A Study to Evaluate the Efficacy and Safety of LCI699 Compared to Placebo in Participants With Resistant Hypertension

Hypertension Clinical Trial

Official title:

A Phase II, Randomized, Double-blind, Placebo and Active Controlled, Parallel Group, Multi-center, Dose Ranging Study to Evaluate the Efficacy and Safety of LCI699 Compared to Placebo After 8 Weeks Treatment in Patients With Resistant Hypertension

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT00817635
• Other study ID #: CLCI699A2216
• Secondary ID: 2008-007338-23
• Status: Completed
• Phase: Phase 2
• Start date: December 22, 2008
• Est. completion date: October 13, 2009

Study information

• Verified date: May 2021
• Source: Novartis
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

This study assessed the blood pressure effect, safety and tolerability of LCI699 compared to placebo and eplerenone in participants with resistant hypertension.

Recruitment information / eligibility

• Status: Completed
• Enrollment: 155
• Est. completion date: October 13, 2009
• Est. primary completion date: October 13, 2009
• Accepts healthy volunteers: No
• Gender: All
• Age group: 18 Years to 75 Years

Eligibility

Inclusion criteria:

• Diagnosis of hypertension with mean sitting systolic blood pressure (MSSBP) =140 millimeters of mercury (mmHg) and <180 mmHg

• Stable on a three-drug regimen (including a diuretic) for at least 4 weeks for the treatment of resistant hypertension

• Male and female participants 18 to 75 years of age

Exclusion criteria:

• Recent history of myocardial infarction (MI), heart failure, unstable angina, coronary artery bypass graft, percutaneous coronary intervention, hypertensive encephalopathy, cerebrovascular accident, or transient ischemic attack

• Clinically significant electrocardiography (ECG) findings related to cardiac conduction defects

• Type 1 diabetes or uncontrolled type 2 diabetes (haemoglobin A1c [HbA1c] >9%)

• Malignancies within the last 5 years (excluding basal cell skin cancer)

Other protocol-defined inclusion/exclusion criteria may apply.

Related Conditions & MeSH terms

• Hypertension

Intervention

Drug:
• LCI699
LCI699 oral capsules
• Eplerenone
Eplerenone oral capsules
• LCI699-matching Placebo
LCI699-matching placebo oral capsules
• Eplerenone-matching Placebo
Eplerenone-matching placebo oral capsules

Locations

Country	Name	City	State
Iceland	Encode Clinic	Reykjavik	SA
United States	Provident Clinical Research	Addison	Illinois
United States	Peter A. Holt	Baltimore	Maryland
United States	Provident Clinical Research	Bloomington	Indiana
United States	Northwest Clinical Trials	Boise	Idaho
United States	Meridien Research	Bradenton	Florida
United States	Clinical Solutions Advantage	Buena Park	California
United States	Daniel Gottlieb, MD	Burien	Washington
United States	Punzi Medical Center	Carrollton	Texas
United States	Medical Research South	Charleston	South Carolina
United States	Charlotte Clinical Research	Charlotte	North Carolina
United States	Chelsea Internal Medicine	Chelsea	Michigan
United States	Cedar-Crosse Research Centereet	Chicago	Illinois
United States	Community Research	Cincinnati	Ohio
United States	Clinical Research of So. Florida	Coral Gables	Florida
United States	KRK Medical Research	Dallas	Texas
United States	Mountain View Clinical Research Associates	Greer	South Carolina
United States	Michael Waldman, MD	Irvine	California
United States	Jacksonville Heart Center	Jacksonville Beach	Florida
United States	FPA Clinical Research	Kissimmee	Florida
United States	Northstate Clinical Research	Lenoir	North Carolina
United States	Metro Clinical Research	Littleton	Colorado
United States	Long Beach Center for Clinical Research	Long Beach	California
United States	DCOL Center for Clinical Research	Longview	Texas
United States	Gemini Scientific	Madison	Wisconsin
United States	Accelovance	Melbourne	Florida
United States	Horizon Research Group, Inc	Mobile	Alabama
United States	Clinical Research Associates, Inc	Nashville	Tennessee
United States	New York Cardiovascular Associates	New York	New York
United States	MD Medical Research	Oxon Hill	Maryland
United States	Cardio-Pulminary Associates	Plantation	Florida
United States	Rainier Clinical Research Center	Renton	Washington
United States	Clinical Trials Research	Roseville	California
United States	Meridien Research	Saint Petersburg	Florida
United States	Cochise Clinical Research	Sierra Vista	Arizona
United States	Accelovance	South Bend	Indiana
United States	Tipton Medical & Diagnostic Center	Tipton	Pennsylvania
United States	Orange County Research Center	Tustin	California

