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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02038036
Other study ID # CINC424B2401
Secondary ID
Status Completed
Phase Phase 3
First received
Last updated
Start date March 25, 2014
Est. completion date April 7, 2020

Study information

Verified date June 2021
Source Novartis
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study compared the efficacy and safety of ruxolitinib to Best Available Therapy (BAT) in patients with polycythemia vera (PV) who were hydroxyurea (HU) resistant or intolerant and did not have a palpable spleen.


Description:

This was a prospective, multi-center, open-label, randomized, Phase IIIb study evaluating efficacy and safety of ruxolitinib versus BAT as selected by the Investigator in patients with PV who are resistant to, or intolerant of HU. The study comprised of the following periods: Screening Period (up to 5 weeks: Day -35 to Day -1): Screening evaluations were performed at one or more clinic visits, and reviewed to determine eligibility before the patient was randomized in the study. Core Treatment Period (Day 1 to Week 80): Patients were randomized in 1:1 ratio to either treatment group (ruxolitinib or BAT) and were to be treated with their randomized treatment. Crossover Treatment Period (Week 28 or after) for BAT patients only: Patients randomized to BAT who did not respond by Week 28 were eligible to crossover and start treatment with ruxolitinib. Patients crossing over on or after Week 28 had to complete all assessments for the End of Treatment (EoT) visit of the Core Treatment Period followed by the assessments in Cross-over visit evaluation schedule. Extended Treatment Period (Week 80 to Week 260): Patients receiving ruxolitinib at Week 80 (including patients who have crossed over from BAT) were eligible to continue up to Week 260 in the Extended Treatment Period. Patients continued the ruxolitinib dose that they received at Week 80. Patients who received BAT at Week 80 were not eligible to enter the Extended Treatment Period and had to have the EoT visit at Week 80 and an End of study (EoS) visit 30 days after the EoT visit. Follow-up Period: Patients were followed for safety during 30 days after the last dose of study drug and EoS visit assessments were performed post 30 days after the last dose of study drug. Patients who completed EoT (Week 80 for patients who received BAT, Week 260 for patients who received ruxolitinib or from the time of premature discontinuation) were to be followed-up for every 3 months for survival till the end of the study.


Recruitment information / eligibility

Status Completed
Enrollment 149
Est. completion date April 7, 2020
Est. primary completion date September 29, 2015
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: Confirmed diagnosis of PV according to the 2008 World Health Organization criteria, Non-palpable spleen, Phlebotomy dependent, Resistant to or intolerant of hydroxyurea, ECOG performance status of 0, 1 or 2. Exclusion Criteria: Inadequate liver or renal function, Significant bacterial, fungal, parasitic, or viral infection requiring treatment, Active malignancy within the past 5 years, excluding specific skin cancers, Previously received treatment with a JAK inhibitor, Being treated with any investigational agent, Women who are pregnant or nursing. Other inclusion/exclusion criteria apply.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Best Available Therapy
Best Available Therapy as selected by the investigator from: Hydroxyurea, Pegylated-Interferon (IFN/PEG-IFN), pipobroman, anagrelide, IMIDs, or observation. Participants randomized to BAT who did not respond by Week 28 were eligible to crossover and start treatment with ruxolitinib.
Ruxolitinib
Ruxolitinib was administered at a starting dose of 10 mg twice a day (bid). Dose was adjusted based on efficacy and safety parameters up to a maximum dose of 25 mg bid.

