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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT02907619
Other study ID # B5161004
Secondary ID 2016-001615-21
Status Terminated
Phase Phase 2
First received
Last updated
Start date October 13, 2016
Est. completion date November 22, 2018

Study information

Verified date October 2020
Source Pfizer
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study is an open-label extension to protocol B5161002 and will provide an assessment of the long term safety, efficacy, pharmacodynamics and pharmacokinetics of intravenous dosing of PF 06252616 in boys with Duchenne muscular dystrophy. Approximately 105 eligible subjects will be assigned to receive a monthly individualized maximum tolerated dose based on their tolerability profile/data from B5161002. This study will not contain a placebo comparator. Subjects will undergo safety evaluations (Laboratory, cardiac monitoring, physical exams, x-ray, MRI), functional capacity evaluations (4 stair climb, range of motion, strength testing, Northstar Ambulatory Assessment, upper limb functional testing, six minute walk test and pulmonary function tests) and pharmacokinetic testing.


Recruitment information / eligibility

Status Terminated
Enrollment 59
Est. completion date November 22, 2018
Est. primary completion date November 22, 2018
Accepts healthy volunteers No
Gender Male
Age group 6 Years to 18 Years
Eligibility Inclusion Criteria: 1. Subjects with Duchenne muscular dystrophy who enrolled and completed study B5161002. 2. Signed and dated informed consent document (ICD) indicating that the subject's parent or legal guardian/caregiver has been informed of all pertinent aspects of the study. 3. Subjects and their legal guardians/caregivers who are willing and able to comply with scheduled visits, treatment plan, laboratory tests, and other study procedures. 4. Subject have; 1. Adequate hepatic function on screening laboratory assessments 2. GLDH less than 20 units/liter (2 x upper limit of normal [ULN]) 3. Iron content estimate on the liver MRI within the normal range. Exclusion Criteria: 1. Unwilling or unable (eg, metal implants) to undergo examination with closed MRI. 2. All male subjects who are able to father children and are sexually active and at risk for impregnating a female partner, who are unwilling or unable to use a highly effective method of contraception. In addition, all sexually active male subjects who are unwilling or unable to prevent potential transfer of and exposure to drug through semen to their partners by using a condom consistently and correctly. . 3. Subjects who are investigational site staff members directly involved in the conduct of the study and their family members, site staff members otherwise supervised by the Investigator, or subjects who are related to Pfizer employees directly involved in the conduct of the study. 4. Other severe acute or chronic medical or psychiatric condition or laboratory abnormality that may increase the risk associated with study participation. 5. Participation in other studies involving investigational drug(s), with the exception of B5161002. 6. History of allergic or anaphylactic reaction to a therapeutic or diagnostic protein or additives of this investigational product.

Study Design


Intervention

Biological:
PF-06252616
Either 5mg/kg, 20mg/kg or 40mg/kg will be assigned to a subject based on their maximum tolerated dose from B5161002

