave doppler in apical 4-chamber view
Time frame: Hour 24, Hour 48
Changes in inferior vena cava maximal diameter on echocardiography
Inferior vena cava maximal diameter (mm) in subcostal view
Time frame: Hour 24, Hour 48