Pulmonary Arterial Hypertension
Conditions
Brief summary
The objective of this clinical trial is to compare the efficacy and safety of an initial triple oral treatment regimen (macitentan, tadalafil, selexipag) versus an initial dual oral treatment regimen (macitentan, tadalafil, placebo) in newly diagnosed, treatment-naïve patients with pulmonary arterial hypertension.
Interventions
DRUGMacitentan
Used open-label in both arms, 10 mg tablet, 1 tablet u.i.d.
DRUGTadalafil
Used open-label in both arms, 20 mg tablet, 1-2 tablets u.i.d.
DRUGSelexipag
Used double-blind in the triple oral treatment arm, 200 microgram tablet, 1-8 tablets b.i.d.
Sponsors
Actelion
Study design
Allocation
RANDOMIZED
Intervention model
PARALLEL
Primary purpose
TREATMENT
Masking
QUADRUPLE (Subject, Caregiver, Investigator, Outcomes Assessor)
Eligibility
Sex/Gender
ALL
Age
18 Years to 75 Years
Healthy volunteers
No
Inclusion criteria
1. Signed informed consent prior to any study-mandated procedure. 2. Male or female ≥ 18 and ≤ 75 years of age at screening. 3. Initial PAH diagnosis \< 6 months prior to enrollment. 4. RHC performed between Day -28 and Day 1, meeting all the following criteria: * Mean pulmonary artery pressure (mPAP) ≥ 25 mmHg. * Pulmonary artery wedge pressure or left ventricular end-diastolic pressure ≤ 15 mmHg. * PVR ≥ 480 dyn•sec/cm5 (≥ 6 Wood Units). * Negative vasoreactivity test mandatory in idiopathic, heritable, and drug/toxin induced PAH (at this or a previous RHC). 5. Symptomatic PAH belonging to one of the following subgroups: * Idiopathic. * Heritable. * Drug or toxin induced. * Associated with one of the following: connective tissue disease; HIV infection; congenital heart disease. 6. 6-minute walk distance (6MWD) ≥ 50 m at screening. 7. Women of childbearing potential must not be pregnant, must perform regular pregnancy tests, and use reliable contraception.
Exclusion criteria
1. Any PAH-specific drug therapy at any time. 2. Cardio pulmonary rehabilitation program based on exercise (planned, or started ≤ 12 weeks prior to Day 1). 3. Body mass index (BMI) \> 40 kg/m2 at screening. 4. Presence of three or more of the following risk factors for heart failure with preserved ejection fraction at screening: * BMI \> 30 kg/m2. * Diabetes mellitus of any type. * Essential hypertension. * Coronary artery disease, i.e., any of the following: * History of stable angina or * More than 50% stenosis in a coronary artery (by coronary angiography) or * History of myocardial infarction or * History of or planned coronary artery bypass grafting and/or coronary artery stenting. 5. Acute myocardial infarction ≤ 12 weeks prior to screening. 6. Stroke ≤ 12 weeks prior to screening. 7. Known permanent atrial fibrillation. 8. SBP \< 90 mmHg at screening or Day 1. 9. Ongoing or planned treatment with organic nitrates and/or doxazosin. 10. Presence of one or more of the following signs of relevant lung disease at any time up to screening: * Diffusing capacity of the lung for carbon monoxide (DLCO) \< 40% of predicted (eligible only if no or mild interstitial lung disease on computed tomography). * Forced vital capacity (FVC) \< 60% of predicted. * Forced expiratory volume in one second (FEV1) \< 60% of predicted. 11. Known or suspected pulmonary veno-occlusive disease (PVOD). 12. Documented severe hepatic impairment (with or without cirrhosis) according to National Cancer Institute organ dysfunction working group criteria, defined as total bilirubin \> 3 × upper limit of the normal range (ULN) accompanied by aspartate aminotransferase (AST) \> ULN (assessed by central laboratory at screening); and/or Child-Pugh Class C. 13. Serum AST and/or alanine aminotransferase (ALT) \> 3 × ULN (assessed by central laboratory at screening). 14. Severe renal impairment (estimated creatinine clearance ≤ 30 mL/min/1.73 m2) assessed by central laboratory at screening. 15. Ongoing or planned dialysis. 16. Hemoglobin \< 100 g/L assessed by central laboratory at screening. 17. Known or suspected uncontrolled thyroid disease (hypo- or hyperthyroidism). 18. Loss of vision in one or both eyes because of non-arteritic ischemic optic neuropathy (NAION). 