Locations

Country Name City State
Australia Novartis Investigative Site Herston Queensland
Belgium Novartis Investigative Site Antwerpen
Belgium Novartis Investigative Site Leuven
Canada Novartis Investigative Site Toronto Ontario
France Novartis Investigative Site Bayonne Bayonne Cedex
France Novartis Investigative Site Bordeaux
France Novartis Investigative Site Brest
France Novartis Investigative Site Lille cedex
France Novartis Investigative Site Nice Cedex
France Novartis Investigative Site Paris
France Novartis Investigative Site Toulouse
Germany Novartis Investigative Site Augsburg
Germany Novartis Investigative Site Dresden
Germany Novartis Investigative Site Jena
Germany Novartis Investigative Site Leipzig
Germany Novartis Investigative Site Magdeburg
Germany Novartis Investigative Site Mainz
Germany Novartis Investigative Site Mannheim Baden-Wuerttemberg
Germany Novartis Investigative Site Minden
Germany Novartis Investigative Site Ulm
Hungary Novartis Investigative Site Budapest
Hungary Novartis Investigative Site Debrecen
Hungary Novartis Investigative Site Kaposvar
India Novartis Investigative Site Mumbai Maharashtra
India Novartis Investigative Site Vellore Tamil Nadu
Israel Novartis Investigative Site Nahariya
Israel Novartis Investigative Site Netanya
Israel Novartis Investigative Site Tel Aviv
Italy Novartis Investigative Site Bologna BO
Italy Novartis Investigative Site Firenze FI
Italy Novartis Investigative Site Milano MI
Italy Novartis Investigative Site Pavia PV
Italy Novartis Investigative Site Roma Lazio
Italy Novartis Investigative Site Torino TO
Italy Novartis Investigative Site Varese VA
Korea, Republic of Novartis Investigative Site Seoul
Korea, Republic of Novartis Investigative Site Seoul
Spain Novartis Investigative Site Alicante Comunidad Valenciana
Spain Novartis Investigative Site Barcelona Catalunya
Spain Novartis Investigative Site La Coruna Galicia
Spain Novartis Investigative Site Las Palmas de Gran Canaria Las Palmas De G.C
Spain Novartis Investigative Site Madrid
Spain Novartis Investigative Site Madrid
Spain Novartis Investigative Site Malaga Andalucia
Spain Novartis Investigative Site Pamplona Navarra
Spain Novartis Investigative Site Salamanca Castilla Y Leon
Turkey Novartis Investigative Site Izmir
Turkey Novartis Investigative Site Talas / Kayseri

Sponsors (1)

