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A Research Study to Show the Effect of Aprocitentan in the Treatment of Difficult to Control (Resistant) High Blood Pressure (Hypertension) and Find Out More About Its Safety (PRECISION)

The safety and scientific validity of this study is the responsibility of the study sponsor and investigators. Listing a study does not mean it has been evaluated by the U.S. Federal Government. Read our disclaimer for details.
 
ClinicalTrials.gov Identifier: NCT03541174
Recruitment Status : Completed
First Posted : May 30, 2018
Results First Posted : March 21, 2023
Last Update Posted : March 21, 2023
Sponsor:
Collaborator:
Janssen Biotech, Inc.
Information provided by (Responsible Party):
Idorsia Pharmaceuticals Ltd.

Study Type Interventional
Study Design Allocation: Randomized;   Intervention Model: Parallel Assignment;   Masking: Triple (Participant, Care Provider, Investigator);   Primary Purpose: Treatment
Condition Resistant Hypertension
Interventions Drug: Aprocitentan 12.5 mg
Drug: Aprocitentan 25 mg
Drug: Placebo
Enrollment 730
Recruitment Details The study was done from 18 June 2018 to 25 April 2022.
Pre-assignment Details 730 participants are considered to be enrolled in the study and were randomized to study treatment.
Arm/Group Title Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind) Aprocitentan 25 mg in Part 2 (Single-blind) Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Hide Arm/Group Description Participants were randomized and received aprocitentan 12.5 mg, orally, once daily in the morning for 4 weeks. Participants were randomized and received aprocitentan 25 mg, orally, once daily in the morning for 4 weeks. Participants were randomized and received placebo (matching aprocitentan), orally, once daily in the morning for 4 weeks. Participants that completed the double-blind part received aprocitentan 25 mg, orally, once daily in the morning for 32 weeks. After the 32-week single-blind, single-arm aprocitentan 25 mg (Part 2), participants were re-randomized and received aprocitentan 25 mg, orally, once daily in the morning for 12 weeks. After the 32-week single-blind, single-arm aprocitentan 25 mg (Part 2), participants were re-randomized and received placebo (matching aprocitentan), orally, once daily in the morning for 12 weeks.
Period Title: Part 1 Double-Blind
Started 243 243 244 0 0 0
Safety Set [1] 243 245 242 0 0 0
Completed 232 234 238 0 0 0
Not Completed 11 9 6 0 0 0
Reason Not Completed
Adverse Event             6             5             2             0             0             0
Withdrawal by Subject             2             2             1             0             0             0
Other reasons             3             2             3             0             0             0
[1]
Two participants randomized to placebo received at least one dose of aprocitentan 25 mg during double-blind part 1.
Period Title: Part 2 Single-Blind
Started 0 [1] 0 [2] 0 [3] 704 [4] 0 0
Completed 0 0 0 613 0 0
Not Completed 0 0 0 91 0 0
Reason Not Completed
Adverse Event             0             0             0             25             0             0
Lack of Efficacy             0             0             0             1             0             0
Withdrawal by Subject             0             0             0             19             0             0
Lost to Follow-up             0             0             0             8             0             0
Death             0             0             0             5             0             0
Pregnancy             0             0             0             1             0             0
Other reasons             0             0             0             32             0             0
[1]
The 232 participants that completed 12.5 mg aprocitentan study treatment in part 1 entered the single-blind 25 mg aprocitentan arm in part 2.
[2]
The 236 participants that completed 25 mg aprocitentan study treatment in part 1 entered the single-blind 25 mg aprocitentan arm in part 2.
[3]
The 236 participants that completed placebo study treatment in part 1 entered the single-blind 25 mg aprocitentan arm in part 2.
[4]
Total number of participants that completed the double-blind part 1 who entered the single-blind, single-arm part 2.
Period Title: Part 3 Double-Blind Withdrawal
Started 0 0 0 0 307 307
Safety Set [1] 0 0 0 0 310 303
Completed 0 0 0 0 288 289
Not Completed 0 0 0 0 19 18
Reason Not Completed
Adverse Event             0             0             0             0             8             7
Withdrawal by Subject             0             0             0             0             1             4
Lost to Follow-up             0             0             0             0             0             1
Other reasons             0             0             0             0             9             6
Re-randomized in part 3, however no drug dispensed             0             0             0             0             1             0
[1]
613 participants started study treatment in Part 3. Four participants re-randomised to placebo received at least one dose of aprocitentan 25 mg during part 3.