Locations

Country Name City State
Canada Alberta Children's Hospital Calgary Alberta
Canada Children's Hospital- London Health Sciences Centre London Ontario
Canada Centre de Readaptation Marie Enfant (CRME) Montreal Quebec
Canada CHU Sainte-Justine Montreal Quebec
Canada UBC Children's and Women's Health Centre of British Columbia Vancouver British Columbia
Italy UOC Farmacia - Istituto Gianna Gaslini, Genova
Italy UOC Medicina Fisica Riabilitativa - Istituto G. Gaslini Genova
Italy UOC Neurologia Pediatrica e Malattie Muscolari Istituto Gianna Gaslini Genova
Italy UOC Radiologia - Istituto Gianna Gaslini, Genova
Italy UOS Dipartimentale Endocrinologia Clinica Sperimentale - Ist. Genova
Italy Dipartimento Pediatrico Universitario-Ospedaliero Endocrinologia Rome
Italy Farmacia Ospedaliera, IRCCS Ospedale Pediatrico Bambino Gesu Rome
Italy IRCCS Ospedale Pediatrico Bambino Gesu - Centro Trials Rome
Italy U.O. Malattie Neuromuscolari e Neurodegenerative, IRCCS Ospedale Pediatrico Bambino Gesu Rome
Japan National Center of Neurology and Psychiatry Kodaira Tokyo
Japan Hyogo college of medicine hospital Nishinomiya-shi Hyogo
United Kingdom Dubowitz Neuromuscular Centre, Institute of Child Health London
United Kingdom Great Ormond Street Hospital London
United Kingdom Clinical Research Facility Newcastle-upon-Tyne
United Kingdom Institute of Genetic Medicine,Muscle Team Newcastle-upon-Tyne
United Kingdom Royal Victoria Infirmary Research Pharmacy Newcastle-upon-Tyne
United States Johns Hopkins Hospital Baltimore Maryland
United States Johns Hopkins Investigational Drug Service Baltimore Maryland
United States Kennedy Krieger Institute Baltimore Maryland
United States Kennedy Krieger Institute Out-patient Center Baltimore Maryland
United States Massachusetts General Hospital Boston Massachusetts
United States Cincinnati Children's Hospital Medical Center Cincinnati Ohio
United States Duke University Medical Center, Lenox Baker Children's Hospital Durham North Carolina
United States Duke University, Investigational Drug Pharmacy Durham North Carolina
United States University of Iowa ICTS, Clinical Research Unit Iowa City Iowa
United States David Geffen School of Medicine at UCLA/UCLA Neurology Los Angeles California
United States Ronald Reagan UCLA Medical Center Los Angeles California
United States Ronald Reagan UCLA Pharmacy Los Angeles California
United States UCLA (David Geffen School of Medicine), Department of Orthopedic Surgery Los Angeles California
United States UCLA Clinical & Translational Research Center Los Angeles California
United States (For Drug deliveries) IDS Pharmacy Minneapolis Minnesota
United States University of Minnesota Masonic Children's Hospital Minneapolis Minnesota
United States Children's Hospital of Philadelphia Philadelphia Pennsylvania
United States Children's Hospital of Pittsburgh of UPMC Pittsburgh Pennsylvania
United States University of California, Davis Medical Center Sacramento California
United States St. Louis Childrens's Hospital Saint Louis Missouri
United States Center for Clinical and Translational Sciences Salt Lake City Utah
United States Investigational Drug Services Salt Lake City Utah
United States University of Utah Hospital Salt Lake City Utah
United States University of Utah School of Medicine Salt Lake City Utah
United States Utah Center for Advanced Imaging and Research (UCAIR) Salt Lake City Utah
United States Utah Program for Inherited Neuromuscular Disorder Salt Lake City Utah

Sponsors (1)

