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A Study Comparing ATB200/AT2221 With Alglucosidase Alfa/Placebo in Adult Subjects With Late-onset Pompe Disease (PROPEL)

Primary Purpose

Pompe Disease (Late-onset)

Status

Completed

Phase

Phase 3

Locations

International

Study Type

Interventional

Intervention

Cipaglucosidase Alfa

Miglustat

Alglucosidase Alfa

Placebo

About this trial

This is an interventional treatment trial for Pompe Disease (Late-onset) focused on measuring Pompe, rhGAA

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

Subject must provide signed informed consent prior to any study-related procedures being performed.
Male and female subjects are ≥ 18 years old and weigh ≥ 40 kg at screening.
Female subjects of childbearing potential and male subjects must agree to use medically accepted methods of contraception during the study and for 90 days after the last dose of study drug.
Subject must have a diagnosis of LOPD based on documentation of one of the following:
1. deficiency of GAA enzyme
2. GAA genotyping
Subject is classified as one of the following with respect to ERT status:
1. ERT-experienced, defined as currently receiving standard of care ERT (alglucosidase alfa) at the recommended dose and regimen (ie, 20 mg/kg dose every 2 weeks) for ≥ 24 months
2. ERT-naïve, defined as never having received investigational or commercially available ERT
Subject has a sitting FVC ≥ 30% of the predicted value for healthy adults (National Health and Nutrition Examination Survey III) at screening.
Subject performs two 6MWTs at screening that are valid, as determined by the clinical evaluator, and that meet all of the following criteria:
1. both screening values of 6MWD are ≥ 75 meters
2. both screening values of 6MWD are ≤ 90% of the predicted value for healthy adults
3. the lower value of 6MWD is within 20% of the higher value of 6MWD

Exclusion Criteria

Subject has received any investigational therapy or pharmacological treatment for Pompe disease, other than alglucosidase alfa, within 30 days or 5 half-lives of the therapy or treatment, whichever is longer, before Day 1 or is anticipated to do so during the study.
Subject has received gene therapy for Pompe disease
Subject is taking any of the following prohibited medications within 30 days before Day 1:
- miglitol (eg, Glyset)
- miglustat (eg, Zavesca)
- acarbose (eg, Precose or Glucobay)
- voglibose (eg, Volix, Vocarb, or Volibo)
Note: None of these medications have a half-life that, when multiplied by 5, is longer than 30 days.
Subject requires the use of invasive or noninvasive ventilation support for > 6 hours per day while awake.
Subject has a hypersensitivity to any of the excipients in ATB200, alglucosidase alfa, or AT2221.
Subject has a medical condition or any other extenuating circumstance that may, in the opinion of the investigator or medical monitor, pose an undue safety risk to the subject or may compromise his/her ability to comply with or adversely impact protocol requirements. This includes clinical depression (as diagnosed by a psychiatrist or other mental health professional) with uncontrolled or poorly controlled symptoms.
Subject, if female, is pregnant or breastfeeding at screening.
Subject, whether male or female, is planning to conceive a child during the study.
Subject does not have documentation of diagnosis of Pompe disease and refuses to undergo genetic testing.

Sites / Locations

Neuromuscular Research Center
University of Arkansas for Medical Sciences
University of California, Irvine
UF Helath: University of Florida Clinical Research Center
University of South Florida Research Center
Emory Clinic
Indiana University Health Neuroscience Center
University of Kansas Medical Center
University of Minnesota Clinical Research Unit
Washington University School of Medicine
Billings Clinic
Hackensack University Medical Center
The Feinstein Institute for Medical Research
NYU School of Medicine
Duke University Medical Center
University of Cincinnati Neurology
Cincinnati Children's Hospital Medical Center
The Ohio State University Wexner Medical Center
Oregon Health & Science University
Penn State Health Milton S. Hershey Medical Center
University of Pennsylvania
University of Pittsburgh
University of Texas Health Science Center San Antonio
University of Utah, Center for Clinical and Translational Sciences
Lysosomal and Rare Disorders Research
Hospital Universitario Austral
Royal Brisbane & Women's Hospital
Royal Adelaide Hospital
Monash Medical Centre
Westmead Hospital
Medizinische Universität Innsbruck
UZ Leuven
University Clinical Centre of the Republic of Srpska
UMHAT Alexandrovska
Heritage Medical Research Clinic, University of Calgary
McMaster University Medical Centre
Aarhus Universitets Hospital
Rigshospitalet Copenhagen Neuromuscular Center
Hôpital Neurologique Pierre Wertheimer
Hôpital Raymond Poincaré
Hôpital Salengro
Hôpital de la Timone
Hôpital Pasteur
Friedrich-Baur Institut
Universitätsklinikum Bonn
Universitätsklinikum Münster
Universitätsklinikum Halle (Saale)
Eginition Hospital
Semmelweis University, Institute of Genomic Medicine and Rare Disease
University of Pécs
University of Szeged
UOC di Neurologia e Malattie Neuromuscolari
UOC Genetica Medica
Hokkaido University Hospital
Fukuoka University Hospital
Kagoshima University Hospital
Izumi City General Hospital
The Jikei University Hospital
National Center of Neurology and Psychiatry
Pusan National University
Seoul National University Hospital
Erasmus MC
University of Auckland
Szpital Uniwersytecki w Krakowie
Centrum Medyczne
University Medical Centre Ljubljana
Hospital de la Santa Creu I Sant Pau
Sahlgrenska University Hospital
National Taiwan University Hospital
Queen Elizabeth Hospital Birmingham
Cambridge University Hospitals
Royal Free Hospital NHS
Salford Royal NHS Foundation Trust

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Active Comparator

Arm Label

Cipaglucosidase Alfa/Miglustat

Alglucosidase Alfa/Placebo

Arm Description

Participants received cipaglucosidase alfa co-administered with miglustat every 2 weeks (Q2W).