Arm/Group Title Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind) Total
Hide Arm/Group Description Participants randomized to aprocitentan 12.5 mg, orally, once daily in the morning for 4 weeks. Participants randomized to aprocitentan 25 mg, orally, once daily in the morning for 4 weeks. Participants randomized to placebo (matching aprocitentan), orally, once daily in the morning for 4 weeks. Total of all reporting groups
Overall Number of Baseline Participants 243 243 244 730
Hide Baseline Analysis Population Description
[Not Specified]
Age, Continuous  
Mean (Standard Deviation)
Unit of measure:  Years
Number Analyzed 243 participants 243 participants 244 participants 730 participants
61.2  (10.3) 61.7  (10.4) 62.2  (11.2) 61.7  (10.6)
Sex: Female, Male  
Measure Type: Count of Participants
Unit of measure:  Participants
Number Analyzed 243 participants 243 participants 244 participants 730 participants
Female 99 98 99 296
Male 144 145 145 434
Ethnicity (NIH/OMB)  
Measure Type: Count of Participants
Unit of measure:  Participants
Number Analyzed 243 participants 243 participants 244 participants 730 participants
Hispanic or Latino 28 22 23 73
Not Hispanic or Latino 213 219 218 650
Unknown or Not Reported 2 2 3 7
Race (NIH/OMB)  
Measure Type: Count of Participants
Unit of measure:  Participants
Number Analyzed 243 participants 243 participants 244 participants 730 participants
American Indian or Alaska Native 0 0 0 0
Asian 11 14 13 38
Native Hawaiian or Other Pacific Islander 1 0 0 1
Black or African American 28 28 26 82
White 203 200 202 605
More than one race 0 0 0 0
Unknown or Not Reported 0 1 3 4
Region of Enrollment  
Measure Type: Number
Unit of measure:  Participants
 Number Analyzed 243 participants 243 participants 244 participants 730 participants
Australia 8 8 7 23
Belgium 1 3 4 8
Canada 8 7 6 21
China 6 11 10 27
Czechia 10 3 15 28
Finland 9 5 2 16
France 0 4 3 7
Germany 3 6 9 18
Greece 5 1 2 8
Hungary 1 4 1 6
Israel 5 2 3 10
Italy 3 2 0 5
Lithuania 2 4 4 10
Netherlands 2 3 3 8
Poland 15 16 20 51
Russia 61 56 49 166
Spain 4 8 6 18
Ukraine 30 26 30 86
United Kingdom 2 0 1 3
United States 68 74 69 211
Body Mass Index at Screening Visit  
Mean (Standard Deviation)
Unit of measure:  Kg/m^2
Number Analyzed 243 participants 243 participants 244 participants 730 participants
33.6  (6.2) 34.3  (6.8) 33.3  (5.6) 33.7  (6.2)
1.Primary Outcome
Title Change From Baseline to Week 4 of Double-blind Treatment in Mean Trough Sitting Systolic Blood Pressure (SiSBP) Measured by Automated Office Blood Pressure Measurement
Hide Description Changes from baseline to Week 4 in mean trough SiSBP were analyzed using a mixed model. Participants had their blood pressure (BP) measured at the study site using the automated oscillometric sphygmomanometer (Microlife WatchBP® Office) which was provided to each site. BP was to be measured at trough (before taking the study treatment and SBAT). The BP assessment, participant preparation (e.g., arm selection, arm position, cuff size) was standardized and followed the American Heart Association guidelines / Canadian Education Program on Hypertension. The participant was resting undisturbed, alone (unattended) in a quiet place for 5 minutes at each visit. BP was measured at each visit with the same device, which recorded five sitting blood pressure readings (one per minute, the first value was excluded from the average). A negative change indicates a decrease in SiSBP from baseline.
Time Frame Pre-dose Day 1 (Part 1 double-blind randomized baseline) up to Week 4 (End of double-blind randomized part 1)
Hide Outcome Measure Data
Hide Analysis Population Description
The Full Analysis Set (FAS) includes all participants who were randomized and had a baseline sitting systolic blood pressure, measured by automated office blood pressure measurement. Baseline was defined as the last measurement before randomization.
Arm/Group Title Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind)
Hide Arm/Group Description:
Participants randomized to aprocitentan 12.5 mg, orally, once daily in the morning for 4 weeks.
Participants randomized to aprocitentan 25 mg, orally, once daily in the morning for 4 weeks.
Participants randomized to placebo (matching aprocitentan), orally, once daily in the morning for 4 weeks.
Overall Number of Participants Analyzed 243 243 244
Least Squares Mean (97.5% Confidence Interval)
Unit of Measure: mmHg
-15.26
(-17.36 to -13.17)
-15.20
(-17.27 to -13.13)
-11.47
(-13.57 to -9.38)
Hide Statistical Analysis 1
Statistical Analysis Overview Comparison Group Selection Aprocitentan 12.5 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments [Not Specified]
Type of Statistical Test Superiority
Comments [Not Specified]
Statistical Test of Hypothesis P-Value 0.0042
Comments Mixed effects model for Repeated Measures: Change from baseline in SiSBP = baseline SiSBP + treatment + visit + treatment x visit + baseline x visit.
