Pivotal Study (Pharmacokinetics, Efficacy, Safety) of BAX 326 (rFIX) in Hemophilia B Patients

April 30, 2021 updated by: Baxalta now part of Shire

Recombinant Factor IX (BAX 326): A Phase 1/3, Prospective, Controlled, Multicenter Study Evaluating Pharmacokinetics, Efficacy, Safety and Immunogenicity in Previously Treated Patients With Severe or Moderately Severe Hemophilia B

The purpose of this pivotal Phase 1/3 study is to determine the pharmacokinetic (PK) parameters, the hemostatic efficacy, and the safety of BAX 326, a recombinant factor IX, in previously treated patients (PTPs) with severe and moderately severe hemophilia B.

Study Overview

Status

Completed

Conditions

Intervention / Treatment

Study Type

Interventional

Enrollment (Actual)

86

Phase

  • Phase 3

Contacts and Locations

This section provides the contact details for those conducting the study, and information on where this study is being conducted.

Study Locations

  • Argentina
      • Rosario, Argentina
  • Brazil
      • Brasilia, Brazil
      • Sao Paulo, Brazil
  • Bulgaria
      • Sofia, Bulgaria
  • Chile
      • Santiago, Chile
  • Colombia
      • Bogotá, Colombia
      • Cali, Colombia
  • Czechia
      • Prague, Czechia
  • Japan
      • Hiroshima, Japan
      • Nara, Japan
      • Tochigi, Japan
      • Tokyo, Japan
  • Poland
      • Gdansk, Poland
      • Krakow, Poland
      • Lodz, Poland
      • Warsaw, Poland
  • Romania
      • Bucharest, Romania
      • Timisoara, Romania
  • Russian Federation
      • Kirov, Russian Federation
      • Moscow, Russian Federation
      • St. Petersburg, Russian Federation
  • Spain
      • Barcelona, Spain
  • Sweden
      • Malmö, Sweden
  • Ukraine
      • Lviv, Ukraine
  • United Kingdom
      • London, United Kingdom

Participation Criteria

Researchers look for people who fit a certain description, called eligibility criteria. Some examples of these criteria are a person's general health condition or prior treatments.

Eligibility Criteria

Ages Eligible for Study

12 years to 65 years (Child, Adult, Older Adult)

Accepts Healthy Volunteers

No

Genders Eligible for Study

All

Description

Main Inclusion Criteria:

  • Participant is 12 to 65 years old at the time of screening
  • Participant and/or legal representative has/have provided signed informed consent
  • Participant has severe (factor IX (FIX) level < 1%) or moderately severe (FIX level 1-2%) hemophilia B (based on the one stage activated partial thromboplastin time (aPTT) assay), as tested at screening at the central laboratory
  • Participant is previously treated with plasma-derived or recombinant FIX concentrate(s) for a minimum of 150 exposure days (EDs) (based on the participant's medical records); if a verifiable, documented history is unavailable, the participant can be enrolled if s/he has 100-150 EDs to any FIX product that are not fully documented and has participated in Study 050901 for at least 50 EDs to Immunine prior to enrollment (not valid for US and Japan).
  • Participant has no evidence of a history of FIX inhibitors
  • If the participant is to receive prophylactic treatment, the participant is willing to receive prophylactic treatment over a period of 6 months.
  • If the participant is to receive on-demand treatment, the participant has ≥12 documented bleeding episodes requiring treatment within 12 months prior to enrollment and is willing to receive on-demand treatment for the duration of this study.