Participants received alglucosidase alfa co-administered with placebo Q2W.

Outcomes

Primary Outcome Measures

Change From Baseline to Week 52 in 6 Minute Walk Distance (6MWD)

The efficacy of cipaglucosidase alfa/miglustat co-administration on ambulatory function was measured by the 6MWT. The 6MWD, measured in meters, is the distance walked on the 6MWT. A greater distance indicated greater endurance. An increase from baseline indicated improvement.

Secondary Outcome Measures

Change From Baseline to Week 52 in Sitting Forced Vital Capacity (FVC; % Predicted)

The efficacy of cipaglucosidase alfa/miglustat co-administration on pulmonary function was measured by sitting FVC (% predicted). FVC is a standard pulmonary function test used to quantify respiratory muscle weakness.

Change From Baseline to Week 52 in the Manual Muscle Test (MMT) Score for the Lower Extremities

The total score for the MMT lower extremity strength included the following 8 body parts: right/left hip flexion, right/left hip abduction, right/left knee flexion and right/left knee extension. The MMT lower extremity score ranged from 0 to 40, with lower scores indicating weaker muscle strength. An increase from baseline indicated increased muscle strength.

Change From Baseline to Week 26 in 6MWD

The 6MWD, measured in meters, is the distance walked on the 6MWT.

Change From Baseline to Week 52 in the Total Score for the Patient- Reported Outcomes Measurement Information System (PROMIS®) - Physical Function

Physical Function Short Form 20a (v2.0) consisted of 20 questions. The first 14 questions were each scored on a scale from 1 to 5 as follows: 1 = unable to do; 2 = with much difficulty; 3 = with some difficulty; 4 = with a little difficulty; 5 = without any difficulty; the next 6 questions were each scored on a scale from 1 to 5 as follows: 1 = cannot do; 2 = quite a lot; 3 = somewhat; 4 = very little; 5 = not at all. The total score was calculated by summing up scores (1 to 5) across all items. Total scores range from 20 to 100. A higher score represented a better outcome.

Change From Baseline to Week 52 in the Total Score for the PROMIS® - Fatigue

Fatigue Short Form 8a consisted of 6 questions, each scored on a scale from 1 to 5 as follows: 1 = not at all; 2 = a little bit; 3 = somewhat; 4 = quite a bit; 5 = very much; and 2 questions, each scored on a scale from 1 to 5 as follows: 1 = never; 2 = rarely; 3 = sometimes; 4 = often; 5 = always. The total score was calculated by summing up scores (1 to 5) across all items. A lower score represented lower fatigue symptoms.

Change From Baseline to Week 52 in the Total Score for the Gait, Stairs, Gowers' Maneuver, and Chair (GSGC)

The GSGC consisted of a 10-meter walk for evaluation of gait, a 4-stair climb, Gowers' maneuver, and arising from a chair. Results of the GSGC included the time required to complete the individual tests, individual scores for each of the tests (1 to 7 points for each of gait, 4-stair climb, and Gowers' maneuver, and 1 to 6 points for arising from a chair), and a total score. GSGC total score was the sum of the component scores from the 4 functional tests. The total score ranged from a minimum of 4 points (normal performance) to a maximum of 27 points (worst performance).

Change From Baseline to Week 52 in Rasch-Built Pompe-Specific Activity (R-PAct) Total Score

The R-PAct scale was an 18-item questionnaire to measure limitations in activities and restriction in social participation. Possible responses to questions were as follows: unable to perform, able to perform, but with difficulty, and able to perform without difficulty. The total score was calculated by summing up the observed scores across the 18 items and it ranged from 0 to 36, with higher values representing lower level of disease impact on the muscles.

Change From Baseline to Week 52 in European Quality of Life-5 Dimensions 5 Response Levels (EQ-5D-5L) Based on the EuroQol Visual Analogue Scale (EQ VAS) Quantitative Score

The EuroQol Visual Analogue Scale (EQ VAS) is a vertical visual analogue scale that records the respondent's own assessment of his or her overall health status at the time of completion. Scores range from 0 (the worst health you can imagine) to 100 (the best health you can imagine). Higher EQ VAS scores represent an improved sense of overall health while lower scores represent a worsening of overall health.

Change From Baseline to Week 52 in Sitting Slow Vital Capacity (SVC) % Predicted

SVC is a standard pulmonary function test used to quantify respiratory muscle weakness.

Change From Baseline to Week 52 in Maximal Inspiratory Pressure (MIP) % Predicted

The percent predicted values of MIP were calculated as: % predicted = (actual result / predicted result)* 100, where the predicted results were obtained using the reference equations from Uldry and Fitting (1995).

Change From Baseline to Week 52 in Maximal Expiratory Pressure (MEP) % Predicted

The percent predicted values of MEP were calculated as: % predicted = (actual result / predicted result) * 100, where the predicted results were obtained using the reference equations from Uldry and Fitting (1995).