Method Mixed Models Analysis
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -3.79
Confidence Interval (2-Sided) 97.5%
-6.76 to -0.82
Estimation Comments [Not Specified]
Hide Statistical Analysis 2
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments [Not Specified]
Type of Statistical Test Superiority
Comments [Not Specified]
Statistical Test of Hypothesis P-Value 0.0046
Comments Mixed effects model for Repeated Measures: Change from baseline in SiSBP = baseline SiSBP + treatment + visit + treatment x visit + baseline x visit.
Method Mixed Models Analysis
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -3.73
Confidence Interval (2-Sided) 97.5%
-6.67 to -0.78
Estimation Comments [Not Specified]
2.Secondary Outcome
Title Change From Double-blind Withdrawal Baseline (Week 36) to Week 40 in Mean Trough Sitting Systolic Blood Pressure (SiSBP) Measured by Unattended Automated Office Blood Pressure Measurement
Hide Description Changes from double-blind withdrawal baseline (Week 36) to Week 40 in mean trough SiSBP were analyzed using a mixed model. Participants had their blood pressure (BP) measured at the study site using the automated oscillometric sphygmomanometer (Microlife WatchBP® Office) which was provided to each site. BP was to be measured at trough (before taking the study treatment and SBAT). The BP assessment, participant preparation (e.g., arm selection, arm position, cuff size) was standardized and followed the American Heart Association guidelines / Canadian Education Program on Hypertension. The participant was resting undisturbed, alone (unattended) in a quiet place for 5 minutes at each visit. BP was measured at each visit with the same device, which recorded five sitting blood pressure readings (one per minute, the first value was excluded from the average). A negative change indicates a decrease in SiSBP from baseline.
Time Frame Pre-dose Week 36 (Part 3 double-blind-withdrawal baseline) up to Week 40
Hide Outcome Measure Data
Hide Analysis Population Description
The modified FAS (mFAS) includes all participants from the FAS who were re-randomized in the double-blind-withdrawal part (DB-WD) of the study and who have a DB-WD baseline sitting systolic blood pressure, measured by automatic office blood pressure measurement device at trough. Baseline was defined as the last measurement before re-randomization.
Arm/Group Title Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Hide Arm/Group Description:
After 32-weeks in the single-blind, single-arm part, participants were re-randomized to aprocitentan 25 mg, orally, once daily in the morning for 12 weeks.
After 32-weeks in the single-blind, single-arm part, participants were re-randomized to placebo (matching aprocitentan), orally, once daily in the morning for 12 weeks.
Overall Number of Participants Analyzed 307 307
Least Squares Mean (95% Confidence Interval)
Unit of Measure: mmHg
-1.47
(-2.97 to 0.04)
4.36
(2.87 to 5.85)
Hide Statistical Analysis 1
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal), Placebo in Part 3 (Double-blind Withdrawal)
Comments [Not Specified]
Type of Statistical Test Superiority
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments Mixed effects model for Repeated Measures: Change from DB-WD baseline in SiSBP = DB-WD baseline SiSBP + stratum (randomized treatment in DB part) + treatment + visit + treatment x visit + DB-WD baseline x visit.
Method Mixed Models Analysis
Comments [Not Specified]
Method of Estimation Estimation Parameter LS mean difference to placebo.
Estimated Value -5.82
Confidence Interval (2-Sided) 95%
-7.94 to -3.71
Estimation Comments [Not Specified]
3.Secondary Outcome
Title Change From Baseline to Week 4 of Double-blind Treatment in Mean Trough Sitting Diastolic Blood Pressure (SiDBP) Measured by Unattended Automated Office Blood Pressure Measurement
Hide Description Changes from baseline to Week 4 in mean trough SiDBP were analyzed using a mixed model. Participants had their blood pressure (BP) measured at the study site using the automated oscillometric sphygmomanometer (Microlife WatchBP® Office) which was provided to each site. BP was to be measured at trough (before taking the study treatment and SBAT). The BP assessment, participant preparation (e.g., arm selection, arm position, cuff size) was standardized and followed the American Heart Association guidelines / Canadian Education Program on Hypertension. BP was measured at each visit with the same device, which recorded five sitting blood pressure readings (one per minute, the first value was excluded from the average). The participant was resting undisturbed, alone (unattended) in a quiet place for 5 minutes at each visit. A negative change indicates a decrease in SiDBP from baseline.
Time Frame Pre-dose Day 1 (Part 1 double-blind randomized baseline) up to Week 4 (End of double-blind randomized part 1)
Hide Outcome Measure Data
Hide Analysis Population Description
The Full Analysis Set (FAS) includes all participants who were randomized and had a baseline sitting systolic blood pressure, measured by automated office blood pressure measurement. Baseline was defined as the last measurement before randomization.