Lead Sponsor Collaborator
Pfizer

Countries where clinical trial is conducted

United States,  Canada,  Italy,  Japan,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of Participants With Dose Reduced or Temporary Discontinuation Due to AEs An adverse event (AE) was any untoward medical occurrence in a clinical investigation participant administered a product; the event did not need to have a causal relationship with the treatment or usage. Treatment-related AEs were determined by the investigator. The number of participants with dose reduced or temporary discontinuation due to both all-causality and treatment-related AEs are presented below. 2 Years
Primary Number of Participants With Severe Treatment-Emergent Adverse Events (TEAEs) An AE was any untoward medical occurrence in a clinical investigation participant administered a product; the event did not need to have a causal relationship with the treatment or usage. TEAEs were AEs occurred following the start of treatment or AEs increasing in severity during treatment. Severe TEAEs were TEAEs that interfered significantly with participants' usual function. Treatment-related TEAEs were determined by the investigator. The number of participants with severe all-causality and treatment-related TEAEs are presented below. 2 Years
Primary Number of Participants Who Discontinued From the Study Due to TEAEs An AE was any untoward medical occurrence in a clinical investigation participant administered a product; the event did not need to have a causal relationship with the treatment or usage. TEAEs were AEs occurred following the start of treatment or AEs increasing in severity during treatment. Treatment-related TEAEs were determined by the investigator. The number of participants who discontinued from the study due to both all-causality and treatment-related TEAEs are presented below. 2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Hematology Hematology evaluation included: hemoglobin, hematocrit, red blood cell (RBC) count, platelets, RBC morphology, white blood cell (WBC) count, absolute lymphocytes, absolute atypical lymphocytes, absolute total neutrophils, absolute total neutrophils count, absolute band cells, absolute basophils, absolute eosinophils and absolute monocytes.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
(ULN=Upper Limit of Normal; LLN=Lower Limit of Normal).
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Coagulation Coagulation evaluation included activated partial thromboplastin time (aPTT) and prothrombin time (PT).
(ULN=Upper Limit of Normal). Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Liver Function Liver function evaluation included: total bilirubin, aspartate aminotransferase (AST), alanine aminotransferase (ALT), gamma-glutamyl transferase (GGT), alkaline phosphatase, total protein, albumin and glutamate dehydrogenase.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
(LLN=Lower Limit of Normal; ULN=Upper Limit of Normal).
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Renal Function Renal function evaluation included: blood urea nitrogen (BUN), creatinine and uric acid.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. (ULN=Upper Limit of Normal).
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Electrolytes Electrolytes evaluation included: sodium, potassium, chloride, calcium, phosphate and bicarbonate.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
(LLN=Lower Limit of Normal, ULN=Upper Limit of Normal).
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Hormones Hormone evaluations included free thyroxine (T4), thyroid stimulating hormone (TSH), lutenizing hormone (LH), follicle stimulating hormone (FSH), and androstenedione. Numbers of participants with abnormalities of LH, FSH and androstenedione were reported in different age groups.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
(LLN=Lower Limit of Normal, ULN=Upper Limit of Normal).
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Clinical Chemistry Clinical chemistry evaluation included glucose, creatine kinase (CK), troponin I, amylase, iron binding capacity, unsaturated iron binding capacity, transferrin saturation, iron and ferritin. Number of participants with iron abnormalities was reported in different age groups.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
(LLN=Lower Limit of Normal, ULN=Upper Limit of Normal).
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Urinalysis Urinalysis Microscopy included: urine red blood cell (RBC), urine white blood cell (WBC), urine uric acid crystals, urine calcium oxalate crystals, urine amorphous crystals, urine bacteria, urine microscopic exam.
Urinalysis Dipstick included: urine pH, urine glucose, urine ketones, urine protein, urine blood/hemoglobin, urine nitrite, urine leukocyte esterase.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
2 Years
Primary Number of Participants With Laboratory Test Abnormalities (Without Regard to B5161004 Baseline Abnormality) - Fecal Blood Number of participants with blood detected in fecal samples is presented. Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
(ULN=Upper Limit of Normal).
2 Years
Primary Number of Participants With Data of Serum Ferritin, Serum Iron and % Transferrin Saturation Meeting Categorical Summarization Criteria - B5161004 Baseline Participants were asked to fast for at least 8 hours prior to collection of blood to evaluate serum iron, serum ferritin and % transferrin saturation. The unit of iron was mcg/dL; the unit of ferritin was ng/mL; the unit of %transferrin saturation was %.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 37, 49, 61, 73 and 85.
Primary Number of Participants With Significant Results of Physical Examinations Including Nose and Throat Mucosal Examinations Physical examinations were conducted by a physician, trained physician's assistant, or nurse practitioner as acceptable according to local regulation. A targeted nose and throat mucosal exam was performed to monitor for any signs of mucosal telangiectasias. The clinically significant physical examination results were determined by the investigator. 2 Years