Change From Baseline to Week 52 in Sniff Nasal Inspiratory Pressure (SNIP) % Predicted

The percent predicted values of SNIP were calculated as: % predicted = (actual result / predicted result) * 100, where the predicted results were obtained using the reference equations from Evans and Whitelaw (2009).

Change From Baseline to Week 52 in % Predicted 6MWD

The % predicted 6MWD = (actual 6MWD / predicted 6MWD) * 100. The predicted values were calculated using Enright And Sherrill 1998 Reference Equations.

Change From Baseline to Week 52 in the Quantitative Muscle Test (QMT) Values

QMT was measured using the hand-held dynamometer. Larger values (in kg) indicated greater muscle strength.

Change From Baseline to Week 52 in Other MMT Scores

Each manual muscle test was evaluated on a scoring scale from 0 to 5, as follows: 0 = no muscle movement; 1 = visible muscle movement, but no movement at the joint; 2 = movement at the joint, but not against gravity; 3 = movement against gravity, but not against added resistance; 4 = movement against resistance, but less than normal; 5 = normal strength. Upper extremity score was the sum of scores for right/left shoulder abduction, right/left shoulder adduction, right/left elbow extension, and right/left elbow flexion, with the total score ranging from 0 to 40. Proximal muscle group score, the sum of scores for right/left hip flexion, right/left hip abduction, right/left shoulder abduction, and right/left shoulder adduction, with the total score ranging from 0 to 40. MMT total score was the sum of the lower and upper extremity scores and ranged from 0 to 80. Lower scores indicated lower overall muscle strength. An increase from baseline indicated improvement in muscle strength.

Change From Baseline to Week 52 in Maximum Vital Capacity (Maximum VC) % Predicted

Maximum VC is the greater of the two VC values (FVC or SVC).

Change From Baseline to Week 52 in PROMIS-Dyspnea and Upper Extremities Total Scores

The Upper Extremities Short Form 7a consisted of 7 items each scored on a decreasing scale from 1 to 5 as follows: 1 = unable to do; 2 = with much difficulty; 3 = with some difficulty; 4 = with a little difficulty; 5 = without any difficulty. Dyspnea Severity Short Form 10a consisted of 10 items each scored on a scale from 0 to 3 as follows: 0 = no shortness of breath; 1 = mildly short of breath; 2 = moderately short of breath; 3 = severely short of breath. A total score was generated for each instrument by adding up each item. Total scores for upper extremities range from 7 to 35. Total scores for dyspnea range from 0 to 30. A higher score for upper extremities represented improvement in symptoms. A lower score for dyspnea severity represented improvement in symptoms.

Change From Baseline in the Time to Complete Individual GSGC Component Tests and Timed Up and Go (TUG) Test at Week 52

Motor function test assessed the time to complete individual GSGC component tests (10-meter walk, 4- stair climb, Gowers' maneuver, and arise from a chair) and the TUG test. The TUG test assessed the time a subject needed to rise from a chair, walk 3 meters, turn around, walk back to the chair, and sit down.

Physician's Global Impression of Change (PGIC) Overall Status at Week 52

Physician's Global Impression of Change is based on a single item that is scored on a 7-point rating scale ranging from 1 "very much worse" to 7 "very much improved". A tertiary response variable (improving, declining, stable) was defined as follows: "Improving", which consisted of improved, moderately improved, and very much improved; "Declining", which consisted of worse, moderately worse, and very much worse; and "Stable", which equaled to no change.

Subject's Global Impression of Change (SGIC) at Week 52

The SGIC is designed to record the participants' impression of their functional status since starting study drug using a 7-point scale ranging from 1 "very much worse" to 7 "very much improved". A tertiary response variable (improving, declining, stable) was defined as follows: "Improving", which consisted of improved, moderately improved, and very much improved; "Declining", which consisted of worse, moderately worse, and very much worse; and "Stable", which equaled to no change.

Number of Participants Improving on Both 6MWD and % Predicted FVC at Week 52

A composite subject-level response of the 2 relevant clinical outcomes, 6MWD and FVC (% predicted), was assessed. Prespecified thresholds were used for assessment of improvement consistent with published minimal clinically important difference values for comparable instruments in similar disease.

Number of Participants With Treatment-Emergent Anti-Drug Antibodies (ADAs)

Treatment-emergent ADAs were defined as participants who had seroconverted or boosted their preexisting ADA during the study period.

Change From Baseline to Week 52 in Urinary Hexose Tetrasaccharide (Hex4) Level

Levels of urinary Hex4, a biomarker of disease substrate, were measured. The assay specifically targets Hex4, the glucose tetrasaccharide (Glc4), which is a biomarker of glycogen storage.

Change From Baseline to Week 52 in Serum Creatine Kinase (CK) Level

Change from baseline to Week 52 in serum CK level. CK levels were measured as part of the serum chemistry panel.