Arm/Group Title Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind)
Hide Arm/Group Description:
Participants randomized to aprocitentan 12.5 mg, orally, once daily in the morning for 4 weeks.
Participants randomized to aprocitentan 25 mg, orally, once daily in the morning for 4 weeks.
Participants randomized to placebo (matching aprocitentan), orally, once daily in the morning for 4 weeks.
Overall Number of Participants Analyzed 243 243 244
Least Squares Mean (95% Confidence Interval)
Unit of Measure: mmHg
-10.43
(-11.58 to -9.27)
-10.95
(-12.09 to -9.82)
-6.48
(-7.63 to -5.33)
Hide Statistical Analysis 1
Statistical Analysis Overview Comparison Group Selection Aprocitentan 12.5 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments [Not Specified]
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments Mixed effects model for Repeated Measures: Change from baseline in SiDBP = baseline SiDBP + treatment + visit + treatment x visit + baseline x visit.
Method Mixed Models Analysis
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -3.94
Confidence Interval (2-Sided) 95%
-5.57 to -2.31
Estimation Comments [Not Specified]
Hide Statistical Analysis 2
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments [Not Specified]
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments Mixed effects model for Repeated Measures: Change from baseline in SiDBP = baseline SiDBP + treatment + visit + treatment x visit + baseline x visit.
Method Mixed Models Analysis
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -4.47
Confidence Interval (2-Sided) 95%
-6.09 to -2.85
Estimation Comments [Not Specified]
4.Secondary Outcome
Title Changes From Baseline to Week 4 of Double-blind Treatment in 24-hour Mean Systolic (SBP) and Diastolic Blood Pressure (DBP) Measured by Ambulatory Blood Pressure Monitoring
Hide Description ABPM devices were provided to each site by the central blood pressure laboratory. On the first day after all visit assessments were performed, the ABPM device (Mobil-O-Graph NG) was fitted to the participant. The following day (i.e., second day), the participant came back to site to have the ABPM device removed. ABPM data collected over the 24-hours was electronically transferred to the central BP laboratory. Systolic blood pressure and diastolic blood pressure were measured at predetermined times every 20 minutes from 06:00 to 21:59, and every 30 minutes from 22:00 to 05:59. For each participant and at each visit (baseline and Week 4) the 24-hour mean SBP (or DBP) was calculated from the area under the SBP (or DBP) time curve and divided by the time span. A negative change indicates a decrease in 24-hour mean systolic / diastolic blood pressure from baseline.
Time Frame Pre-dose Day 1 (Part 1 double-blind randomized baseline) and Week 4 (End of double-blind randomized part 1)
Hide Outcome Measure Data
Hide Analysis Population Description
The ambulatory blood pressure monitoring full analysis set (aFAS) includes all participants from the FAS who have a baseline 24-hour mean systolic and diastolic blood pressure measured by ambulatory blood pressure monitoring with a total duration of at least 21 hours and at least 70% valid readings.
Arm/Group Title Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind)
Hide Arm/Group Description:
Participants randomized to aprocitentan 12.5 mg, orally, once daily in the morning for 4 weeks.
Participants randomized to aprocitentan 25 mg, orally, once daily in the morning for 4 weeks.
Participants randomized to placebo (matching aprocitentan), orally, once daily in the morning for 4 weeks.
Overall Number of Participants Analyzed 206 207 220
Least Squares Mean (95% Confidence Interval)
Unit of Measure: mmHg
24-hour mean systolic blood pressure
-6.73
(-8.20 to -5.26)
-8.44
(-9.88 to -7.00)
-2.55
(-4.00 to -1.10)
24-hour mean diastolic blood pressure
-6.25
(-7.20 to -5.29)
-7.74
(-8.67 to -6.80)
-1.92
(-2.87 to -0.98)
Hide Statistical Analysis 1
Statistical Analysis Overview Comparison Group Selection Aprocitentan 12.5 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments 24-hour mean systolic (SBP)
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments [Not Specified]
Method ANCOVA
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -4.18
Confidence Interval (2-Sided) 95%
-6.25 to -2.12
Estimation Comments [Not Specified]
Hide Statistical Analysis 2
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments 24-hour mean systolic (SBP)
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments [Not Specified]
Method ANCOVA
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -5.90
Confidence Interval (2-Sided) 95%
-7.94 to -3.85
Estimation Comments [Not Specified]
Hide Statistical Analysis 3
Statistical Analysis Overview Comparison Group Selection Aprocitentan 12.5 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments 24-hour mean diastolic (DBP)
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments [Not Specified]
Method ANCOVA
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -4.32
Confidence Interval (2-Sided) 95%
-5.66 to -2.98
Estimation Comments [Not Specified]
Hide Statistical Analysis 4
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 1 (Double-blind), Placebo in Part 1 (Double-blind)
Comments 24-hour mean diastolic (DBP)
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments [Not Specified]
Method ANCOVA
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean
Estimated Value -5.81
Confidence Interval (2-Sided) 95%
-7.14 to -4.49
Estimation Comments [Not Specified]
5.Secondary Outcome
Title Change From Double-blind Withdrawal Baseline (Week 36) to Week 40 of Double-blind-withdrawal (DB-WD) Treatment in Trough Sitting Diastolic Blood Pressure (SiDBP) Measured by Unattended Automated Office Blood Pressure
Hide Description Changes from double-blind withdrawal (Week 36) to Week 40 in mean trough SiDBP were analyzed using a mixed model. Participants had their blood pressure (BP) measured at the study site using the automated oscillometric sphygmomanometer (Microlife WatchBP® Office) which was provided to each site. BP was to be measured at trough (before taking the study treatment and SBAT). The BP assessment, participant preparation (e.g., arm selection, arm position, cuff size) was standardized and followed the American Heart Association guidelines / Canadian Education Program on Hypertension. The participant was resting undisturbed, alone (unattended) in a quiet place for 5 minutes at each visit. BP was measured at each visit with the same device, which recorded five sitting blood pressure readings (one per minute, the first value was excluded from the average). A negative change indicates a decrease in SiDBP from baseline.