Sponsors (3)

Lead Sponsor	Collaborator
Novartis	Great Lakes Drug Development, Inc., Integrium

Countries where clinical trial is conducted

United States,  Iceland, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Change From Baseline in MSSBP at Week 8 Last Observation Carried Forward (LOCF)	Arterial blood pressure (BP) determinations were made after the participant was in the sitting position for 5 minutes according to the American Heart Association guidelines using a calibrated standard aneroid or mercury sphygmomanometer or a calibrated standard sphygmomanometer. The change in the MSSBP was calculated comparing the Week 8 readings to the readings taken at Baseline. The change from Baseline in MSSBP was analyzed using an analysis of covariance model (ANCOVA) with treatment and country as factors and Baseline MSSBP as a covariate.	Baseline, Week 8
Secondary	Change From Baseline in MSDBP at Week 8 LOCF	Arterial BP determinations were made after the participant was in the sitting position for 5 minutes according to the American Heart Association guidelines using a calibrated standard aneroid or mercury sphygmomanometer or a calibrated standard sphygmomanometer. The change in the MSDBP was calculated comparing the Week 8 readings to the readings taken at Baseline. The change from Baseline in MSDBP was analyzed using an ANCOVA with treatment and country as factors and Baseline MSDBP as a covariate.	Baseline, Week 8
Secondary	Percentage of Participants With a MSSBP Response and MSSBP Control at Week 8, as Measured by Office Blood Pressure (OBP)	MSSBP response was defined as the percentage of participants with a MSSBP <140 mmHg or a >=20 mmHg reduction from baseline reduction from baseline. MSSBP control was defined as the percentage of participants with a MSSBP <140 mmHg for non-diabetic participants and <130mHg for diabetic participants.	Week 8
Secondary	Percentage of Participants With a MSDBP Response and MSDBP Control at Week 8, as Measured by OBP	MSDBP response was defined as the percentage of participants with a MSDBP <90 mmHg or a >=10 mmHg reduction from baseline. MSDBP control was defined as the percentage of participants with a MSDBP <90 mmHg for non-diabetic participants and <80mHg for diabetic participants.	Week 8
Secondary	Dose/Exposure BP Response Relationship of LCI699, as Measured by Change From Baseline in MSSBP at Week 8	Arterial BP determinations were made after the participant was in the sitting position for 5 minutes according to the American Heart Association guidelines using a calibrated standard aneroid or mercury sphygmomanometer or a calibrated standard sphygmomanometer. The change in the MSSBP was calculated comparing the Week 8 readings to the readings taken at Baseline. The change from Baseline in MSSBP was analyzed using an ANCOVA with treatment and country as factors and Baseline MSSBP as a covariate.	Baseline, Week 8
Secondary	Dose/Exposure BP Response Relationship of LCI699, as Measured by Change From Baseline in MSDBP at Week 8	Arterial BP determinations were made after the participant was in the sitting position for 5 minutes according to the American Heart Association guidelines using a calibrated standard aneroid or mercury sphygmomanometer or a calibrated standard sphygmomanometer. The change in the MSDBP was calculated comparing the Week 8 readings to the readings taken at Baseline. The change from Baseline in MSDBP was analyzed using an ANCOVA with treatment and country as factors and Baseline MSDBP as a covariate.	Baseline, Week 8
Secondary	Change From Baseline in Mean 24 Hours, Mean Daytime and Mean Nighttime Systolic Blood Pressure (SBP) at Week 8 LOCF, as Measured by Ambulatory Blood Pressure Measurement (ABPM)	An ABPM measured a participant's blood pressure over a 24-hour period including daytime and nighttime readings, using an automated validated monitoring device from Baseline to Week 8. The 24-hour SBP was calculated by taking the mean of all ambulatory systolic blood pressure readings for the 24-hour period. The change from Baseline in SBP was analyzed using ANCOVA with treatment and country as factors and Baseline MSSBP as a covariate.	Baseline, Week 8
Secondary	Change From Baseline in Mean 24 Hours, Mean Daytime and Mean Nighttime Diastolic Blood Pressure (DBP) at Week 8 LOCF, as Measured by ABPM	An ABPM measured a participant's blood pressure over a 24-hour period including daytime and nighttime readings, using an automated validated monitoring device from Baseline to Week 8. The 24-hour DBP was calculated by taking the mean of all ambulatory diastolic blood pressure readings for the 24-hour period. The change from Baseline in DBP was analyzed using an ANCOVA with treatment and country as factors and Baseline MSDBP as a covariate.	Baseline, Week 8