Population Pharmacokinetics (PK): Maximum Observed Concentration (Cmax) of Cipaglucosidase Alfa and Alglucosidase Alfa in ERT-Experienced Participants Using Plasma Total GAA Protein Level by Signature Peptide Assay and Plasma Miglustat Concentration

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis in ERT-experienced participants at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Population PK: Area Under the Concentration-Time Curve (AUC) of Cipaglucosidase Alfa and Alglucosidase Alfa in ERT-Experienced Participants Using Plasma Total GAA Protein Level by Signature Peptide Assay and Plasma Miglustat Concentration

Population PK: Cmax of Cipaglucosidase Alfa and Alglucosidase Alfa in ERT-Naïve Participants

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis in ERT-naïve participants at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Population PK: AUC of Cipaglucosidase Alfa and Alglucosidase Alfa in ERT-Naïve Subjects

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis in ERT-naïve participants at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Noncompartmental Analysis: Cmax of Plasma Total GAA Protein by Signature Peptide T09 in ERT-Naïve Subjects

A noncompartmental analysis was performed on ERT-naïve subjects, who underwent serial PK sampling during the study. On Day 1, serial blood samples were collected for ERT-naïve participants just prior to initiation of cipaglucosidase alfa/alglucosidase alfa infusion (time 0) and at 1, 2, 3, 3.5, 4, 4.5, 6, 8, 10, and 24 hours after the start of cipaglucosidase alfa/alglucosidase alfa infusion for plasma total human acid α-glucosidase (GAA) protein signature peptide T09 and plasma miglustat determinations.

Noncompartmental Analysis: AUC From Time 0 (Predose) to the Time of Last Quantifiable Concentration of Plasma Total GAA Protein by Signature Peptide T09 in ERT-Naïve Subjects

A noncompartmental analysis was performed on ERT-naïve subjects, who underwent serial PK sampling during the study. On Day 1, serial blood samples were collected for ERT-naïve participants just prior to initiation of cipaglucosidase alfa/alglucosidase alfa infusion (time 0) and at 1, 2, 3, 3.5, 4, 4.5, 6, 8, 10, and 24 hours after the start of cipaglucosidase alfa/alglucosidase alfa infusion for plasma total GAA protein signature peptide T09 and plasma miglustat determinations.

Comparison of Cmax of Cipaglucosidase Alfa in ERT-Experienced and ERT-Naïve Populations

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Comparison of AUC of Cipaglucosidase Alfa in ERT- Experienced and ERT-Naïve Populations

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Full Information

NCT ID

NCT03729362

First Posted

October 10, 2018

Last Updated

August 25, 2023

Sponsor

Amicus Therapeutics

1. Study Identification

Unique Protocol Identification Number

NCT03729362

Brief Title

A Study Comparing ATB200/AT2221 With Alglucosidase Alfa/Placebo in Adult Subjects With Late-onset Pompe Disease

Acronym

PROPEL

Official Title

A Phase 3 Double-blind Randomized Study to Assess the Efficacy and Safety of Intravenous ATB200 Co-administered With Oral AT2221 in Adult Subjects With Late-onset Pompe Disease Compared With Alglucosidase Alfa/Placebo

Study Type

Interventional

2. Study Status

Record Verification Date

June 2023

Overall Recruitment Status

Completed

Study Start Date

December 4, 2018 (Actual)

Primary Completion Date

December 15, 2020 (Actual)

Study Completion Date

January 15, 2021 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

Amicus Therapeutics

4. Oversight

Studies a U.S. FDA-regulated Drug Product

Yes

Studies a U.S. FDA-regulated Device Product

Data Monitoring Committee

Yes

5. Study Description

Brief Summary

This is a phase 3 double-blind randomized study to study the efficacy and safety of intravenous ATB200 Co-administered with oral AT2221 in adult subjects with Late Onset Pompe Disease compared with Alglucosidase Alfa/placebo.

Detailed Description

This is a double-blind, randomized, multicenter, international study of ATB200/AT2221 in adult subjects with late-onset Pompe disease (LOPD) who have received enzyme replacement therapy with alglucosidase alfa (ie, ERT-experienced) or who have never received ERT (ie, ERT naïve) compared with alglucosidase alfa/placebo. The study will consist of a screening period up to 30 days, a 12-month treatment period, and a 30 day safety follow-up period. Subjects who complete this study will have the option to participate in an open label extension study to receive ATB200/AT2221 under a separate protocol. Enzyme replacement therapy-experienced subjects will continue to take alglucosidase alfa during the screening period; treatment with alglucosidase alfa will then be replaced by study drug (ATB200/AT2221 or alglucosidase alfa/placebo) on the same schedule without interruption (ie, every 2 weeks). Infusion visits will be scheduled every 2 weeks throughout the study; assessments (eg, clinical laboratory tests) for initial safety monitoring will be performed at these visits for the first 6 weeks of the study. Study visits that include efficacy, safety, and other assessments will be scheduled approximately every 3 months and may occur over 2 days, provided all study assessments and procedures (with the exception of pharmacokinetic [PK] sample collection) are performed before administration of study drug. Efficacy assessments (ie, functional assessments) include evaluation of ambulatory function (6MWT), motor function tests (Gait, Stair, Gowers' maneuver, and Chair [GSGC] test and Timed Up and Go [TUG] test), muscle strength (manual muscle testing and quantitative muscle testing), and pulmonary function tests (forced vital capacity [FVC], slow vital capacity [SVC], maximal inspiratory pressure [MIP], maximal expiratory pressure [MEP], and sniff nasal inspiratory pressure [SNIP]). Patient reported outcomes (Rasch-built Pompe-specific Activity [R PAct] Scale, EuroQol 5 Dimensions 5 Levels Instrument [EQ-5D-5L], Patient-Reported Outcomes Measurement Information System [PROMIS®] instruments for physical function, fatigue, dyspnea, and upper extremity, and Subject's Global Impression of Change). The Physician's Global Impression of Change will also be performed. Pharmacodynamic assessments include measurement of biomarkers of muscle injury (creatine kinase [CK]) and disease substrate (urinary hexose tetrasaccharide [Hex4]). Blood samples will be collected for determination of total GAA protein levels and AT2221 concentrations in plasma for a population PK analysis. Safety assessments include monitoring of adverse events (AEs), including infusion associated reactions (IARs), clinical laboratory tests (chemistry, hematology, and urinalysis), vital signs, physical examinations including weight, electrocardiograms (ECGs), and immunogenicity. Concomitant medications and nondrug therapies will also be recorded.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study

