Uncontrolled Hypertension Clinical Trial
Official title:
Efficacy and Safety of Adrenal Artery Ablation(AAA)in the Treatment of Uncontrolled Hypertension: A Randomized, Parallel, Active-controlled Clinical Trial
Verified date | September 2018 |
Source | Third Military Medical University |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The activation of the renin-angiotensin-aldosterone system (RAAS) plays a key role in
uncontrolled hypertension or resistant hypertension. Surgery and and medicine are the main
treatment for primary aldosteronism(PA) by the current guidelines. However, only a small part
of patients with PA meet the surgical criteria, and most of patients with uncontrolled
hypertension and activation of RAAS have to take spironolactone or other antihypertensive
drugs for long time. On the other side, long-term inhibition of aldosterone receptor may
cause hyperkalemia, male breast hyperplasia and other adverse reactions. Moreover,
hyperaldosterone is still not corrected by spironolactone, which causes extensive
cerebrovascular damages even though blood pressure and blood potassium had been normalized.
With the development of adrenal vein sampling and adrenal ablation, selective arterial
ablation of adrenal gland(AAA) was observed with significant decrease of blood aldosterone
and blood pressure in patients with PA, which made it promising that uncontrolled
hypertension could be relieved by selective AAA.
Status | Recruiting |
Enrollment | 40 |
Est. completion date | January 1, 2020 |
Est. primary completion date | July 1, 2019 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 30 Years to 60 Years |
Eligibility |
Inclusion Criteria: - Male or female, aged between 30-60 years old. - Patients with poorly controlled hypertension (office blood pressure =130/80 mmHg) with rational lifestyle change and triple antihypertensive drugs (irbesartanhydrochlorothiazide 162.5 mg/d, amlodipine 5 mg/d) for at least 2 weeks - Positional blood aldosterone =100pg/ml. - Informed consent signed and agreed to participate in this trial. Exclusion Criteria: - Hyperkalemia or hypokalemia. - Secondary hypertension. - History of depression, schizophrenia or vascular dementia. - Renal failure or the following history of nephropathy: serum creatinine 1.5 times higher than the upper limit; dialysis history; or nephrotic syndrome. - Adrenergic insufficiency. - Heart failure with NYHA grade ?-? grade or unstable angina, severe cardiovascular and cerebrovascular stenosis, myocardial infarction, intracranial aneurysm, stroke and other acute cardiovascular events. - Acute infections, tumors and severe arrhythmias, psychiatric disorders, - drugs or alcohol addicts. - Liver dysfunction or the following history of liver disease: AST or ALT 3 times higher than the upper limit, liver cirrhosis, history of hepatic encephalopathy, esophageal variceal history or portal shunt history. - Fertile woman without contraceptives. - Coagulation dysfunction. - Pregnant women or lactating women. - Participated in other clinical trials or admitted with other research drugs within 3 months prior to the trial. - Any surgical or medical condition which can significantly alter the absorption, distribution, metabolism, or excretion of any study drug. - Allergy or any contraindications for the study drugs, contrast agents and alcohol. - Refused to sign informed consent |
Country | Name | City | State |
---|---|---|---|
China | The third hospital affiliated to the Third Military Medical University | Chongqing | Chongqing |
Lead Sponsor | Collaborator |
---|---|
Third Military Medical University |
China,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | Change of sex hormones measured at baseline and the end of the trial | Difference in the change of 17-OH, DHEAS, testosterone and estrogen levels between the intervention and control group is to be analysed. | 24 weeks | |
Other | Change of 24-h urine microalbumin measured at baseline and the end of the trial | Difference in the change of 24-h urine microalbumin, microalbumin/creatinine ratio between the intervention and control group is to be analysed. | 24 weeks | |
Other | Change of echocardiography measured at baseline and the end of the trial | Difference in the change of cardiac parameters assessed by echocardiography (IVSd?IVSs?LVPWd, LVPWs, LVEDD, in millimetre(mm), and LVEF(%), LVM in gram) between the intervention and control group is to be analysed. | 24 weeks | |
Other | Change of carotid intima-media thickness assessed by carotid ultrasound at baseline and the end of the trial | Difference in the change of carotid intima-media thickness(CIMT) assessed by carotid ultrasound between the intervention and control group is to be analysed. | 24 weeks | |
Primary | Change of 24-h average systolic blood pressure measured at baseline and the end of the trial | Difference in the change of 24-h average systolic blood pressure between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of 24-h average systolic blood pressure compared with the baseline | Change of 24-h average systolic blood pressure compared with the baseline at the end of the study (24 weeks) in the intervention group. | 24 weeks | |
Secondary | Change of anti-hypertensive regimen measured at baseline and the end of the trial | Difference in the change of anti-hypertensive regimen between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of 24-h average diastolic blood pressure, daytime mean systolic blood pressure, daytime mean diastolic blood pressure, and nighttime average systolic and diastolic blood pressure measured at baseline and the end of the trial | Difference in the change of 24-h average diastolic blood pressure, daytime mean systolic blood pressure, daytime mean diastolic blood pressure, and nighttime average systolic and diastolic blood pressure between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of home systolic and diastolic pressure measured at baseline and the end of the trial | Difference in the change of home systolic and diastolic pressure between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of office systolic and diastolic pressure measured at baseline and the end of the trial | Difference in the change of office systolic and diastolic pressure between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of blood electrolytes measured at baseline and the end of the trial | Difference in the change of blood electrolytes between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of plasma and urine adrenal hormones measured at baseline and the end of the trial | Difference in the change of plasma and urine adrenal hormones between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of plasma renin measured at baseline and the end of the trial | Difference in the change of plasma renin between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of liver enzymes measured at baseline and the end of the trial | Difference in the change of liver enzymes (ALT, AST in IU/L) between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of kidney function measured at baseline and the end of the trial | Difference in the change of serum creatinine in umol/L between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of fasting blood glucose measured at baseline and the end of the trial | Difference in the change of fasting blood glucose in mmol/L between the intervention and control group is to be analysed. | 24 weeks | |
Secondary | Change of lipids profiles measured at baseline and the end of the trial | Difference in the change of lipids profiles (TC, HDL-C, LDL-C, TG) in mmol/L between the intervention and control group is to be analysed. | 24 weeks |
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