19. Treatment with strong inducers of cytochrome P450 3A4 (CYP3A4; e.g., carbamazepine, rifampin, rifampicin, rifabutin, rifapentin, phenobarbital, phenytoin, and St. John's wort) ≤ 28 days prior to Day 1. 20. Treatment with strong inhibitors of CYP3A4 (e.g., ketoconazole, itraconazole, voriconazole, clarithromycin, telithromycin, nefazodone, ritonavir, and saquinavir) and/or strong inhibitors of CYP2C8 (e.g., gemfibrozil) ≤ 28 days prior to Day 1. 21. Treatment with another investigational drug (planned, or taken ≤ 12 weeks prior to Day 1). 22. Hypersensitivity to any of the 3 study treatments or any excipient of their formulations. 23. Pregnancy, breastfeeding, or intention to become pregnant during the study. 24. Concomitant life-threatening disease with a life expectancy \< 12 months. 25. Alcohol abuse. 26. Any factor or condition likely to affect protocol compliance of the subject, as judged by the investigator.
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Change From Baseline to Week 26 in Pulmonary Vascular Resistance (PVR) | Baseline, Week 26 | Change from baseline to Week 26 in PVR was expressed as the ratio of Week 26 to baseline PVR value (Week 26 divided by baseline) using re-calculated PVR. PVR was determined by right heart catheterization (RHC). A geometric least square mean ratio of Week 26 to baseline PVR less than (\<) 1 corresponds to a reduction in PVR from baseline. Missing values were imputed using a last observation carried forward (LOCF) approach. |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| Change From Baseline to Week 26 in 6-minute Walk Distance (6MWD) | Baseline, Week 26 | The change from baseline to Week 26 in 6MWD was calculated as Week 26 minus baseline. The test measures the distance an individual is able to walk over a total of six minutes on a hard, flat surface. The goal is for the individual to walk as far as possible in six minutes. Missing values were imputed using a LOCF approach. |
| Change From Baseline to Week 26 in N-terminal Pro B-type Natriuretic Peptide (NT-proBNP) Levels | Baseline, Week 26 | The change from baseline to Week 26 in NT-proBNP was expressed as the ratio of Week 26 to baseline NT-proBNP (Week 26 divided by baseline). A geometric least square mean ratio of Week 26 to baseline NT-proBNP \<1 corresponds to a reduction in NT-proBNP from baseline. Missing values were imputed using a LOCF approach. |
| Percentage of Participants With Absence of Worsening From Baseline to Week 26 in World Health Organization (WHO) Functional Class (FC) | Week 26 | WHO FC is a classification graded from Class I to IV which reflects disease severity based on symptoms. Worsening was defined as death or hospitalization due to PAH. Class I: No limitation of activity; Class II: slight limitation with ordinary activities; Class III: may not have symptoms at rest but greatly limited activities; Class IV: symptoms at rest and inability to carry out any physical activity without symptoms. Missing values were imputed using a LOCF approach. |
| Change From Baseline to Week 26 in Mean Pulmonary Arterial Pressure (mPAP) | Baseline, Week 26 | Change from baseline to Week 26 in mean Pulmonary Arterial Pressure (mPAP) was measured. The pulmonary artery pressure is a measure of the blood pressure found in the main pulmonary artery. Missing values were imputed using a LOCF approach. |
| Change From Baseline to Week 26 in Mean Right Atrial Pressure (mRAP) | Baseline, Week 26 | Change from baseline to Week 26 in mean Right Atrial Pressure (mRAP) was measured. Missing values were imputed using a LOCF approach. |
| Change From Baseline to Week 26 in Total Pulmonary Resistance | Baseline, Week 26 | Change from baseline to Week 26 in total pulmonary resistance was measured. Total pulmonary resistance was calculated as mPAP/CO\*80, where CO is cardiac output. Re-calculated values were used for analysis and missing values were imputed using a LOCF approach. |
| Change From Baseline to Week 26 in Cardiac Index | Baseline, Week 26 | Change from baseline to Week 26 in cardiac index was measured. Cardiac index is the amount of blood pumped by the heart, per minute, per meter square of body surface area. Re-calculated values were used for analysis and missing values were imputed using a LOCF approach. |