Pompe Disease (Late-onset)

Keywords

Pompe, rhGAA

7. Study Design

Primary Purpose

Treatment

Study Phase

Phase 3

Interventional Study Model

Parallel Assignment

Masking

ParticipantInvestigator

Allocation

Randomized

Enrollment

125 (Actual)

8. Arms, Groups, and Interventions

Arm Title

Cipaglucosidase Alfa/Miglustat

Arm Type

Experimental

Arm Description

Participants received cipaglucosidase alfa co-administered with miglustat every 2 weeks (Q2W).

Arm Title

Alglucosidase Alfa/Placebo

Arm Type

Active Comparator

Arm Description

Participants received alglucosidase alfa co-administered with placebo Q2W.

Intervention Type

Biological

Intervention Name(s)

Cipaglucosidase Alfa

Other Intervention Name(s)

ATB200

Intervention Description

Participants received an intravenous (IV) infusion dose over a 4-hour duration every 2 weeks (Q2W).

Intervention Type

Drug

Intervention Name(s)

Miglustat

Other Intervention Name(s)

AT2221

Intervention Description

Participants received weight-based doses 1 hour prior to cipaglucosidase alfa infusion Q2W.

Intervention Type

Biological

Intervention Name(s)

Alglucosidase Alfa

Other Intervention Name(s)

Myozyme

Intervention Description

Participants received an IV infusion dose over a 4-hour duration Q2W.

Intervention Type

Drug

Intervention Name(s)

Placebo

Intervention Description

Miglustat matching placebo was administered orally 1 hour prior to alglucosidase alfa infusion Q2W.

Primary Outcome Measure Information:

Title

Change From Baseline to Week 52 in 6 Minute Walk Distance (6MWD)

Description

Time Frame

Baseline, Week 52

Secondary Outcome Measure Information:

Title

Change From Baseline to Week 52 in Sitting Forced Vital Capacity (FVC; % Predicted)

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in the Manual Muscle Test (MMT) Score for the Lower Extremities

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 26 in 6MWD

Description

The 6MWD, measured in meters, is the distance walked on the 6MWT.

Time Frame

Baseline, Week 26

Title

Change From Baseline to Week 52 in the Total Score for the Patient- Reported Outcomes Measurement Information System (PROMIS®) - Physical Function

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in the Total Score for the PROMIS® - Fatigue

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in the Total Score for the Gait, Stairs, Gowers' Maneuver, and Chair (GSGC)

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Rasch-Built Pompe-Specific Activity (R-PAct) Total Score

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in European Quality of Life-5 Dimensions 5 Response Levels (EQ-5D-5L) Based on the EuroQol Visual Analogue Scale (EQ VAS) Quantitative Score

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Sitting Slow Vital Capacity (SVC) % Predicted

Description

SVC is a standard pulmonary function test used to quantify respiratory muscle weakness.

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Maximal Inspiratory Pressure (MIP) % Predicted

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Maximal Expiratory Pressure (MEP) % Predicted

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Sniff Nasal Inspiratory Pressure (SNIP) % Predicted

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in % Predicted 6MWD

Description

The % predicted 6MWD = (actual 6MWD / predicted 6MWD) * 100. The predicted values were calculated using Enright And Sherrill 1998 Reference Equations.

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in the Quantitative Muscle Test (QMT) Values

Description

QMT was measured using the hand-held dynamometer. Larger values (in kg) indicated greater muscle strength.

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Other MMT Scores

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Maximum Vital Capacity (Maximum VC) % Predicted

Description

Maximum VC is the greater of the two VC values (FVC or SVC).

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in PROMIS-Dyspnea and Upper Extremities Total Scores

Description

Time Frame

Baseline, Week 52

Title

Change From Baseline in the Time to Complete Individual GSGC Component Tests and Timed Up and Go (TUG) Test at Week 52

Description

Time Frame

Baseline, Week 52

Title

Physician's Global Impression of Change (PGIC) Overall Status at Week 52

Description

Time Frame

Week 52

Title

Subject's Global Impression of Change (SGIC) at Week 52

Description

Time Frame

Week 52

Title

Number of Participants Improving on Both 6MWD and % Predicted FVC at Week 52

Description

Time Frame

Week 52

Title

Number of Participants With Treatment-Emergent Anti-Drug Antibodies (ADAs)

Description

Treatment-emergent ADAs were defined as participants who had seroconverted or boosted their preexisting ADA during the study period.

