The purpose of this study is to assess the efficacy of two different treatment regimens for treating resistant hypertension previously uncontrolled with at least 3 antihypertensive treatments. The study hypothesis is that these two regimens (one based on increasing diuretics and the other based on increasing renin angiotensin system blockage) may not differ in terms of efficacy.
Tested hypothesis: For essential resistant hypertension, a new regimen based on intensive RAS blockage is non inferior to the recommended regimen based on intensive sodium depletion. Primary objective: To demonstrate non-inferiority (i.e difference between the two regimen less than 5 mmHg for the mean day-time SBP at week 12) * One treatment arm including irbesartan 300 mg, hydrochlorothiazide (HCTZ) 12.5mg, amlodipine 5 mg, ramipril 10mg and bisoprolol 10 mg * One treatment arm including irbesartan 300 mg, HCTZ 12.5mg, amlodipine 5 mg, spironolactone 25 mg, furosemide 40 mg and amiloride 5 mg. Secondary objectives: * To assess clinical and biological safety and efficacy of these regimen * To evaluate predicted factors of controlled or uncontrolled BP * To evaluate compliance to treatment * To compare the cost of the different strategies * To compare the two strategies in terms of endothelial function and left ventricular diastolic filling Study design: * Period 1 from week-4 to week 0 : 4-week treatment for all patients with irbesartan 300 mg, HCTZ 12.5mg, amlodipine 5 mg. At the end of this period, an ABPM will be performed: only patients with a mean day time SBP\>135 and/or DBP\>85 mmHg will be randomized for a further 3 months treatment * Period 2 from week 0 to week 4: patients will be randomized in two groups, the first one receiving spironolactone 25mg and the second one receiving ramipril 5 mg as add-on therapy (on top of the previous tri-therapy). * Period 3 from week 4 to week 8: Patients with BP controlled at week 4 (i.e mean home blood pressure measurement (HBPM) \<135/85 mmHg at week 4) remain on the same treatment. For those uncontrolled (i.e. mean HBPM \>135/85 mmHg at week 4), furosemide 20 mg will be added in the first group and ramipril will be titrated to 10 mg in the second group * Period 4 from week 8 to week 10: Patients with BP controlled at week 8 (i.e. mean HBPM \<135/85 mmHg at week 8) remain on the same treatment. For those uncontrolled (i.e. mean HBPM \>135/85 mmHg at week 8), furosemide will be titrated to 40 mg in the first group and bisoprolol 5 mg will be added in the second group. * Period 5 from week 10 to week 12 (end of the study): Patients with BP controlled at week 10 (i.e mean HBPM \<135/85 mmHg at week 10) remain on the same treatment. For those uncontrolled (i.e mean HBPM \> 135/85 mmHg at week 10), amiloride 5 mg will be added to the previous treatment in the first group and bisoprolol will be titrated to 10 mg in the second group. Reasons for treatment discontinuation: * Patient decision * Informed consent withdrawal * SBP\>180 mmHg or \<100 mmHg (HBPM) whatever the time during the trial * Adverse events related to treatment or not
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
180
irbesartan, amlodipine and hydrochlorothiazide
Investigation Clinical Center European Georges Pompidou Hospital
Paris, Île-de-France Region, France
Mean day-time systolic blood pressure (SBP) at week 12, measured with an average blood pressure measurement (ABPM) device
Mean day-time systolic blood pressure (SBP) at week 12, measured with an average blood pressure measurement (ABPM) device
Time frame: at week 12
Efficacy: mean day-time diastolic blood pressure (DBP) at week 12, mean 24 hours SBP and DBP at week 12 measured with an ABPM device
hours SBP and DBP at week 12 measured with an ABPM device
Time frame: at week 12,
Safety and tolerability:
Safety and tolerability:
Time frame: during the study
During the study BP will be evaluated every 4 weeks by home blood pressure measurement [HBPM] in order to detect hypotension)
During the study BP will be evaluated every 4 weeks by home blood pressure measurement \[HBPM\] in order to detect hypotension)
Time frame: every 4 weeks
Biological examinations:
Biological examinations:
Time frame: during the study
blood and urinary electrolytes with creatinemia at week 0, 4, 8, 10 and 12
blood and urinary electrolytes with creatinemia at week 0, 4, 8, 10 and 12
Time frame: at week 0, 4, 8, 10 and 12
brain natriuretic peptide (BNP), active renin, aldosterone at week 0 and 12
brain natriuretic peptide (BNP), active renin, aldosterone at week 0 and 12
Time frame: at week 0 and 12
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Other explorations:
Other explorations:
Time frame: during
Treatment compliance (study drug accounting, N-acetyl-seryl-aspartyl-lysyl-proline [Ac SDKP] for angiotensin converting enzyme inhibitor [ACEi])
Treatment compliance (study drug accounting, N-acetyl-seryl-aspartyl-lysyl-proline \[Ac SDKP\] for angiotensin converting enzyme inhibitor \[ACEi\])
Time frame: during the study
Echocardiography (week 0 and 12)
Echocardiography (week 0 and 12)
Time frame: week 0 and 12
Endothelial function (week 0 and 12)
Endothelial function (week 0 and 12)
Time frame: week 0 and 12
Pharmacokinetics of drugs (week 0 and 12)
Pharmacokinetics of drugs (week 0 and 12)
Time frame: week 0 and 12