Time Frame Pre-dose Week 36 (Part 3 double-blind-withdrawal baseline) up to Week 40
Hide Outcome Measure Data
Hide Analysis Population Description
The modified FAS (mFAS) includes all participants in the FAS who were re-randomized in the double-blind-withdraw part of the study and who had a week 36 sitting systolic blood pressure, measured by automated office blood pressure measurement. Baseline was defined as the last measurement before re-randomization into part 3 of the double-blind withdrawal part of the study.
Arm/Group Title Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Hide Arm/Group Description:
After 32-weeks in the single-blind, single-arm part, participants were re-randomized to aprocitentan 25 mg, orally, once daily in the morning for 12 weeks.
After 32-weeks in the single-blind, single-arm part, participants were re-randomized to placebo (matching aprocitentan), orally, once daily in the morning for 12 weeks.
Overall Number of Participants Analyzed 307 307
Least Squares Mean (95% Confidence Interval)
Unit of Measure: mmHg
-0.52
(-1.54 to 0.50)
4.67
(3.66 to 5.68)
Hide Statistical Analysis 1
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal), Placebo in Part 3 (Double-blind Withdrawal)
Comments [Not Specified]
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments Mixed effects model for Repeated Measures: Change from DB-WD baseline in SiDBP = Double-blind withdrawal baseline SiDBP + stratum (randomized treatment in DB part) + treatment + visit + treatment x visit + Double-blind withdrawal baseline x visit.
Method Mixed Models Analysis
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -5.19
Confidence Interval (2-Sided) 95%
-6.62 to -3.76
Estimation Comments [Not Specified]
6.Secondary Outcome
Title Changes From Double-blind Withdrawal Baseline (Week 36) to Week 40 of Double-blind-withdrawal (DB-WD) Treatment in 24-hour Mean Systolic (SBP) and Diastolic Blood Pressure (DBP) Measured by Ambulatory Blood Pressure Monitoring
Hide Description ABPM devices were provided to each site by the central blood pressure laboratory. On the first day after all visit assessments were performed, the ABPM device (Mobil-O-Graph NG) was fitted to the participant. The following day (i.e., second day), the participant came back to site to have the ABPM device removed. ABPM data collected over the 24-hours was electronically transferred to the central BP laboratory. Systolic blood pressure and diastolic blood pressure were measured at predetermined times every 20 minutes from 06:00 to 21:59, and every 30 minutes from 22:00 to 05:59. For each participant and at each visit (the double-blind withdrawal baseline [Week 36] and the week 40) the 24-hour mean SBP (or DBP) was calculated from the area under the SBP (or DBP) time curve. A negative change indicates a decrease in 24-hour mean systolic / diastolic blood pressure from baseline.
Time Frame From Week 36 (Part 3 double-blind-withdrawal baseline) and Week 40
Hide Outcome Measure Data
Hide Analysis Population Description
The modified ambulatory blood pressure monitoring full analysis set (maFAS) includes all participants from the modified Full Analysis Set (mFAS) who had a double-blind withdrawal (DB-WD) baseline 24-hour mean systolic and diastolic blood pressure, measured by ambulatory blood Pressure monitoring (ABPM) with a total duration of at least 21 hours and at least 70% valid readings.
Arm/Group Title Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Hide Arm/Group Description:
After 32-weeks in the single-blind, single-arm part, participants were re-randomized to aprocitentan 25 mg, orally, once daily in the morning for 12 weeks.