Main Exclusion Criteria:

  • The participant has a history of FIX inhibitors with a titer ≥0.6 Bethesda Units (BU) (as determined by the Nijmegen modification of the Bethesda assay or the assay employed in the respective local laboratory) at any time prior to screening
  • The participant has a detectable FIX inhibitor at screening, with a titer ≥0.6 BU as determined by the Nijmegen modification of the Bethesda assay in the central laboratory
  • The participant's weight is < 35 kg or > 120 kg
  • The participant has a history of allergic reaction, eg, anaphylaxis, following exposure to FIX concentrate(s)
  • The participant has a known hypersensitivity to hamster proteins or recombinant furin (rFurin)
  • The participant has ongoing or recent evidence of a thrombotic disease, fibrinolysis or disseminated intravascular coagulation (DIC)

Study Plan

This section provides details of the study plan, including how the study is designed and what the study is measuring.

How is the study designed?

Design Details

  • Primary Purpose: Treatment
  • Allocation: Randomized
  • Interventional Model: Crossover Assignment
  • Masking: Double

Arms and Interventions

Participant Group / Arm
Intervention / Treatment
Experimental: BAX 326
Recombinant factor IX (rFIX)
Biological: BAX 326
  • Study Part 1: Pharmacokinetic (PK) Crossover with BAX326 and BeneFIX
  • Study Part 2: Open-label evaluation of prophylaxis and on-demand BAX326 only
  • Study Part 3: Open-label repeat of PK evaluation (repeat Study Part 1) with BAX326 only and same study participants as Study Part 1
Other Names:
  • RIXUBIS
  • Recombinant factor IX (rFIX)
Active Comparator: BeneFIX
Recombinant Factor IX (rFIX)
Biological: BeneFIX
  • Study Part 1: Pharmacokinetic (PK) Crossover with BAX326 and BeneFIX.
  • BeneFIX only used in Part 1 of this study.
  • Study Part 2 and 3 only utilized BAX326
Other Names:
  • Recombinant factor IX (rFIX)

What is the study measuring?

Primary Outcome Measures

Outcome Measure
Measure Description
Time Frame
Study Part 1- Area Under the Plasma Concentration Versus Time Curve From 0 to 72 Hours Per Dose
Time Frame: 72 hours
Computed using the linear trapezoidal method. The concentration at 72 hours was interpolated from the two nearest sampling time points or extrapolated using the last quantifiable concentration and the terminal rate constant λz. λz was estimated from the slope of natural log-linear fitting to latter quantifiable concentrations, with largest adjusted R^2.
72 hours