Lead Sponsor Collaborator
Novartis Pharmaceuticals

Countries where clinical trial is conducted

Australia,  Belgium,  Canada,  France,  Germany,  Hungary,  India,  Israel,  Italy,  Korea, Republic of,  Spain,  Turkey, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of Participants Achieving Hematocrit (Hct) Control at Week 28 Proportion of patients achieving Hct control at Week 28 was defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 28, with no more than one phlebotomy eligibility occurring post randomization and prior to Week 8.
Phlebotomy eligibility was defined by:
Confirmed Hct > 45% that is at least 3 percentage points higher than the Hct obtained at Baseline Or
Confirmed Hct > 48% The confirmation occurred 2 to 14 days subsequent to the initial observation.
Week 28
Secondary Number of Participants Achieving a Complete Hematological Remission at Week 28 Proportion of patients achieving a complete hematological remission at Week 28 was defined by:
Hct control at Week 28 defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 28, with no more than one phlebotomy eligibility occurring post randomization and prior to Week 8, and
WBC < 10 x109/L at Week 28, and
Platelets = 400 x 109/L at Week 28
Week 28
Secondary Number of Participants Achieving a Hematocrit (Hct) Control at Week 52 and Week 80 Proportion of patients achieving a Hct control at Week 52 was defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 52, and no more than one phlebotomy eligibility occurring post randomization and prior to Week 8
- Endpoint for Week 80 was defined, similarly.
Week 52 and 80
Secondary Number of Participants Achieving a Complete Hematological Remission at Week 52 and Week 80 Proportion of patients achieving a complete hematological remission at Week 52, was defined by:
Hct control at Week 52, as defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 52 with no more than one phlebotomy eligibility occurring post randomization and prior to Week 8, and
White Blood Count (WBC) < 10 x10^9/L at Week 52, and
Platelets = 400 x 10^9/L at Week 52
Endpoint for Week 80 was defined, similarly.
Week 52 and 80
Secondary Number of Participants With Phlebotomies Over Time Phlebotomy eligibility was defined by Confirmed Hct > 45% that is at least 3 percentage points higher than the Hct obtained at Baseline Or Confirmed Hct > 48%. The confirmation occurred 2 to 14 days subsequent to the initial observation. Baseline to Week 260
Secondary Change From Baseline in Hematocrit (Hct) at Each Visit Hematocrit is the volume percentage of red blood cells (RBC) in the blood. Baseline, Week 4, 8, 12, 16, 20, 24, 28, 40, 52, 66, 80, 92, 104, 117, 130, 143, 156, 169, 182, 195, 208, 221, 234, 247 and 260
Secondary Change From Baseline in Hematocrit (Hct) at Each Scheduled Visit After Crossover in Participants Randomized to BAT Who Cross Over to Ruxolitinib Hematocrit is the percentage of red blood cells (RBC) in the blood. Baseline (last assessment before cross over), Week 4, 8, 12, 16, 20, 24, 28, 40, 52, 64, 76, 89, 102, 115, 128, 141, 154, 167, 180, 193, 206, 219 and 232 after cross-over
Secondary Spleen Length by Visit Spleen length was assessed by manual palpation at every study visit. Week 4, 8, 12, 16, 20, 24, 28, 40, 52, 66, 80, 92, 104, 117, 130, 143, 156, 169, 182, 195, 208, 221, 234, 247 and 260
Secondary Change From Baseline in Eastern Cooperative Oncology Group (ECOG) Performance Status to Week 28 The ECOG scale of performance status described the level of functioning of participants in terms of their ability to care for themselves, daily activity, and physical ability. The ECOG performance was recorded as per ECOG performance status grades ranging from 0 (fully active, able to carry on all pre-disease performance without restriction) to 5 (dead). Baseline and Week 28
Secondary Number of Participants Achieving a Partial Remission Based on the European Leukemia Net (ELN) and International Working Group for Myelofibrosis Research and Treatment (IWG-MRT) Criteria at Week 28 Proportion of patients achieving a partial remission at Week 28, based on the ELN and IWG-MRT criteria, as defined by:
Myeloproliferative Neoplasm Symptom Assessment Form Total Symptom Score (MPN-SAF TSS) score reduction of greater than or equal to 10 points from baseline to Week 28, and
Hct control defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 28, with no more than one phlebotomy eligibility occurring post randomization and prior to Week 8, and
WBC < 10 x10^9/L at Week 28, and
Platelets = 400 x 10^9/L at Week 28, and
No palpable spleen at Week 28, and
No hemorrhagic or thrombotic events, and
No transformation into post-PV myelofibrosis, myelodysplastic syndrome (IWG-MRT criteria) or acute leukemia (WHO criteria).
Week 28
Secondary Number of Participants Who Achieved Partial Remission Based on the European Leukemia Net (ELN) and International Working Group for Myelofibrosis Research and Treatment (IWG-MRT) Criteria at Week 52 and Week 80 Proportion of patients who achieved partial remission at Week 52 based on the ELN and IWG-MRT criteria, as defined by:
MPN-SAF TSS score reduction of greater than or equal to 10 points from baseline to Week 52 and
Hct control defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 52 with no more than one phlebotomy eligibility occurring post randomization and prior to Week 8, and
WBC < 10 x109/L at Week 52 and
Platelets = 400 x 109/L at Week 52 and
No palpable spleen at Week 52 and
No hemorrhagic or thrombotic events, and
No transformation into post-PV myelofibrosis, myelodysplastic syndrome (IWG-MRT criteria) or acute leukemia (WHO criteria).
Endpoint for Week 80 was defined, similarly.
Week 52 and 80
Secondary Number of Participants Achieving a Hematocrit (Hct) Control at Week 104, Week 156, Week 208 and Week 260. Proportion of patients achieving a Hct control at Week 104 as defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 104 and with no more than one phlebotomy eligibility occurring post randomization and prior to Week 8 Endpoint for Week 156, Week 208 and Week 260 were defined, similarly. From Week 8 to Week 104, 156, 208 and 260
Secondary Number of Participants Achieving a Complete Hematological Remission at Week 104, Week 156, Week 208 and Week 260 Proportion of patients achieving a complete hematological remission at Week 104 as defined by Hct control defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 104, with no more than one phlebotomy eligibility occurring post randomization and prior to Week 8, and
WBC < 10 x10^9/L at Week 104, and
Platelets = 400 x 10^9/L at Week 104 Endpoint for Week 156, Week 208 and Week 260 were defined, similarly.
From Week 8 to Week 104, 156, 208 and 260
Secondary Number of Participants Who Achieved Partial Remission Based on the European Leukemia Net (ELN) and International Working Group for Myelofibrosis Research and Treatment (IWG-MRT) Criteria at Week 104, Week 156, Week 208 and Week 260. Proportion of patients who achieved partial remission at Week 104, based on the ELN and IWG-MRT criteria, as defined by:
MPN-SAF TSS score reduction of greater than or equal to 10 points from baseline to Week 104, and
Hct control defined by the absence of phlebotomy eligibility starting at Week 8 and continuing through Week 104, with no more than one phlebotomy eligibility occurring post-randomization and prior to Week 8, and
WBC < 10 x10^9/L at Week 104, and
Platelets = 400 x 10^9/L at Week 104, and
No palpable spleen at Week 104, and
No hemorrhagic or thrombotic events, and
No transformation into post-PV myelofibrosis, myelodysplastic syndrome (IWG-MRT criteria) or acute leukemia (WHO criteria) Endpoint for Week 156, Week 208 and Week 260 are defined, similarly.
From Week 8 to Week 104, 156, 208 and 260
Secondary Number of Participants With Transformation Free Survival Events Transformation-free survival is defined as one of the following:
Myelofibrosis (MF) as evidenced by bone marrow biopsy, or
Acute leukemia as evidenced by bone marrow blast counts of at least 20%, or peripheral blast counts of at least 20% lasting at least 2 weeks.
Death due to any cause during treatment period
Week 260 (ruxolitinib arm) and Week 80 (BAT arm)
Secondary Number of Participants With Overall Survival (OS) Events Overall survival (OS) event is defined as death due to any cause. OS events were counted in the BAT arm, irrespective of whether participants crossed over to receive ruxolitinib when the event occurred. up to Week 260
Secondary Change From Baseline in Myeloproliferative Neoplasm Symptom Assessment Form Total Symptom Score (MPN-SAF TSS) The MPN-SAF TSS is a disease specific questionnaire comprised of 10 items that measures fatigue related to MPN disease and the severity of nine of the most prevalent associated symptoms. Each item is scored on a scale ranging from 0 (no fatigue/absent) to 10 (As bad as you can imagine/worst imaginable).The MPN-SAF TSS is computed as the average of the observed items multiplied by 10 to achieve a 0-to-100 scale. The MPN-SAF TSS thus has a possible score range of 0 to 100 where a decrease indicates improvement. Baseline, Week 4, 8, 16, 28, 40, 52, 80, 92, 104, 117, 130, 143, 156, 169, 182, 195, 208, 221, 234 and 247
Secondary Change From Baseline in Total Scores of MPN-SAF by Visit in Patients From BAT Group Who Cross Over to Ruxolitinib After Crossover The MPN-SAF TSS is a disease specific questionnaire comprised of 10 items that measures fatigue related to MPN disease and the severity of nine of the most prevalent associated symptoms. Each item is scored on a scale ranging from 0 (no fatigue/absent) to 10 (As bad as you can imagine/worst imaginable).The MPN-SAF TSS is computed as the average of the observed items multiplied by 10 to achieve a 0-to-100 scale. The MPN-SAF TSS thus has a possible score range of 0 to 100 where a decrease indicates improvement. Baseline (last assessment before cross over), Week 4, 8, 16, 24, 28, 40, 52, 92, 104, 117, 130, 143, 156, 169, 182, 195, 208, 221, 234 and 247 after cross-over