| Change From Baseline to Week 26 in Venous Oxygen Saturation (%) | Baseline, Week 26 | Change from baseline to Week 26 in venous oxygen saturation was measured. Missing values were imputed using a LOCF approach. |
| Number of Participants With Disease Progression Event | Week 26, Month 12, Month 18, Month 24, Month 30, and End of Analysis Period (up to 40 months) | Number of participants with disease progression event were reported. Disease progression event as adjudicated by the CEC, defined as any of the following: a. Death (all causes; adjudicated for PAH relationship); b. Hospitalization for worsening PAH; c. Initiation of prostacyclin, a prostacyclin analog, or a prostacyclin receptor agonist for worsening PAH; d. Clinical worsening defined as a post-baseline decrease in 6MWD by more than (\>) 15 percent (%) from the highest 6MWD obtained at or after baseline, accompanied by WHO FC III or IV (both conditions confirmed at two consecutive post-baseline visits separated by 1-21 days). |
Countries
Australia, Austria, Belgium, Canada, Denmark, France, Germany, Ireland, Italy, Netherlands, Spain, Sweden, Switzerland, United Kingdom, United States
Participant flow
Participants by arm
| Arm | Count |
|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) Participants received macitentan oral tablet, 10 milligrams (mg) once daily and tadalafil oral tablet, 20 mg, once daily from Day 1 up to End of treatment (10 months after last participant was enrolled). Tadalafil was up-titrated from 20 mg to 40 mg on Day 8. In addition, participants received selexipag oral tablet at a starting dose of 200 micrograms (mcg), twice daily from Day 15 up-titrated to a maximum of 1600 mcg, up to End of treatment (10 months after last participant was enrolled). | 123 |
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) Participants received macitentan oral tablet, 10 milligrams (mg) once daily and tadalafil oral tablet, 20 mg, once daily from Day 1 up to End of treatment (10 months after last participant was enrolled). Tadalafil was up-titrated from 20 mg to 40 mg on Day 8. In addition, participants received selexipag oral tablet at a starting dose of 200 micrograms (mcg), twice daily from Day 15 up-titrated to a maximum of 1600 mcg, up to End of treatment (10 months after last participant was enrolled). | 123 |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) Participants received macitentan oral tablet, 10 mg once daily and tadalafil oral tablet, 20 once daily from Day 1 up to End of treatment (10 months after last participant was enrolled). Tadalafil was up-titrated from 20 mg to 40 mg on Day 8. In addition, participants received placebo matching to selexipag oral tablet, at a starting dose of 200 micrograms (mcg), twice daily from Day 15 and dose up-titrated to a maximum of 1600 mcg, up to End of treatment (10 months after last participant was enrolled). | 124 |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) Participants received macitentan oral tablet, 10 mg once daily and tadalafil oral tablet, 20 once daily from Day 1 up to End of treatment (10 months after last participant was enrolled). Tadalafil was up-titrated from 20 mg to 40 mg on Day 8. In addition, participants received placebo matching to selexipag oral tablet, at a starting dose of 200 micrograms (mcg), twice daily from Day 15 and dose up-titrated to a maximum of 1600 mcg, up to End of treatment (10 months after last participant was enrolled). | 124 |
| Total | 494 |
Withdrawals & dropouts
| Period | Reason | FG000 | FG001 |
|---|---|---|---|
| Overall Study | Death | 4 | 12 |
| Overall Study | Lost to Follow-up | 7 | 4 |
| Overall Study | Physician Decision | 7 | 5 |
| Overall Study | Sponsor Decision | 0 | 1 |
| Overall Study | Withdrawal by Subject | 7 | 4 |
Baseline characteristics
| Characteristic | Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Total | Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) |
|---|---|---|---|