Time Frame

Baseline up to Week 52

Title

Change From Baseline to Week 52 in Urinary Hexose Tetrasaccharide (Hex4) Level

Description

Levels of urinary Hex4, a biomarker of disease substrate, were measured. The assay specifically targets Hex4, the glucose tetrasaccharide (Glc4), which is a biomarker of glycogen storage.

Time Frame

Baseline, Week 52

Title

Change From Baseline to Week 52 in Serum Creatine Kinase (CK) Level

Description

Change from baseline to Week 52 in serum CK level. CK levels were measured as part of the serum chemistry panel.

Time Frame

Baseline, Week 52

Title

Description

Time Frame

Days 1 and 364 (Week 52)

Title

Description

Time Frame

Days 1 and 364 (Week 52)

Title

Population PK: Cmax of Cipaglucosidase Alfa and Alglucosidase Alfa in ERT-Naïve Participants

Description

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis in ERT-naïve participants at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Time Frame

Days 1 and 364 (Week 52)

Title

Population PK: AUC of Cipaglucosidase Alfa and Alglucosidase Alfa in ERT-Naïve Subjects

Description

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis in ERT-naïve participants at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Time Frame

Days 1 and 364 (Week 52)

Title

Noncompartmental Analysis: Cmax of Plasma Total GAA Protein by Signature Peptide T09 in ERT-Naïve Subjects

Description

Time Frame

Day 1

Title

Noncompartmental Analysis: AUC From Time 0 (Predose) to the Time of Last Quantifiable Concentration of Plasma Total GAA Protein by Signature Peptide T09 in ERT-Naïve Subjects

Description

A noncompartmental analysis was performed on ERT-naïve subjects, who underwent serial PK sampling during the study. On Day 1, serial blood samples were collected for ERT-naïve participants just prior to initiation of cipaglucosidase alfa/alglucosidase alfa infusion (time 0) and at 1, 2, 3, 3.5, 4, 4.5, 6, 8, 10, and 24 hours after the start of cipaglucosidase alfa/alglucosidase alfa infusion for plasma total GAA protein signature peptide T09 and plasma miglustat determinations.

Time Frame

Day 1

Title

Comparison of Cmax of Cipaglucosidase Alfa in ERT-Experienced and ERT-Naïve Populations

Description

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Time Frame

Days 1 and 364 (Week 52)

Title

Comparison of AUC of Cipaglucosidase Alfa in ERT- Experienced and ERT-Naïve Populations

Description

On Days 1 and 364 (Week 52), sparse blood samples were collected for PK analysis at 0, 1, 4, 6, 12, and 24 hours post-dose. Collection of the 12-hour sample was optional.

Time Frame

Days 1 and 364 (Week 52)

10. Eligibility

Sex

All

Minimum Age & Unit of Time

18 Years

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria: Subject must provide signed informed consent prior to any study-related procedures being performed. Male and female subjects are ≥ 18 years old and weigh ≥ 40 kg at screening. Female subjects of childbearing potential and male subjects must agree to use medically accepted methods of contraception during the study and for 90 days after the last dose of study drug. Subject must have a diagnosis of LOPD based on documentation of one of the following: deficiency of GAA enzyme GAA genotyping Subject is classified as one of the following with respect to ERT status: ERT-experienced, defined as currently receiving standard of care ERT (alglucosidase alfa) at the recommended dose and regimen (ie, 20 mg/kg dose every 2 weeks) for ≥ 24 months ERT-naïve, defined as never having received investigational or commercially available ERT Subject has a sitting FVC ≥ 30% of the predicted value for healthy adults (National Health and Nutrition Examination Survey III) at screening. Subject performs two 6MWTs at screening that are valid, as determined by the clinical evaluator, and that meet all of the following criteria: both screening values of 6MWD are ≥ 75 meters both screening values of 6MWD are ≤ 90% of the predicted value for healthy adults the lower value of 6MWD is within 20% of the higher value of 6MWD Exclusion Criteria Subject has received any investigational therapy or pharmacological treatment for Pompe disease, other than alglucosidase alfa, within 30 days or 5 half-lives of the therapy or treatment, whichever is longer, before Day 1 or is anticipated to do so during the study. Subject has received gene therapy for Pompe disease Subject is taking any of the following prohibited medications within 30 days before Day 1: miglitol (eg, Glyset) miglustat (eg, Zavesca) acarbose (eg, Precose or Glucobay) voglibose (eg, Volix, Vocarb, or Volibo) Note: None of these medications have a half-life that, when multiplied by 5, is longer than 30 days. Subject requires the use of invasive or noninvasive ventilation support for > 6 hours per day while awake. Subject has a hypersensitivity to any of the excipients in ATB200, alglucosidase alfa, or AT2221. Subject has a medical condition or any other extenuating circumstance that may, in the opinion of the investigator or medical monitor, pose an undue safety risk to the subject or may compromise his/her ability to comply with or adversely impact protocol requirements. This includes clinical depression (as diagnosed by a psychiatrist or other mental health professional) with uncontrolled or poorly controlled symptoms. Subject, if female, is pregnant or breastfeeding at screening. Subject, whether male or female, is planning to conceive a child during the study. Subject does not have documentation of diagnosis of Pompe disease and refuses to undergo genetic testing.