Secondary Outcome Measures

Outcome Measure
Measure Description
Time Frame
Study Parts 1 and 3: Area Under the Plasma Concentration/Time Curve From Time 0 to Infinity Per Dose (AUC0-∞/ Dose)
Time Frame: 0-30 minutes before infusion up to 72 hours post-infusion
Defined as (AUC0-t + Ct)/ λz/ dose, where t is the time of last quantifiable concentration, Ct is the last quantifiable concentration. λz will be estimated from the slope of natural log-linear fitting to latter quantifiable concentrations, with largest adjusted R^2. The objective of Study Part 3 was to re-evaluate the Pharmacokinetic (PK) parameters for BAX 326 after a period of 6 months of treatment, in participants who accumulated at least 30 EDs to BAX 326, and to compare them with those determined in the same participants participating in Study Part 1.
0-30 minutes before infusion up to 72 hours post-infusion
Study Parts 1 and 3: Mean Residence Time (MRT)
Time Frame: 0-30 minutes before infusion up to 72 hours post-infusion
Computed as Area under the moment curve 0-∞ (AUMC0-∞) / AUC0-∞- TI/2, where AUMC0-∞ will be determined in a similar manner as AUC0-∞ and TI represents infusion duration [hr] The objective of Study Part 3 was to re-evaluate the Pharmacokinetic (PK) parameters for BAX 326 after a period of 6 months of treatment, in participants who accumulated at least 30 EDs to BAX 326, and to compare them with those determined in the same participants participating in Study Part 1.
0-30 minutes before infusion up to 72 hours post-infusion
Study Parts 1 and 3: Clearance (CL)
Time Frame: 0-30 minutes before infusion up to 72 hours post-infusion
Computed as Dose/ AUC0-∞. The objective of Study Part 3 was to re-evaluate the Pharmacokinetic (PK) parameters for BAX 326 after a period of 6 months of treatment, in participants who accumulated at least 30 EDs to BAX 326, and to compare them with those determined in the same participants participating in Study Part 1.
0-30 minutes before infusion up to 72 hours post-infusion
Study Parts 1 and 3: Incremental Recovery at Cmax (IR at Cmax)
Time Frame: 0-30 minutes before infusion up to 1 hour post-infusion
Defined as (Cmax - Cpre-infusion)/Dose, where maximum concentration (Cmax) will be determined as the highest concentration achieved within one hour after infusion. The objective of Study Part 3 was to re-evaluate the Pharmacokinetic (PK) parameters for BAX 326 after a period of 6 months of treatment, in participants who accumulated at least 30 EDs to BAX 326, and to compare them with those determined in the same participants participating in Study Part 1.
0-30 minutes before infusion up to 1 hour post-infusion
Incremental Recovery (IR) at 30 Minutes Over Time
Time Frame: 0-30 minutes before infusion and 30 minutes post-infusion
IR at 30 Minutes was measured at the following time points during the study: - Part 1 or Part 2, Exposure Day (ED) 1. (If participant was present for Study Part 1, then ED 1 from Part 1 was used. If Participant entered study in Study Part 2, then ED 1 from Part 2 was used.) - Part 2: Week 5 - Part 2: Week 13 - Part 2 or Part 3: Week 26 (Week 26 of study participation) - Study Completion or Termination Visit
0-30 minutes before infusion and 30 minutes post-infusion
Change in Incremental Recovery (IR) at 30 Minutes Over Time
Time Frame: 0-30 minutes before infusion and 30 minutes post-infusion
The median changes in IR at 30 Minutes, calculated as the change in IR value from exposure day 1 (ED1).
0-30 minutes before infusion and 30 minutes post-infusion
Study Parts 1 and 3: Half Life (T 1/2)
Time Frame: 0-30 minutes before infusion up to 72 hours post-infusion
Elimination phase half-life will be determined as ln2/ λz. The objective of Study Part 3 was to re-evaluate the Pharmacokinetic (PK) parameters for BAX 326 after a period of 6 months of treatment, in participants who accumulated at least 30 EDs to BAX 326, and to compare them with those determined in the same participants participating in Study Part 1.
0-30 minutes before infusion up to 72 hours post-infusion
Study Parts 1 and 3: Volume of Distribution at Steady State (Vss)
Time Frame: 0-30 minutes before infusion up to 72 hours post-infusion
Vss computed as CL·MRT. The objective of Study Part 3 was to re-evaluate the Pharmacokinetic (PK) parameters for BAX 326 after a period of 6 months of treatment, in participants who accumulated at least 30 EDs to BAX 326, and to compare them with those determined in the same participants participating in Study Part 1.
0-30 minutes before infusion up to 72 hours post-infusion
Study Part 2: Annualized Bleed Rate (ABR) During Treatment With BAX326
Time Frame: Study Part 2 = 26 weeks ± 1 week (Note: Study Part 1 = 2-4 weeks)
ABR during prophylaxis (twice-weekly) in Part 2 was calculated as (Number of bleeding episodes/observed treatment period in days) * 365.25. The treatment period on prophylaxis was defined as time between the first and the last prophylactic infusions and ABR on prophylaxis was calculated for participants who received a minimum of 3 months of prophylactic treatment with BAX326.