| Age, Continuous | 51.6 years STANDARD_DEVIATION 13.92 | 51.9 years STANDARD_DEVIATION 13.67 | 52.2 years STANDARD_DEVIATION 13.48 |
| Ethnicity (NIH/OMB) Hispanic or Latino | 10 Participants | 20 Participants | 10 Participants |
| Ethnicity (NIH/OMB) Not Hispanic or Latino | 108 Participants | 214 Participants | 106 Participants |
| Ethnicity (NIH/OMB) Unknown or Not Reported | 6 Participants | 13 Participants | 7 Participants |
| Race/Ethnicity, Customized American Indian or Alaska Native | 0 participants | 1 participants | 1 participants |
| Race/Ethnicity, Customized Asian | 3 participants | 10 participants | 7 participants |
| Race/Ethnicity, Customized Black or African American | 5 participants | 10 participants | 5 participants |
| Race/Ethnicity, Customized Native Hawaiian or Other Pacific Islander | 0 participants | 0 participants | 0 participants |
| Race/Ethnicity, Customized Other | 3 participants | 6 participants | 3 participants |
| Race/Ethnicity, Customized Unknown or Not Reported | 5 participants | 10 participants | 5 participants |
| Race/Ethnicity, Customized White | 108 participants | 210 participants | 102 participants |
| Region of Enrollment AUSTRALIA | 2 participants | 4 participants | 2 participants |
| Region of Enrollment AUSTRIA | 5 participants | 14 participants | 9 participants |
| Region of Enrollment BELGIUM | 5 participants | 7 participants | 2 participants |
| Region of Enrollment CANADA | 14 participants | 25 participants | 11 participants |
| Region of Enrollment DENMARK | 2 participants | 5 participants | 3 participants |
| Region of Enrollment FRANCE | 5 participants | 9 participants | 4 participants |
| Region of Enrollment GERMANY | 23 participants | 36 participants | 13 participants |
| Region of Enrollment IRELAND | 0 participants | 1 participants | 1 participants |
| Region of Enrollment ITALY | 6 participants | 11 participants | 5 participants |
| Region of Enrollment NETHERLANDS | 2 participants | 4 participants | 2 participants |
| Region of Enrollment SPAIN | 1 participants | 3 participants | 2 participants |
| Region of Enrollment SWEDEN | 0 participants | 7 participants | 7 participants |
| Region of Enrollment SWITZERLAND | 1 participants | 2 participants | 1 participants |
| Region of Enrollment UNITED KINGDOM | 2 participants | 5 participants | 3 participants |
| Region of Enrollment UNITED STATES | 56 participants | 114 participants | 58 participants |
| Sex: Female, Male Female | 94 Participants | 187 Participants | 93 Participants |
| Sex: Female, Male Male | 30 Participants | 60 Participants | 30 Participants |
Adverse events
| Event type | EG000 affected / at risk | EG001 affected / at risk |
|---|---|---|
| deaths Total, all-cause mortality | 4 / 119 | 12 / 127 |
| other Total, other adverse events | 118 / 119 | 119 / 127 |
| serious Total, serious adverse events | 58 / 119 | 48 / 127 |
Outcome results
Primary
Change From Baseline to Week 26 in Pulmonary Vascular Resistance (PVR)
Change from baseline to Week 26 in PVR was expressed as the ratio of Week 26 to baseline PVR value (Week 26 divided by baseline) using re-calculated PVR. PVR was determined by right heart catheterization (RHC). A geometric least square mean ratio of Week 26 to baseline PVR less than (\<) 1 corresponds to a reduction in PVR from baseline. Missing values were imputed using a last observation carried forward (LOCF) approach.
Time frame: Baseline, Week 26
Population: Full analysis set (FAS) included all randomized participants.
| Arm | Measure | Value (GEOMETRIC_LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in Pulmonary Vascular Resistance (PVR) | 0.46 ratio |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in Pulmonary Vascular Resistance (PVR) | 0.48 ratio |
p-value: 0.423995% CI: [0.86, 1.07]ANCOVA
Secondary
Change From Baseline to Week 26 in 6-minute Walk Distance (6MWD)
The change from baseline to Week 26 in 6MWD was calculated as Week 26 minus baseline. The test measures the distance an individual is able to walk over a total of six minutes on a hard, flat surface. The goal is for the individual to walk as far as possible in six minutes. Missing values were imputed using a LOCF approach.