After 32-weeks in the single-blind, single-arm part, participants were re-randomized to placebo (matching aprocitentan), orally, once daily in the morning for 12 weeks.
Overall Number of Participants Analyzed 237 241
Least Squares Mean (95% Confidence Interval)
Unit of Measure: mmHg
24-hour mean systolic blood pressure
-0.07
(-1.46 to 1.32)
6.46
(5.06 to 7.85)
24-hour mean diastolic blood pressure
-0.47
(-1.34 to 0.40)
6.28
(5.40 to 7.15)
Hide Statistical Analysis 1
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal), Placebo in Part 3 (Double-blind Withdrawal)
Comments 24-hour mean systolic (SBP)
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments [Not Specified]
Method ANCOVA
Comments [Not Specified]
Method of Estimation Estimation Parameter LS Mean difference to placebo
Estimated Value -6.53
Confidence Interval (2-Sided) 95%
-8.50 to -4.56
Estimation Comments [Not Specified]
Hide Statistical Analysis 2
Statistical Analysis Overview Comparison Group Selection Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal), Placebo in Part 3 (Double-blind Withdrawal)
Comments 24-hour mean diastolic (DBP)
Type of Statistical Test Other
Comments [Not Specified]
Statistical Test of Hypothesis P-Value <0.0001
Comments [Not Specified]
Method ANCOVA
Comments [Not Specified]
Method of Estimation Estimation Parameter LSM Mean difference to placebo
Estimated Value -6.75
Confidence Interval (2-Sided) 95%
-7.98 to -5.52
Estimation Comments [Not Specified]
Time Frame Adverse events (AEs) were considered treatment-emergent, if the onset date is between the first intake of treatment up to 30 days after the stop of study treatment. Study treatment was for up to 48 weeks. In Part 1 double-blind (DB) treatment was for 4 weeks. Part 2 single-blind (SB) study treatment was for 32 weeks. In Part 3 double-blind withdrawal (DB-WD) study treatment was for 12 weeks.
Adverse Event Reporting Description Only participants entering the randomized treatment period were considered enrolled for the study and are included in AE analysis. The Run-in period was designed to exclude potential placebo responders and is not part of statistical analysis of this study.
 
Arm/Group Title Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind) Aprocitentan 25 mg in Part 2 (Single-blind) Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Hide Arm/Group Description Participants received aprocitentan 12.5 mg, orally, once daily in the morning for 4 weeks. Participants received aprocitentan 25 mg, orally, once daily in the morning for 4 weeks. Participants received placebo, orally, once daily in the morning for 4 weeks. All participants received aprocitentan 25 mg, orally, once daily in the morning for 32 weeks. After 32-weeks in the single-blind, single-arm part, participants received aprocitentan 25 mg, orally, once daily in the morning for 12 weeks. After 32-weeks in the single-blind, single-arm part, participants received placebo (matching aprocitentan), orally, once daily in the morning for 12 weeks.
All-Cause Mortality
Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind) Aprocitentan 25 mg in Part 2 (Single-blind) Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Affected / at Risk (%) Affected / at Risk (%) Affected / at Risk (%) Affected / at Risk (%) Affected / at Risk (%) Affected / at Risk (%)
Total   1/243 (0.41%)      0/245 (0.00%)      0/242 (0.00%)      9/704 (1.28%)      1/310 (0.32%)      0/303 (0.00%)    
Hide Serious Adverse Events
Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind) Aprocitentan 25 mg in Part 2 (Single-blind) Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events
Total   8/243 (3.29%)      8/245 (3.27%)      3/242 (1.24%)      82/704 (11.65%)      18/310 (5.81%)      9/303 (2.97%)    
Blood and lymphatic system disorders             
Anaemia  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Cardiac disorders             
Acute left ventricular failure  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Acute myocardial infarction  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 2/704 (0.28%)  2 0/310 (0.00%)  0 0/303 (0.00%)  0
Angina unstable  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 5/704 (0.71%)  5 1/310 (0.32%)  1 0/303 (0.00%)  0
Atrial fibrillation  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 3/704 (0.43%)  3 3/310 (0.97%)  3 0/303 (0.00%)  0
Atrioventricular block  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Atrioventricular block second degree  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Cardiac failure  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Cardiac failure acute  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 1/303 (0.33%)  1
Cardiac failure chronic  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Cardiac failure congestive  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 3/704 (0.43%)  3 0/310 (0.00%)  0 0/303 (0.00%)  0
Cardiogenic shock  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Coronary artery disease  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 2/704 (0.28%)  2 0/310 (0.00%)  0 0/303 (0.00%)  0
Coronary artery dissection  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 1/303 (0.33%)  1
Left ventricular dysfunction  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Myocardial infarction  1  1/243 (0.41%)  1 0/245 (0.00%)  0 0/242 (0.00%)  0 2/704 (0.28%)  2 1/310 (0.32%)  1 0/303 (0.00%)  0
Ear and labyrinth disorders             
Meniere's disease  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Vestibular ataxia  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Gastrointestinal disorders             