Study Part 2 = 26 weeks ± 1 week (Note: Study Part 1 = 2-4 weeks)
Bleeding Episodes Treated With 1, 2 or ≥3 Infusions of BAX326 by Bleeding Site and Cause
Time Frame: Study Part 2 = 26 weeks ± 1 week (Study Part 2 began at week 3-5)
The number of bleeding episodes treated with 1, 2, or ≥3 infusions of BAX326 to achieve adequate hemostasis. Only infusions required until resolution of bleed were considered.
Study Part 2 = 26 weeks ± 1 week (Study Part 2 began at week 3-5)
Hemostatic Efficacy at Resolution of All Bleeding Episodes (BEs) Treated With BAX326 by Bleeding Site and Cause
Time Frame: At bleed resolution throughout the study period of 22 months (Study Parts 1, 2, and 3)
Rating Scale for Treatment of BEs (4-point ordinal scale): -Excellent: Full relief of pain and cessation of objective signs of bleeding (eg, swelling, tenderness, and decreased range of motion in the case of musculoskeletal hemorrhage) after a single infusion. No additional infusion required for the control of bleeding. Administration of further infusions to maintain hemostasis did not affect this scoring. -Good: Definite pain relief and/or improvement in signs of bleeding after a single infusion. Possibly requires more than 1 infusion for complete resolution. -Fair: Probable and/or slight relief of pain and slight improvement in signs of bleeding after single infusion. Required more than 1 infusion for complete resolution. -None: No improvement or condition worsens.
At bleed resolution throughout the study period of 22 months (Study Parts 1, 2, and 3)
Total Weight-adjusted Dose Per Bleeding Episode (BEs) of All BEs Treated With BAX326 by Bleeding Site and Cause
Time Frame: Study Part 2 = 26 weeks ± 1 week (Note: Study Part 1 = 2-4 weeks)
Study Part 2 = 26 weeks ± 1 week (Note: Study Part 1 = 2-4 weeks)
Consumption of BAX326 Per Event Per Participant
Time Frame: Study Part 2 = 26 weeks ± 1 week (Note: Study Part 1 = 2-4 weeks)
Weight-adjusted consumption of BAX326 by event per participant, i.e., for prophylactic treatment and for treatment of bleeds until resolution of bleed.
Study Part 2 = 26 weeks ± 1 week (Note: Study Part 1 = 2-4 weeks)
Consumption of BAX326 Per Participant: Median Number of Infusions Per Month
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week (Prophylaxis and On-Demand period), Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week (Prophylaxis and On-Demand period), Study Part 3 = 1 week (Total = 29-31 weeks)
Consumption of BAX326 Per Participant: Median Weight-adjusted Consumption Per Month
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week (Prophylaxis and On-Demand period), Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week (Prophylaxis and On-Demand period), Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants Who Developed Inhibitory Antibodies to Factor IX (FIX)
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Occurrence of Total Binding Antibodies of Indeterminate Specificity (Within Assay Variability)
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Occurrence of total binding antibodies of indeterminate specificity (within assay variability) to FIX, antibodies to CHO proteins and rFurin is defined by a dilution of 2 or less increase as compared to levels at screening visit (e.g. negative to 1:20 or 1:40).
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Occurrence of Treatment Related Total Binding Antibodies
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Occurrence of treatment related total binding antibodies to Factor IX (FIX), antibodies to Chinese hamster ovary (CHO) proteins, and recombinant furin (rFurin) is defined by more than 2-dilution increase as compared to levels at screening visit and confirmed specificity (e.g. negative to 1:80)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants Who Experienced Severe Allergic Reactions (e.g. Anaphylaxis)
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants Who Experienced Thrombotic Events
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants With Clinically Significant Changes in Laboratory Parameters: Clinical Chemistry
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Clinically significant changes in chemistry assessments for Alanine Aminotransferase, Albumin, Alkaline Phosphatase, Aspartate Aminotransferase, Bicarbonate, Bilirubin, Blood Urea Nitrogen, Chloride, Glucose, Potassium, Protein (Serum), Sodium. Clinically Significant (CS) defined as: -1. The abnormal value constitutes an adverse event (AE) and, -2. The abnormal value is a symptom of or related to a disease that is already recorded as an AE in Case Report Form (CRF).
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants With Clinically Significant Changes in Laboratory Parameters: Hematology