Time frame: Baseline, Week 26
Population: Full analysis set included all randomized participants. Here, N (number of participants analyzed) signifies the number of participants analyzed for this outcome measure.
| Arm | Measure | Value (LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in 6-minute Walk Distance (6MWD) | 54.96 meter |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in 6-minute Walk Distance (6MWD) | 56.39 meter |
p-value: 0.875895% CI: [-19.393, 16.538]ANCOVA
Secondary
Change From Baseline to Week 26 in Cardiac Index
Change from baseline to Week 26 in cardiac index was measured. Cardiac index is the amount of blood pumped by the heart, per minute, per meter square of body surface area. Re-calculated values were used for analysis and missing values were imputed using a LOCF approach.
Time frame: Baseline, Week 26
Population: Full analysis set included all randomized participants.
| Arm | Measure | Value (LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in Cardiac Index | 0.97 liters per minute per meter square |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in Cardiac Index | 0.84 liters per minute per meter square |
p-value: 0.190295% CI: [-0.066, 0.328]ANCOVA
Secondary
Change From Baseline to Week 26 in Mean Pulmonary Arterial Pressure (mPAP)
Change from baseline to Week 26 in mean Pulmonary Arterial Pressure (mPAP) was measured. The pulmonary artery pressure is a measure of the blood pressure found in the main pulmonary artery. Missing values were imputed using a LOCF approach.
Time frame: Baseline, Week 26
Population: Full analysis set included all randomized participants.
| Arm | Measure | Value (LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in Mean Pulmonary Arterial Pressure (mPAP) | -12.92 millimeters of mercury (mmHg) |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in Mean Pulmonary Arterial Pressure (mPAP) | -12.20 millimeters of mercury (mmHg) |
p-value: 0.499895% CI: [-2.834, 1.386]ANCOVA
Secondary
Change From Baseline to Week 26 in Mean Right Atrial Pressure (mRAP)
Change from baseline to Week 26 in mean Right Atrial Pressure (mRAP) was measured. Missing values were imputed using a LOCF approach.
Time frame: Baseline, Week 26
Population: Full analysis set included all randomized participants. Here, N (number of participants analyzed) signifies the number of participants analyzed for this outcome measure.
| Arm | Measure | Value (LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in Mean Right Atrial Pressure (mRAP) | -1.78 mmHg |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in Mean Right Atrial Pressure (mRAP) | -1.69 mmHg |
p-value: 0.852895% CI: [-1.003, 0.83]ANCOVA
Secondary
Change From Baseline to Week 26 in N-terminal Pro B-type Natriuretic Peptide (NT-proBNP) Levels
The change from baseline to Week 26 in NT-proBNP was expressed as the ratio of Week 26 to baseline NT-proBNP (Week 26 divided by baseline). A geometric least square mean ratio of Week 26 to baseline NT-proBNP \<1 corresponds to a reduction in NT-proBNP from baseline. Missing values were imputed using a LOCF approach.
Time frame: Baseline, Week 26
Population: Full analysis set included all randomized participants. Here, N (number of participants analyzed) signifies the number of participants analyzed for this outcome measure.
| Arm | Measure | Value (GEOMETRIC_LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in N-terminal Pro B-type Natriuretic Peptide (NT-proBNP) Levels | 0.26 ratio |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in N-terminal Pro B-type Natriuretic Peptide (NT-proBNP) Levels | 0.25 ratio |
p-value: 0.852995% CI: [0.77, 1.371]ANCOVA
Secondary
Change From Baseline to Week 26 in Total Pulmonary Resistance
Change from baseline to Week 26 in total pulmonary resistance was measured. Total pulmonary resistance was calculated as mPAP/CO\*80, where CO is cardiac output. Re-calculated values were used for analysis and missing values were imputed using a LOCF approach.