Gastrointestinal haemorrhage  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Pancreatitis chronic  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Rectal fissure  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Umbilical hernia, obstructive  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Upper gastrointestinal haemorrhage  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
General disorders             
Chest pain  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Death  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Multiple organ dysfunction syndrome  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Oedema peripheral  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Pyrexia  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Sudden cardiac death  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Hepatobiliary disorders             
Cholecystitis acute  1  1/243 (0.41%)  1 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Infections and infestations             
Abscess jaw  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
COVID-19  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
COVID-19 pneumonia  1  2/243 (0.82%)  2 0/245 (0.00%)  0 1/242 (0.41%)  1 14/704 (1.99%)  14 4/310 (1.29%)  4 2/303 (0.66%)  2
Cellulitis  1  0/243 (0.00%)  0 2/245 (0.82%)  2 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Cholecystitis infective  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Diabetic gangrene  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Diverticulitis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Erysipelas  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Gastroenteritis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Peritonsillar abscess  1  0/243 (0.00%)  0 0/245 (0.00%)  0 1/242 (0.41%)  1 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Pneumonia  1  1/243 (0.41%)  1 1/245 (0.41%)  1 0/242 (0.00%)  0 2/704 (0.28%)  2 2/310 (0.65%)  2 0/303 (0.00%)  0
Pneumonia bacterial  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Pyelonephritis acute  1  0/243 (0.00%)  0 0/245 (0.00%)  0 1/242 (0.41%)  1 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Sepsis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 1/242 (0.41%)  1 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Ureteritis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Urinary tract infection  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Wound infection  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Injury, poisoning and procedural complications             
Chest injury  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Procedural intestinal perforation  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Road traffic accident  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Subdural haemorrhage  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Tibia fracture  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Traumatic intracranial haemorrhage  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Investigations             
Blood creatinine increased  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Blood pressure increased  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Metabolism and nutrition disorders             
Hyperkalaemia  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 2/704 (0.28%)  2 0/310 (0.00%)  0 0/303 (0.00%)  0
Hypoglycaemia  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Musculoskeletal and connective tissue disorders             
Musculoskeletal chest pain  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Osteoarthritis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Osteochondrosis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Rotator cuff syndrome  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Neoplasms benign, malignant and unspecified (incl cysts and polyps)             
Adenocarcinoma of colon  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Invasive breast carcinoma  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Lung neoplasm malignant  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Mantle cell lymphoma  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Metastatic neoplasm  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Renal cancer  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 1/303 (0.33%)  1
Renal cell carcinoma  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Nervous system disorders             
Brain oedema  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Cerebral infarction  1  1/243 (0.41%)  1 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Cerebrovascular accident  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 2/704 (0.28%)  2 0/310 (0.00%)  0 0/303 (0.00%)  0
Facial paresis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Haemorrhage intracranial  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 1/303 (0.33%)  1
Ischaemic stroke  1  1/243 (0.41%)  1 0/245 (0.00%)  0 1/242 (0.41%)  1 0/704 (0.00%)  0 0/310 (0.00%)  0 1/303 (0.33%)  1
Seizure  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Syncope  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 2/704 (0.28%)  2 0/310 (0.00%)  0 0/303 (0.00%)  0
Transient ischaemic attack  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 1/310 (0.32%)  1 0/303 (0.00%)  0
Renal and urinary disorders             
Acute kidney injury  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Calculus urinary  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 2/704 (0.28%)  2 0/310 (0.00%)  0 0/303 (0.00%)  0
Nephropathy toxic  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Ureteric stenosis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  2 0/310 (0.00%)  0 0/303 (0.00%)  0
Reproductive system and breast disorders             
Endometrial hyperplasia  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 1/303 (0.33%)  1