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Clinically significant changes in hematology assessments for Basophils, Basophils/Leukocytes, Eosinophils, Eosinophils/Leukocytes, Erythrocyte Mean Corpuscular Hemoglobin Concentration, Erythrocyte Mean Corpuscular Volume, Erythrocytes, Hematocrit, Hemoglobin, Leukocytes, Lymphocytes, Lymphocytes/Leukocytes, Monocytes, Monocytes/Leukocytes, Neutrophils, Neutrophils/Leukocytes, Platelets,
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants With Clinically Significant Changes in Laboratory Parameters: Vital Signs
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Clinically significant changes in vital signs assessments for pulse rate, systolic/diastolic blood pressure, respiratory rate, body temperature
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants With Clinically Significant Changes in Laboratory Parameters: Thrombogenic Markers
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Clinically significant changes in thrombogenic markers assessments for thrombin-antithrombin (TAT), prothrombin fragment 1.2, and D-dimer as evaluated by an independent Data Monitoring Committee (DMC)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Adverse Events (AEs) After BAX326 Treatment
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, and Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, and Study Part 3 = 1 week (Total = 29-31 weeks)
Number of Participants With Adverse Events (AEs) After BAX326 Treatment
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, and Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, and Study Part 3 = 1 week (Total = 29-31 weeks)
EuroQoL (Quality of Life)-5 Dimensions (EQ-5D) Total Index Scores
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
EQ-5D is a participant answered questionnaire scoring 5 dimensions - mobility, self-care, usual activities, pain/discomfort and anxiety/depression. The EQ-5D total score ranges from 0 (worst health state) to 1 (perfect health state) and 1 reflects the best outcome.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
EuroQoL (Quality of Life)-5 Dimensions Visual Analogue Scale (EQ-5D VAS) Scores
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Participant rated questionnaire to assess health-related quality of life in terms of a single index value. The VAS component rates current health state on a scale from 0 (worst imaginable health state) to 100 (best imaginable health state); higher scores indicate a better quality of life.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
General Pain Assessment Through a Visual Analog Scale (VAS)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Participant rated assessment of health-related quality of life. The VAS Pain Scale rates current health state on a scale from 0 (no pain) to 100 (worst imaginable pain). For the pain scale, a higher score indicates worse pain.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Short Form (36) Health Survey (SF-36): HRQoL 'Physical Component Score' (PCS)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
The PCS is a summary scale of the dimensions physical functioning, role physical, bodily pain, and general health. The component score is normalized to a standard population. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL 'Mental Health' (MH)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL Physical Functioning' (PF)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL Role-Physical (RP)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL Role-Emotional
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL Bodily Pain
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL Mental Health
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL Vitality
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL Social Functioning
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
SF-36: HRQoL General Health
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Quality of life survey response as measured using the SF-36 questionnaire. Scores range from 0 to 100 with higher scores representing better health. There is no total overall score; scoring is done for both subscores and summary scores. The raw data from the SF-36 items were transformed to norm based scores for each of the 8 HRQoL/SF-36 health domain scores.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Pediatric Quality of Life Questionnaire (PedsQL) Physical Health Summary Score (Ages 12-16)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
The Peds-QL is a generic Health-Related Quality of Life (HR QoL) instrument designed specifically for a pediatric population. It captures the following domains: general health/activities, feelings/emotional, social functioning, school functioning. For this study, the Peds-QL for 12 to 16-year-old subjects was used. Higher scores indicate better quality of life (QOL) for all domains of the Peds-QL. This modular instrument uses a 5-point scale: from 0 (never) to 4 (almost always). Items are reversed scored and linearly transformed to a 0-100 scale as follows: 0=100, 1=75, 2=50, 3=25, 4=0. 4 dimensions (physical, emotional, social, & school functioning) are scored.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Pediatric Quality of Life Questionnaire (PedsQL) Psychosocial Health Summary Score (Ages 12-16)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