Facility Information:

Facility Name

Neuromuscular Research Center

City

Phoenix

State/Province

Arizona

ZIP/Postal Code

85028

Country

United States

Facility Name

University of Arkansas for Medical Sciences

City

Little Rock

State/Province

Arkansas

ZIP/Postal Code

72205

Country

United States

Facility Name

University of California, Irvine

City

Irvine

State/Province

California

ZIP/Postal Code

92868

Country

United States

Facility Name

UF Helath: University of Florida Clinical Research Center

City

Gainesville

State/Province

Florida

ZIP/Postal Code

32610

Country

United States

Facility Name

University of South Florida Research Center

City

Tampa

State/Province

Florida

ZIP/Postal Code

33612

Country

United States

Facility Name

Emory Clinic

City

Atlanta

State/Province

Georgia

ZIP/Postal Code

30322

Country

United States

Facility Name

Indiana University Health Neuroscience Center

City

Indianapolis

State/Province

Indiana

ZIP/Postal Code

46202

Country

United States

Facility Name

University of Kansas Medical Center

City

Kansas City

State/Province

Kansas

ZIP/Postal Code

66205

Country

United States

Facility Name

University of Minnesota Clinical Research Unit

City

Minneapolis

State/Province

Minnesota

ZIP/Postal Code

55455

Country

United States

Facility Name

Washington University School of Medicine

City

Saint Louis

State/Province

Missouri

ZIP/Postal Code

63110

Country

United States

Facility Name

Billings Clinic

City

Billings

State/Province

Montana

ZIP/Postal Code

59101

Country

United States

Facility Name

Hackensack University Medical Center

City

Hackensack

State/Province

New Jersey

ZIP/Postal Code

07601

Country

United States

Facility Name

The Feinstein Institute for Medical Research

City

Manhasset

State/Province

New York

ZIP/Postal Code

11030

Country

United States

Facility Name

NYU School of Medicine

City

New York

State/Province

New York

ZIP/Postal Code

10017

Country

United States

Facility Name

Duke University Medical Center

City

Durham

State/Province

North Carolina

ZIP/Postal Code

27710

Country

United States

Facility Name

University of Cincinnati Neurology

City

Cincinnati

State/Province

Ohio

ZIP/Postal Code

45219

Country

United States

Facility Name

Cincinnati Children's Hospital Medical Center

City

Cincinnati

State/Province

Ohio

ZIP/Postal Code

45229

Country

United States

Facility Name

The Ohio State University Wexner Medical Center

City

Columbus

State/Province

Ohio

ZIP/Postal Code

43210

Country

United States

Facility Name

Oregon Health & Science University

City

Portland

State/Province

Oregon

ZIP/Postal Code

97239

Country

United States

Facility Name

Penn State Health Milton S. Hershey Medical Center

City

Hershey

State/Province

Pennsylvania

ZIP/Postal Code

17033

Country

United States

Facility Name

University of Pennsylvania

City

Philadelphia

State/Province

Pennsylvania

ZIP/Postal Code

19104

Country

United States

Facility Name

University of Pittsburgh

City

Pittsburgh

State/Province

Pennsylvania

ZIP/Postal Code

15213

Country

United States

Facility Name

University of Texas Health Science Center San Antonio

City

San Antonio

State/Province

Texas

ZIP/Postal Code

78229

Country

United States

Facility Name

University of Utah, Center for Clinical and Translational Sciences

City

Salt Lake City

State/Province

Utah

ZIP/Postal Code

84108

Country

United States

Facility Name

Lysosomal and Rare Disorders Research

City

Fairfax

State/Province

Virginia

ZIP/Postal Code

22030

Country

United States

Facility Name

Hospital Universitario Austral

City

Buenos Aires

ZIP/Postal Code

B1629ODT

Country

Argentina

Facility Name

Royal Brisbane & Women's Hospital

City

Herston

State/Province

Queensland

ZIP/Postal Code

4029

Country

Australia

Facility Name

Royal Adelaide Hospital

City

Adelaide

State/Province

South Australia

ZIP/Postal Code

5000

Country

Australia

Facility Name

Monash Medical Centre

City

Melbourne

State/Province

Victoria

ZIP/Postal Code

3168

Country

Australia

Facility Name

Westmead Hospital

City

Westmead

ZIP/Postal Code

2145

Country

Australia

Facility Name

Medizinische Universität Innsbruck

City

Innsbruck

Country

Austria

Facility Name

UZ Leuven

City

Leuven

ZIP/Postal Code

3000

Country

Belgium

Facility Name

University Clinical Centre of the Republic of Srpska

City

Banja Luka

ZIP/Postal Code

78000

Country

Bosnia and Herzegovina

Facility Name

UMHAT Alexandrovska

City

Sofia

Country

Bulgaria

Facility Name

Heritage Medical Research Clinic, University of Calgary

City

Calgary

State/Province

Alberta

ZIP/Postal Code

T2N 4Z6

Country

Canada

Facility Name

McMaster University Medical Centre

City