Primary Summary of Pubertal Development by Tanner Stage Tanner staging was performed before the first dose of this study to monitor for signs of accelerated sexual development. The physical changes in pubertal development (pubic hair, penis and testes) were assessed using the system described by Marshall and Tanner. Stage 1 is preadolescent, Stages 2, 3, and 4 are initiation of puberty and Stage 5 is mature adult. Details about the system can be referred to Tanner JM. Growth at Adolescence. Blackwell Scientific Publications 1962; 2nd edition.
Participant's Week 97 visit within study B5161002 (parent study) was collected as screening data.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Screening, Baseline, Week 49.
Primary Summary of Testicular Volume Testicular volume was used to monitor pubertal development. Participant's Week 97 visit within Study B5161002 (parent study) was collected as screening data in current study.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Screening, Baseline, Week 49.
Primary Number of Participants With Post-Baseline Vital Signs Data Meeting Categorical Summarization Criteria - B5161004 Baseline The number of participants pre-dose supine blood pressure and pulse rate meeting categorical summarization criteria are recorded in this table.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004.
(DBP=diastolic blood pressure, SBP=systolic blood pressure; The unit for blood pressure is: mmHg, the unit for pulse rate is: beats per minute [BPM])
2 Years
Primary Number of Participants With Post-Baseline Vital Signs Data Meeting Categorical Summarization Criteria - Overall Baseline The number of participants with data of pre-dose supine blood pressure meeting categorical summarization were recorded in this table.
Overall Baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002.
(DBP=diastolic blood pressure, SBP=systolic blood pressure; The unit for blood pressure is: mmHg).
2 Years
Primary Number of Participants With Post-Baseline ECG Data Meeting Categorical Summarization Criteria - B5161004 Baseline QTcF=QT/(60/Hour)**(1/3). Means of replicates were used in the calculations. QT=time between the start of the Q wave and the end of the T wave in the heart's electrical cycle; QTcF=corrected QT (Fridericia correction). All scheduled ECGs were performed after the participant had rested quietly for at least 10 minutes in a supine position.
Baseline was defined as the average of the last triplicate pre-dose measurements prior to Day 1 in B5161004.
2 Years
Primary Number of Participants With Post-Baseline ECG Data Meeting Categorical Summarization Criteria - Overall Baseline QT=time between the start of the Q wave and the end of the T wave in the heart's electrical cycle; QTcF=corrected QT (Fridericia correction). All scheduled ECGs were performed after the participant had rested quietly for at least 10 minutes in a supine position.
Overall baseline was defined as the average of the last triplicate pre-dose measurements prior to the first day of dosing in study B5161002.
2 Years
Primary Number of Participants With Iron Accumulation Data Meeting Categorical Summarization Criteria Liver Magnetic Resonance Imaging (MRIs) were sent to an independent central radiology imaging facility for calculation of the average R2* value which was used to monitor for iron accumulation in the liver. Mean R2* values had been used in the calculations.
Normal: R2* <= 75 Hz at 1.5 T or <=139 Hz at 3.0 T; Above Normal: R2* > 75 Hz and <= 190 Hz at 1.5 T or R2* > 139 Hz and <= 369 Hz at 3.0 T Mild overload: R2* > 190 Hz at 1.5 T or R2* > 369 Hz at 3.0 T Data from participant's Week 93 visit in Study B5161002 (parent study) were used for screening in the current study.
Screening and Week 49.
Primary Change From Baseline in Left Ventricular Ejection Fraction (LVEF) by Cardiac MRI - B5161004 Baseline The LVEF was the ratio of blood ejected during systole to blood in the ventricle at the end of diastole. LVEF was measured by cardiac magnetic resonance imaging (MRI) or echocardiography. The same method of cardiac imaging was used consistently for each participant. Cardiac MRIs were read by a central imaging vendor, while echocardiograms were read locally (at each site). The table presents the results from cardiac MRIs. Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004. Baseline and Week 49.
Primary Change From Baseline in Left Ventricular Ejection Fraction (LVEF) by Cardiac MRI - Overall Baseline The LVEF was the ratio of blood ejected during systole to blood in the ventricle at the end of diastole. LVEF was measured by cardiac magnetic resonance imaging (MRI) or echocardiography. The same method of cardiac imaging was used consistently for each participant. Cardiac MRIs were read by a central imaging vendor, while echocardiograms were read locally (at each site). The table presents the results from cardiac MRIs.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 49, 97, 146.
Primary Change From Baseline in Left Ventricular Ejection Fraction (LVEF) by Echocardiogram - B5161004 Baseline The LVEF was the ratio of blood ejected during systole to blood in the ventricle at the end of diastole. LVEF was measured by cardiac magnetic resonance imaging (MRI) or echocardiography. The same method of cardiac imaging was used consistently for each participant. Cardiac MRIs were read by a central imaging vendor, while echocardiograms were read locally (at each site). The table presents the results from echocardiograms.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Week 49.
Primary Change From Baseline in Left Ventricular Ejection Fraction (LVEF) by Echocardiogram - Overall Baseline The LVEF was the ratio of blood ejected during systole to blood in the ventricle at the end of diastole. LVEF was measured by cardiac magnetic resonance imaging (MRI) or echocardiography. The same method of cardiac imaging was used consistently for each participant. Cardiac MRIs were read by a central imaging vendor, while echocardiograms were read locally (at each site). The table presents the results from echocardiograms.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 49, 97, 146.