Uterine polyp  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Respiratory, thoracic and mediastinal disorders             
Asthma  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Dyspnoea  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 1/310 (0.32%)  1 0/303 (0.00%)  0
Pulmonary embolism  1  1/243 (0.41%)  1 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Pulmonary oedema  1  0/243 (0.00%)  0 1/245 (0.41%)  1 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Respiratory failure  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Skin and subcutaneous tissue disorders             
Angioedema  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 1/303 (0.33%)  1
Dermatitis allergic  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Skin ulcer  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Surgical and medical procedures             
Coronary artery bypass  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Hip arthroplasty  1  1/243 (0.41%)  1 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 0/310 (0.00%)  0 0/303 (0.00%)  0
Peripheral artery bypass  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Toe amputation  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Vascular disorders             
Aortic stenosis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Deep vein thrombosis  1  1/243 (0.41%)  1 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Distributive shock  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Hypertension  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 0/704 (0.00%)  0 1/310 (0.32%)  1 0/303 (0.00%)  0
Hypertensive crisis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Hypertensive urgency  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Hypotension  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Intermittent claudication  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
Peripheral artery stenosis  1  0/243 (0.00%)  0 0/245 (0.00%)  0 0/242 (0.00%)  0 1/704 (0.14%)  1 0/310 (0.00%)  0 0/303 (0.00%)  0
1
Term from vocabulary, MedDRA (24.1)
Indicates events were collected by systematic assessment
Hide Other (Not Including Serious) Adverse Events
Frequency Threshold for Reporting Other Adverse Events 5%
Aprocitentan 12.5 mg in Part 1 (Double-blind) Aprocitentan 25 mg in Part 1 (Double-blind) Placebo in Part 1 (Double-blind) Aprocitentan 25 mg in Part 2 (Single-blind) Aprocitentan 25 mg in Part 3 (Double-blind Withdrawal) Placebo in Part 3 (Double-blind Withdrawal)
Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events Affected / at Risk (%) # Events
Total   16/243 (6.58%)      34/245 (13.88%)      5/242 (2.07%)      95/704 (13.49%)      6/310 (1.94%)      4/303 (1.32%)    
General disorders             
Oedema peripheral  1  16/243 (6.58%)  16 34/245 (13.88%)  34 5/242 (2.07%)  5 95/704 (13.49%)  102 6/310 (1.94%)  7 4/303 (1.32%)  4
1
Term from vocabulary, MedDRA (24.1)
Indicates events were collected by systematic assessment
[Not Specified]
Certain Agreements
Principal Investigators are NOT employed by the organization sponsoring the study.
There IS an agreement between Principal Investigators and the Sponsor (or its agents) that restricts the PI's rights to discuss or publish trial results after the trial is completed.
Any study-related publication written independently by investigators must be submitted to the sponsor for review at least 30 days prior to submission for publication or presentation at a congress. Upon review, the sponsor may provide comments, and may also request alterations and/or deletions for the sole purpose of protecting its confidential information and/or patent rights. Neither the institution nor the investigator should permit publication during such a review period.
Results Point of Contact
Layout table for Results Point of Contact information
Name/Title: Clinical Trial Disclosure Desk
Organization: Idorsia Pharmaceuticals Ltd
Phone: +41 58844 1977
EMail: idorsiaclinicaltrials@idorsia.com
Publications of Results:
Danaietash P, Verweij P, Wang JG, Dresser G, Kantola I, Lawrence MK, Narkiewicz K, Schlaich M, Bellet M; PRECISION investigators. Identifying and treating resistant hypertension in PRECISION: A randomized long-term clinical trial with aprocitentan. J Clin Hypertens (Greenwich). 2022 Jul;24(7):804-813. doi: 10.1111/jch.14517. Epub 2022 Jun 9.
Other Publications:
Daskalopoulou SS, Khan NA, Quinn RR, Ruzicka M, McKay DW, Hackam DG, Rabkin SW, Rabi DM, Gilbert RE, Padwal RS, Dawes M, Touyz RM, Campbell TS, Cloutier L, Grover S, Honos G, Herman RJ, Schiffrin EL, Bolli P, Wilson T, Feldman RD, Lindsay MP, Hemmelgarn BR, Hill MD, Gelfer M, Burns KD, Vallee M, Prasad GV, Lebel M, McLean D, Arnold JM, Moe GW, Howlett JG, Boulanger JM, Larochelle P, Leiter LA, Jones C, Ogilvie RI, Woo V, Kaczorowski J, Trudeau L, Bacon SL, Petrella RJ, Milot A, Stone JA, Drouin D, Lamarre-Cliche M, Godwin M, Tremblay G, Hamet P, Fodor G, Carruthers SG, Pylypchuk G, Burgess E, Lewanczuk R, Dresser GK, Penner B, Hegele RA, McFarlane PA, Sharma M, Campbell NR, Reid D, Poirier L, Tobe SW; Canadian Hypertension Education Program. The 2012 Canadian hypertension education program recommendations for the management of hypertension: blood pressure measurement, diagnosis, assessment of risk, and therapy. Can J Cardiol. 2012 May;28(3):270-87. doi: 10.1016/j.cjca.2012.02.018.
Publications automatically indexed to this study by ClinicalTrials.gov Identifier (NCT Number):
Layout table for additonal information
Responsible Party: Idorsia Pharmaceuticals Ltd.
ClinicalTrials.gov Identifier: NCT03541174    
Other Study ID Numbers: ID-080A301
2017-004393-33 ( EudraCT Number )
First Submitted: May 17, 2018
First Posted: May 30, 2018
Results First Submitted: November 8, 2022
Results First Posted: March 21, 2023
Last Update Posted: March 21, 2023