Hamilton

State/Province

Ontario

ZIP/Postal Code

L8N 3Z5

Country

Canada

Facility Name

Aarhus Universitets Hospital

City

Aarhus N

ZIP/Postal Code

8200

Country

Denmark

Facility Name

Rigshospitalet Copenhagen Neuromuscular Center

City

Copenhagen

ZIP/Postal Code

2100

Country

Denmark

Facility Name

Hôpital Neurologique Pierre Wertheimer

City

Bron

ZIP/Postal Code

69677

Country

France

Facility Name

Hôpital Raymond Poincaré

City

Garches

ZIP/Postal Code

92380

Country

France

Facility Name

Hôpital Salengro

City

Lille

ZIP/Postal Code

59037

Country

France

Facility Name

Hôpital de la Timone

City

Marseille

ZIP/Postal Code

13385

Country

France

Facility Name

Hôpital Pasteur

City

Nice

ZIP/Postal Code

06001

Country

France

Facility Name

Friedrich-Baur Institut

City

Munich

State/Province

Bavaria

ZIP/Postal Code

80336

Country

Germany

Facility Name

Universitätsklinikum Bonn

City

Bonn

State/Province

NRW

ZIP/Postal Code

53105

Country

Germany

Facility Name

Universitätsklinikum Münster

City

Münster

State/Province

NRW

ZIP/Postal Code

48149

Country

Germany

Facility Name

Universitätsklinikum Halle (Saale)

City

Halle (Saale)

State/Province

Sachsen-Anhalt

ZIP/Postal Code

06120

Country

Germany

Facility Name

Eginition Hospital

City

Athens

State/Province

Attica

ZIP/Postal Code

11528

Country

Greece

Facility Name

Semmelweis University, Institute of Genomic Medicine and Rare Disease

City

Budapest

ZIP/Postal Code

1083

Country

Hungary

Facility Name

University of Pécs

City

Pécs

ZIP/Postal Code

7623

Country

Hungary

Facility Name

University of Szeged

City

Szeged

ZIP/Postal Code

6725

Country

Hungary

Facility Name

UOC di Neurologia e Malattie Neuromuscolari

City

Messina

State/Province

NAP

ZIP/Postal Code

98125

Country

Italy

Facility Name

UOC Genetica Medica

City

Napoli

State/Province

NAP

ZIP/Postal Code

80131

Country

Italy

Facility Name

Hokkaido University Hospital

City

Sapporo

State/Province

Hokkaido

ZIP/Postal Code

060 8648

Country

Japan

Facility Name

Fukuoka University Hospital

City

Fukuoka

ZIP/Postal Code

814-0180

Country

Japan

Facility Name

Kagoshima University Hospital

City

Kagoshima

Country

Japan

Facility Name

Izumi City General Hospital

City

Osaka

Country

Japan

Facility Name

The Jikei University Hospital

City

Tokyo

ZIP/Postal Code

105-8471

Country

Japan

Facility Name

National Center of Neurology and Psychiatry

City

Tokyo

Country

Japan

Facility Name

Pusan National University

City

Yangsan

State/Province

Gyeongsangnam-do

ZIP/Postal Code

50612

Country

Korea, Republic of

Facility Name

Seoul National University Hospital

City

Seoul

ZIP/Postal Code

03080

Country

Korea, Republic of

Facility Name

Erasmus MC

City

Rotterdam

ZIP/Postal Code

3015GD

Country

Netherlands

Facility Name

University of Auckland

City

Auckland

Country

New Zealand

Facility Name

Szpital Uniwersytecki w Krakowie

City

Małogoskie

ZIP/Postal Code

31-066

Country

Poland

Facility Name

Centrum Medyczne

City

Rzeszów

ZIP/Postal Code

35-326

Country

Poland

Facility Name

University Medical Centre Ljubljana

City

Ljubljana

ZIP/Postal Code

1000

Country

Slovenia

Facility Name

Hospital de la Santa Creu I Sant Pau

City

Barcelona

ZIP/Postal Code

08026

Country

Spain

Facility Name

Sahlgrenska University Hospital

City

Gothenburg

ZIP/Postal Code

41345

Country

Sweden

Facility Name

National Taiwan University Hospital

City

Taipei

ZIP/Postal Code

100

Country

Taiwan

Facility Name

Queen Elizabeth Hospital Birmingham

City

Birmingham

Country

United Kingdom

Facility Name

Cambridge University Hospitals

City

Cambridge

Country

United Kingdom

Facility Name

Royal Free Hospital NHS

City

London

ZIP/Postal Code

NW3 2QG

Country

United Kingdom

Facility Name

Salford Royal NHS Foundation Trust

City

Salford

ZIP/Postal Code

M6 8HD

Country

United Kingdom

12. IPD Sharing Statement

Plan to Share IPD

Citations:

PubMed Identifier

34800400

Citation

Schoser B, Roberts M, Byrne BJ, Sitaraman S, Jiang H, Laforet P, Toscano A, Castelli J, Diaz-Manera J, Goldman M, van der Ploeg AT, Bratkovic D, Kuchipudi S, Mozaffar T, Kishnani PS; PROPEL Study Group. Safety and efficacy of cipaglucosidase alfa plus miglustat versus alglucosidase alfa plus placebo in late-onset Pompe disease (PROPEL): an international, randomised, double-blind, parallel-group, phase 3 trial. Lancet Neurol. 2021 Dec;20(12):1027-1037. doi: 10.1016/S1474-4422(21)00331-8. Erratum In: Lancet Neurol. 2023 Oct;22(10):e11.

Results Reference

derived

Learn more about this trial

A Study Comparing ATB200/AT2221 With Alglucosidase Alfa/Placebo in Adult Subjects With Late-onset Pompe Disease

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