Secondary	Change From Baseline in Mean 24 Hours, Mean Daytime and Mean Nighttime SBP in LCI699 1mg QD Versus LCI699 0.5mg BID Arm at Week 4, as Measured by ABPM	An ABPM measured a participant's blood pressure over a 24-hour period including daytime and nighttime readings using an automated validated monitoring device from Baseline to Week 4. The 24-hour SBP was calculated by taking the mean of all ambulatory systolic blood pressure readings for the 24-hour period. The change from Baseline in SBP was analyzed using an ANCOVA with treatment and country as factors and Baseline MSDBP as a covariate.	Baseline, Week 4
Secondary	Change From Baseline in Mean 24 Hours, Mean Daytime and Mean Nighttime DBP in LCI699 1mg QD Versus LCI699 0.5mg BID Arm at Week 4, as Measured by ABPM	An ABPM measured a participant's blood pressure over a 24-hour period including daytime and nighttime readings using an automated validated monitoring device from Baseline to Week 4. The 24-hour DBP was calculated by taking the mean of all ambulatory diastolic blood pressure readings for the 24-hour period. The change from Baseline in DBP was analyzed using an ANCOVA with treatment and country as factors and Baseline MSDBP as a covariate.	Baseline, Week 4
Secondary	Number of Participants With Adverse Event (AEs), Serious Adverse Events (SAEs), Hyperkalemia, and Hyponatremia	An AE was an adverse medical event which occurs in a participant of the study and which is not necessarily in a causal relationship with the treatment the participant receives. SAEs were AEs leading to death, are life-threatening, require hospitalizations or prolongation of hospitalizations, represent an innate malformation or a congenital abnormality. Hyperkalemia was defined as potassium level >5.5 millimoles per liter (mmol/L). It is the medical term that describes a potassium level that's higher than normal. Hyponatremia was defined as sodium level <135 mmol/L. It is the medical term that describes a sodium level that's lesser than normal.	AEs, Hyperkalemia, and Hyponatremia: From start of the study drug treatment up to 10 weeks; SAE: From signing of the informed consent up to 10 weeks
Secondary	Number of Participants With Cortisol Levels Below 500 Nmol/L at 1 Hour After Adrenocorticotropic Hormone (ACTH) Injection at Week 8	Serum cortisol concentrations at 1 hour after injection were measured to assess the maximum stimulated cortisol level achieved. Potential adrenal suppression was indicated if the serum cortisol concentration was <500 nanomoles per liter (nmol/L) at 1 hour after the injection.	1-hour post-dose at Week 8
Secondary	Percent Change From Baseline in Renin-Angiotensin-Aldosterone-System (RAAS) Biomarker: Plasma Aldosterone (PA) in LCI699 Compared to Eplerenone 50 mg at Week 8 LOCF	Percent change from Baseline was analyzed by ANCOVA model using PA values measured at Baseline and Week 8 LOCF, with treatment and country as factors and Baseline value as the covariate. Negative percent change from Baseline shows improvement.	Baseline, Week 8
Secondary	Percent Change From Baseline in RAAS Biomarker: Plasma Renin Activity (PRA) in LCI699 Compared to Eplerenone 50mg at Week 8 LOCF	Percent change from Baseline was analyzed by ANCOVA model using plasma renin values measured at Baseline and Week 8 LOCF, with treatment and country as factors and Baseline value as the covariate. Negative percent change from Baseline shows improvement.	Baseline, Week 8
Secondary	Percent Change From Baseline in RAAS Biomarker: Active Renin (ARC) in LCI699 Compared to Eplerenone 50mg at Week 8 LOCF	Percent change from Baseline was analyzed by ANCOVA model using active renin values measured at Baseline and Week 8 LOCF, with treatment and country as factors and Baseline value as the covariate. Negative percent change from Baseline shows improvement.	Baseline, Week 8
Secondary	Percent Change From Baseline in RAAS Biomarker: Ratio of PA to PRA in LCI699 Compared to Eplerenone 50mg at Week 8 LOCF	Percent change from Baseline was analyzed by ANCOVA model using percent ratio of PA to PRA values measured at Baseline and Week 8 LOCF, with treatment and country as factors and Baseline value as the covariate. Negative percent change from Baseline shows improvement.	Baseline, Week 8