The Peds-QL is a generic Health-Related Quality of Life (HR QoL) instrument designed specifically for a pediatric population. It captures the following domains: general health/activities, feelings/emotional, social functioning, school functioning. For this study, the Peds-QL for 12 to 16-year-old subjects was used. Higher scores indicate better quality of life (QOL) for all domains of the Peds-QL. This modular instrument uses a 5-point scale: from 0 (never) to 4 (almost always). Items are reversed scored and linearly transformed to a 0-100 scale as follows: 0=100, 1=75, 2=50, 3=25, 4=0. 4 dimensions (physical, emotional, social, & school functioning) are scored.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Pediatric Quality of Life Questionnaire (PedsQL) Total Score (Ages 12-16)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
The Peds-QL is a generic Health-Related Quality of Life (HR QoL) instrument designed specifically for a pediatric population. It captures the following domains: general health/activities, feelings/emotional, social functioning, school functioning. For this study, the Peds-QL for 12 to 16-year-old subjects was used. Higher scores indicate better quality of life (QOL) for all domains of the Peds-QL. This modular instrument uses a 5-point scale: from 0 (never) to 4 (almost always). Items are reversed scored and linearly transformed to a 0-100 scale as follows: 0=100, 1=75, 2=50, 3=25, 4=0. 4 dimensions (physical, emotional, social, & school functioning) are scored.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Health-Related Quality of Life (HRQoL) Disease-specific: Haem-A-QoL
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
The Haem-A-QOL instrument has been developed and used in hemophilia A patients. As a hemophilia-specific instrument, this measure assesses very specific aspects of dealing with hemophilia. The areas covered by this instrument are: physical health, sports/leisure, school/work, dealing with hemophilia, and outlook for the future. For the Haem-A-QOL, higher scores indicate a worse quality of life. Scores on a scale range between 0 and 100.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Health-Related Quality of Life (HRQoL) Disease-specific: Haemo-QoL - Participants On-Demand (Ages 12-16)
Time Frame: Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
The Haemo-QoL is a quality of life (QoL) assessment instrument for children and adolescents with haemophilia. As a hemophilia-specific instrument, this measure assesses very specific aspects of dealing with hemophilia. For the Haemo-QoL, higher scores indicate a worse quality of life. Scores on a scale range between 0 and 100.
Baseline at either Study Part 1, or Study Part 2, and End of Study (study weeks 29-31)
Health Resource Use - Number of Hospitalizations
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Health Resource Use - Total Days of Hospital Stay
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Health Resource Use - Emergency Room Visits
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Health Resource Use - Unscheduled Doctor's Office Visits
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Health Resource Use - Days Lost From Work or School
Time Frame: Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)
Study Part 1 = 2-4 weeks, Study Part 2 = 26 weeks ± 1 week, Study Part 3 = 1 week (Total = 29-31 weeks)

Collaborators and Investigators

This is where you will find people and organizations involved with this study.

Sponsor

Baxalta now part of Shire

Publications and helpful links

The person responsible for entering information about the study voluntarily provides these publications. These may be about anything related to the study.

General Publications

Study record dates

These dates track the progress of study record and summary results submissions to ClinicalTrials.gov. Study records and reported results are reviewed by the National Library of Medicine (NLM) to make sure they meet specific quality control standards before being posted on the public website.

Study Major Dates

Study Start (Actual)

July 29, 2010

Primary Completion (Actual)

May 3, 2012

Study Completion (Actual)

May 3, 2012

Study Registration Dates

First Submitted

August 2, 2010

First Submitted That Met QC Criteria

August 2, 2010

First Posted (Estimate)

August 3, 2010

Study Record Updates

Last Update Posted (Actual)

May 20, 2021

Last Update Submitted That Met QC Criteria

April 30, 2021

Last Verified

April 1, 2021

More Information

Terms related to this study

Additional Relevant MeSH Terms

Other Study ID Numbers

  • 250901
  • 2009-016720-31 (EudraCT Number)

This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.

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