Primary Bone Age to Chronological Age Ratio Bone age assessment was evaluated by the ratio of the bone age to the chronological age using the X rays of the hand and wrist. Ratio of bone age to chronological age was calculated by bone age/chronological age at scan date. Chronological age at scan date was calculated by (scan date - date of birth + 1)/365.25.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline and Week 49.
Primary Whole Body and Spine DXA: Bone Mineral Density Z-Score, Height Adjusted Over Time Bone mineral density (BMD) was monitored by dual energy x-ray absorptiometry (DXA). DXA scans were obtained to evaluate bone mineral density of the spine and whole body without head.
The height adjusted Z-score presented below is the number of standard deviations which compares the BMD of the participant to the average BMD matched for their age, sex and ethnicity. If the Z-score was -2 standard deviations or lower, the result was "below the expected range for age". If the Z-score was above -2 standard deviations, the result was "within the expected range for age".
Screening (Week 97 visit within parent study B5161002) and Week 49
Primary Number of Participants With Suicidal Ideation or Suicidal Behavior The Columbia Suicide Severity Rating Scale (C-SSRS) was performed to identify the risk of suicide ideation or behavior. C-SSRS was conducted with the participant's caregiver/legal guardian on the participant's behalf throughout the study, rather than administering this evaluation directly with the study participants. If at any visit the participant endorsed a 4 or 5 on the C-SSRS ideation section or reported any suicidality behavior, then an evaluation of suicide risk (risk assessment) had to be completed and the participant must have been discontinued. The significant result of C-SSRS was determined by the investigator. 2 Years
Secondary Change From Baseline on the 4 Stair Climb (4SC) - B5161004 Baseline The 4SC quantified the time required for a participant to ascend 4 standard steps. The functional assessment of 4SC was conducted by a physiotherapist (or exercise physiologist). In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessments were completed at approximately the same time of day.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49, 73.
Secondary Change From Baseline on the 4SC - Overall Baseline The 4SC quantified the time required for a participant to ascend 4 standard steps. The functional assessment of 4SC was conducted by a physiotherapist (or exercise physiologist). In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessments were completed at approximately the same time of day.
This is the overall change from baseline which included the change since enrolling in the parent study B5161002.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the Forced Vital Capacity (FVC) - B5161004 Baseline FVC was measured using the FVC maneuver by spirometry to evaluate respiratory muscle function. The best (largest) FVC measurement from a set of 3 was captured on the database.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49 and 73.
Secondary Change From Baseline on the FVC - Overall Baseline Forced vital capacity (FVC) was measured using the FVC maneuver by spirometry to evaluate respiratory muscle function. The best (largest) FVC measurement from a set of 3 was captured on the database. This is the overall change from baseline which included the change since enrolling in the parent study B5161002.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the Northstar Ambulatory Assessment (NSAA) Score - B5161004 Baseline The NSAA was a 17-item test that measured gross motor function. Each individual item was evaluated with either 0-unable to perform independently, 1-able to perform with assistance, 2-able to perform without assistance. A total score was achieved by summing all the individual items. The total score could range from 0 to 34 (fully-independent function).
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49, 73.
Secondary Change From Baseline on the NSAA Score - Overall Baseline The NSAA was a 17-item test that measured gross motor function. Each individual item was evaluated with either 0-unable to perform independently, 1-able to perform with assistance, 2-able to perform without assistance. A total score was achieved by summing all the individual items. The total score could range from 0 to 34 (fully-independent function). This is the overall change from baseline which included the change since enrolling in the parent study B5161002.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the NSAA - Time to Stand From Supine - B5161004 Baseline Rise from supine was a timed functional test within NSAA. This test of time-to-stand from supine was analyzed separately for summary tabulation along with the total NSAA score.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49, 73.
Secondary Change From Baseline on the NSAA - Time to Stand From Supine - Overall Baseline Rise from supine was a timed functional test within NSAA. This test of time-to-stand from supine was analyzed separately for summary tabulation along with the total NSAA score. This is the overall change from baseline which included the change since enrolling in the parent study B5161002.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the NSAA - Time to Complete 10 m Run/Walk - B5161004 Baseline A time to event analysis was performed for loss of ambulation. Loss of ambulation was defined as the inability to walk unassisted and without braces for at least 10 m, as assessed and reported by the investigator at each study visit, and confirmed by the inability to walk/run 10 m (as 1 component of the NSAA) evaluated at the next visit at which timed function tests were performed.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49, 73.
Secondary Change From Baseline on the NSAA - Time to Complete 10 m Run/Walk - Overall Baseline A time to event analysis was performed for loss of ambulation. Loss of ambulation was defined as the inability to walk unassisted and without braces for at least 10 m, as assessed and reported by the investigator at each study visit, and confirmed by the inability to walk/run 10 m (as 1 component of the NSAA) evaluated at the next visit at which timed function tests were performed. This is the overall change from baseline which included the change since enrolling in the parent study B5161002.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the Ankle Range of Motion (ROM) - B5161004 Baseline ROM of the ankle was evaluated by goniometry and any occurrences of ankle contractures were recorded. In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessment of ankle ROM was completed at approximately the same time of day.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49 and 73.