Time frame: Baseline, Week 26
Population: Full analysis set included all randomized participants.
| Arm | Measure | Value (LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in Total Pulmonary Resistance | -511.88 dynes*second per centimeter^5 |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in Total Pulmonary Resistance | -514.28 dynes*second per centimeter^5 |
p-value: 0.947495% CI: [-69.368, 74.178]ANCOVA
Secondary
Change From Baseline to Week 26 in Venous Oxygen Saturation (%)
Change from baseline to Week 26 in venous oxygen saturation was measured. Missing values were imputed using a LOCF approach.
Time frame: Baseline, Week 26
Population: Full analysis set included all randomized participants. Here, N (number of participants analyzed) signifies the number of participants analyzed for this outcome measure.
| Arm | Measure | Value (LEAST_SQUARES_MEAN) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Change From Baseline to Week 26 in Venous Oxygen Saturation (%) | 5.59 percentage of oxygen saturation |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Change From Baseline to Week 26 in Venous Oxygen Saturation (%) | 6.79 percentage of oxygen saturation |
p-value: 0.122795% CI: [-2.737, 0.327]ANCOVA
Secondary
Number of Participants With Disease Progression Event
Number of participants with disease progression event were reported. Disease progression event as adjudicated by the CEC, defined as any of the following: a. Death (all causes; adjudicated for PAH relationship); b. Hospitalization for worsening PAH; c. Initiation of prostacyclin, a prostacyclin analog, or a prostacyclin receptor agonist for worsening PAH; d. Clinical worsening defined as a post-baseline decrease in 6MWD by more than (\>) 15 percent (%) from the highest 6MWD obtained at or after baseline, accompanied by WHO FC III or IV (both conditions confirmed at two consecutive post-baseline visits separated by 1-21 days).
Time frame: Week 26, Month 12, Month 18, Month 24, Month 30, and End of Analysis Period (up to 40 months)
Population: Full analysis set included all randomized participants.
| Arm | Measure | Group | Value (COUNT_OF_PARTICIPANTS) |
|---|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Number of Participants With Disease Progression Event | Month 12 | 13 Participants |
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Number of Participants With Disease Progression Event | Month 18 | 15 Participants |
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Number of Participants With Disease Progression Event | Month 24 | 15 Participants |
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Number of Participants With Disease Progression Event | Month 30 | 16 Participants |
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Number of Participants With Disease Progression Event | End of Analysis Period (up to 40 months) | 16 Participants |
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Number of Participants With Disease Progression Event | Week 26 | 8 Participants |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Number of Participants With Disease Progression Event | End of Analysis Period (up to 40 months) | 27 Participants |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Number of Participants With Disease Progression Event | Month 12 | 20 Participants |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Number of Participants With Disease Progression Event | Month 30 | 27 Participants |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Number of Participants With Disease Progression Event | Month 18 | 23 Participants |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Number of Participants With Disease Progression Event | Week 26 | 13 Participants |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Number of Participants With Disease Progression Event | Month 24 | 25 Participants |
p-value: 0.086795% CI: [0.32, 1.09]Log Rank
Secondary
Percentage of Participants With Absence of Worsening From Baseline to Week 26 in World Health Organization (WHO) Functional Class (FC)
WHO FC is a classification graded from Class I to IV which reflects disease severity based on symptoms. Worsening was defined as death or hospitalization due to PAH. Class I: No limitation of activity; Class II: slight limitation with ordinary activities; Class III: may not have symptoms at rest but greatly limited activities; Class IV: symptoms at rest and inability to carry out any physical activity without symptoms. Missing values were imputed using a LOCF approach.
Time frame: Week 26
Population: FAS included all randomized participants. Here, N (number of participants analyzed) signifies number of participants analyzed for this outcome measure. Participants with WHO FC IV at baseline were excluded from this analysis as they could not shift to a worse category.
| Arm | Measure | Value (NUMBER) |
|---|---|---|
| Triple Oral Therapy (Macitentan, Tadalafil, and Selexipag) | Percentage of Participants With Absence of Worsening From Baseline to Week 26 in World Health Organization (WHO) Functional Class (FC) | 99.2 percentage of participants |
| Double Oral Therapy (Macitentan, Tadalafil, and Placebo) | Percentage of Participants With Absence of Worsening From Baseline to Week 26 in World Health Organization (WHO) Functional Class (FC) | 97.5 percentage of participants |