Secondary Change From Baseline in Score as Per European Quality of Life 5-Dimension 5-level (EQ-5D-5L) Questionnaire EQ-5D-5L is a standardized instrument for measuring health outcomes in a wide range of health conditions and treatments. It consists of visual analogue scale (EQ VAS) which records the respondent's self-rated health on a vertical, visual analogue scale where the endpoints are labeled 'Best imaginable health state' and 'worst imaginable health state'. The EQ VAS scores were anchored on 100 = the best health you can imagine and 0 = worst health you can imagine. Baseline, Week 4, 8, 16, 28, 52, 80, 92, 104, 117, 130, 143, 156, 169, 182, 195, 208, 221, 234 and 247
Secondary Change From Baseline in EQ-5D-5L VAS, by Visit in Patients From BAT Group Who Cross Over to Ruxolitinib After Crossover EQ-5D-5L is a standardized instrument for measuring health outcomes in a wide range of health conditions and treatments. It consists of visual analogue scale (EQ VAS) which records the respondent's self-rated health on a vertical, visual analogue scale where the endpoints are labeled 'Best imaginable health state' and 'worst imaginable health state'. The EQ VAS scores were anchored on 100 = the best health you can imagine and 0 = worst health you can imagine. Baseline (last assessment before cross over), Week 4, 8, 16, 24, 28, 52, 92, 104, 117, 130, 143, 156, 169, 182, 195, 208, 221, 234 and 247 after cross-over
Secondary Change From Baseline in Work Productivity and Activity Impairment (WPAI) Questionnaire The Work Productivity and Activity Impairment Questionnaire: Specific Health Problem (WPAI:SHP) is a six item questionnaire which intended to measure work and activity impairment associated with polycythemia vera. WPAI consisted of 6 questions (Q1=Employment status; Q2=Hours absent from work due to the polycythemia vera; Q3=Hours absent from work due to other reasons; Q4=Hours actually worked; Q5=Impact of the polycythemia vera on productivity while working; Q6=Impact of the polycythemia vera on productivity while doing regular daily activities other than work). Higher WPAI scores indicated greater activity impairment. Scores were multiplied by 100 to express in percentages.
Percent work time missed due to problem (past 7 days) =Q2/(Q2+Q4) Percent impairment while working due to problem (past 7 days): Q5/10 Percent overall work impairment due to problem (past 7 says): Q2/(Q2+Q4)+[(1 Q2/(Q2+Q4))x(Q5/10)] Percent activity impairment due to problem (past 7 says): Q6/10
Baseline, Week 4, 8, 16, 28, 52 and 80
Secondary Change From Baseline in Work Productivity and Activity Impairment Questionnaire (WPAI), by Visit in Patients From BAT Group Who Cross Over to Ruxolitinib After Crossover The Work Productivity and Activity Impairment Questionnaire: Specific Health Problem (WPAI:SHP) is a six item questionnaire which intended to measure work and activity impairment associated with polycythemia vera. WPAI consisted of 6 questions (Q1=Employment status; Q2=Hours absent from work due to the polycythemia vera; Q3=Hours absent from work due to other reasons; Q4=Hours actually worked; Q5=Impact of the polycythemia vera on productivity while working; Q6=Impact of the polycythemia vera on productivity while doing regular daily activities other than work). Higher WPAI scores indicated greater activity impairment. Scores were multiplied by 100 to express in percentages.
Percent work time missed due to problem (past 7 days) =Q2/(Q2+Q4) Percent impairment while working due to problem (past 7 days): Q5/10 Percent overall work impairment due to problem (past 7 says): Q2/(Q2+Q4)+[(1 Q2/(Q2+Q4))x(Q5/10)] Percent activity impairment due to problem (past 7 says): Q6/10
Baseline (last assessment before cross over), Week 4, 8, 16, 24, 28 and 52 after cross-over
Secondary Patient Global Impression of Change (PGIC) The Patient Global Impression of Change (PGIC) is comprised of a single question intended to measure a patient's perspective of improvement or deterioration over time relative to treatment. The PGIC uses a seven-point scale where one (1) equals very much improved and seven (7) equals very much worse. Week 4, 8, 16, 28, 40, 52 and 80
Secondary Summary of Patient Global Impression of Change (PGIC), by Visit in Patients From BAT Group Who Cross Over to Ruxolitinib After Crossover The Patient Global Impression of Change (PGIC) is comprised of a single question intended to measure a patient's perspective of improvement or deterioration over time relative to treatment. The PGIC uses a seven-point scale where one (1) equals very much improved and seven (7) equals very much worse. Baseline (last assessment before cross over), Week 4, 8, 16, 24, 28, 40, and 52 after cross-over
Secondary Number of Participants Developing Thrombosis Proportion of participants developing any arterial or venous thromboembolic event From randomization to Week 80 for BAT and Week 260 for Ruxolitinib
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