Secondary Change From Baseline on the Ankle ROM - Overall Baseline ROM of the ankle was evaluated by goniometry and any occurrences of ankle contractures were recorded. In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessment of ankle ROM was completed at approximately the same time of day. This is the overall change from baseline which included the change since enrolling in the parent study B5161002.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the Performance of Upper Limb (PUL) Overall Score - B5161004 Baseline The PUL scale was used to assess motor performance of the upper limb for individuals with DMD. The PUL scale includes 22 items; an entry item defining the starting functional level, and 21 items subdivided into 3 levels; shoulder (4 items), middle (9 items) and distal (8 items). Scoring options per item may not be uniform and may vary from 0-1 to 0-6, according to the performance, with higher values corresponding to better performance. A total maximum score of 74 is achieved by adding the individual level scores; shoulder maximum 16, middle level maximum score 34 and distal level maximum score 24. In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessment of PUL was completed at approximately the same time of day.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49 and 73.
Secondary Change From Baseline on the PUL Overall Score - Overall Baseline The PUL scale was used to assess motor performance of the upper limb for individuals with DMD. The PUL scale includes 22 items; an entry item defining the starting functional level, and 21 items subdivided into 3 levels; shoulder (4 items), middle (9 items) and distal (8 items). Scoring options per item may not be uniform and may vary from 0-1 to 0-6, according to the performance, with higher values corresponding to better performance. A total maximum score of 74 is achieved by adding the individual level scores; shoulder maximum 16, middle level maximum score 34 and distal level maximum score 24.
This is the overall change from baseline which included the change since enrolling in parent study B5161002. Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was counted starting from the study treatment in study B5161002.
Baseline, Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the Six Minute Walk Distance (6MWD) - B5161004 Baseline The 6MWD evaluated ambulation ability by measuring the distance walked in 6 minutes. In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessment of 6MWD was completed at approximately the same time of day.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49 and 73.
Secondary Change From Baseline on the 6MWD - Overall Baseline The 6MWD evaluated ambulation ability by measuring the distance walked in 6 minutes. In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessment of 6MWD was completed at approximately the same time of day. This is the overall change from baseline which included the change since enrolling in the parent study B5161002.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was start of the study treatment in parent study B5161002.
Baseline,Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Change From Baseline on the Forced Expiratory Volume in One Second (FEV1) - B5161004 Baseline The FEV1 was recorded as an absolute volume in litres and in terms of predicted values according to age, height, race and gender. The best single FEV1 measurement from a set of 3 was recorded in the database.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49 and 73.
Secondary Change From Baseline on the Peak Expiratory Flow Rate (PEFR)- B5161004 Baseline PEFR was one of the Pulmonary Function Tests (PFTs). Three technically adequate peak expiratory flow rate (PEFR) maneuvers were performed and reported in Litres/Minute (L/min), and the highest single PEFR was reported in the database. In order to provide optimal testing conditions and consistency in endpoint measurements, the functional assessment of PEFR was completed at approximately the same time of day.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49 and 73.
Secondary Change From Baseline on the Myometry Based Muscle Strength - B5161004 Baseline Muscle strength was quantified by means of a handheld dynamometer. The following muscle groups were evaluated: knee extension, elbow flexion, elbow extension, hip abduction and shoulder abduction. 95% Confidence Interval was not calculated when less than or equal to 3 participants' data were available.
Baseline was defined as the last assessment prior to dosing on Day 1 in B5161004. Week 1 was counted starting from the study treatment in study B5161004.
Baseline, Weeks 13, 25, 49, 73.
Secondary Change From Baseline on the Myometry Based Muscle Strength - Overall Baseline Muscle strength was quantified by means of a handheld dynamometer. The following muscle groups were evaluated: knee extension, elbow flexion, elbow extension, hip abduction and shoulder abduction. 95% Confidence Interval was not calculated when less than or equal to 3 participants' data were available.
Overall baseline was defined as the last pre-dose assessment prior to the first day of dosing in study B5161002. Week 1 was start of the study treatment in parent study B5161002.
Baseline,Weeks 9,17,25,33,41,49,57,65,73,81,89,97,110,122,146,170.
Secondary Serum PF-06252616 (Domagrozumab) Concentration Versus Time Summary Weeks 1, 25, 49 and 73
Secondary Number of Participants With Anti-drug Antibodies (ADA) Development The criterion for positive result of ADA samples was ADA titer >=1.88. The criterion for negative result of ADA samples was ADA titer <1.88. Weeks 1, 25, 49, 73 and Early Termination
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