Switching Enzyme Replacement Therapy for Late‐Onset Pompe Disease From Alglucosidase Alfa to Cipaglucosidase Alfa Plus Miglustat: Post Hoc Effect Size Analysis of PROPEL

ABSTRACT Introduction/Aims The randomized, double‐blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus placebo (alg+pbo) in enzyme replacement therapy (ERT)‐experienced adults with late‐onset Pompe disease (LOPD). To fu...

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Published in	Muscle & nerve Vol. 72; no. 2; pp. 230 - 239
Main Authors	Kushlaf, Hani, Díaz‐Manera, Jordi, Bratkovic, Drago, Byrne, Barry J., Claeys, Kristl G., Clemens, Paula R., Dimachkie, Mazen M., Kishnani, Priya S., Laforêt, Pascal, Roberts, Mark, Schoser, Benedikt, Toscano, Antonio, Castelli, Jeff, Holdbrook, Fred, Sitaraman Das, Sheela, Goldman, Mitchell, Mozaffar, Tahseen
Format	Journal Article
Language	English
Published	Hoboken, USA John Wiley & Sons, Inc 01.08.2025 Wiley Subscription Services, Inc
Subjects	1-Deoxynojirimycin - administration & dosage 1-Deoxynojirimycin - analogs & derivatives 1-Deoxynojirimycin - therapeutic use Adult Aged alpha-Glucosidases - therapeutic use Biomarkers cipaglucosidase alfa Creatine Creatine kinase Double-Blind Method Dyspnea Enzyme Replacement Therapy - methods Enzymes Fatigue tests Female Glycogen Storage Disease Type II - drug therapy Health services Human motion Humans Kinases late‐onset Pompe disease Lungs Male Middle Aged miglustat Muscle strength Muscle Strength - drug effects Muscular fatigue Patients Quality of Life Respiration Respiratory function Stability Statistical analysis Treatment Outcome cipaglucosidase alfa late‐onset Pompe disease miglustat
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ISSN	0148-639X 1097-4598 1097-4598
DOI	10.1002/mus.28420

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Abstract	ABSTRACT Introduction/Aims The randomized, double‐blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus placebo (alg+pbo) in enzyme replacement therapy (ERT)‐experienced adults with late‐onset Pompe disease (LOPD). To further assess treatment response and the effect of switching treatment from alg to cipa+mig, we conducted a within‐group effect size analysis in ERT‐experienced patients. Methods In this post hoc analysis, standardized within‐group effect sizes (Cohen's d for correlated measurements from baseline to week 52) were calculated by dividing the mean change from baseline by the corresponding standard deviation for motor function, lung function, and muscle strength outcomes; patient‐reported outcomes/quality of life; and biomarker levels (creatine kinase and hexose tetrasaccharide). Results In PROPEL, 77% of patients received ERT with alg before study entry (median ERT duration 7.4 years). ERT‐experienced patients remaining on alg+pbo (n = 30) generally showed within‐group worsening (d ≤ −0.2) or stability (−0.2 < d < 0.2) across most outcomes, while those switched to cipa+mig (n = 65) mostly showed improvement (d ≥ 0.2) or stability. Patients remaining on alg+pbo demonstrated statistically significant worsening for several lung function outcomes, biomarker levels, and significant improvement for Patient‐Reported Outcomes Measurement Information System (PROMIS)‐Dyspnea. Patients switched to cipa+mig did not demonstrate significant worsening for any outcomes and showed significant improvements for 6‐min walk distance (absolute and % predicted); upper, lower, and overall manual muscle testing; PROMIS‐Fatigue; Physician (overall score) and Subject Global Impression of Change (5/8 subdomains); and biomarker levels. Discussion ERT‐experienced patients with LOPD who switched from alg to cipa+mig treatment achieved improvements or stability in most outcomes. Trial Registration: ClinicalTrials.gov identifier: NCT03729362 A total of 95 ERT‐experienced adults with LOPD were randomized to switch to cipaglucosidase alfa + miglustat or remain on alglucosidase alfa treatment. After 52 weeks, patients remaining on alglucosidase alfa showed worsening or stability for most outcomes, whereas patients who switched to cipaglucosidase alfa + miglustat generally showed stability or improvement.
AbstractList	Introduction/Aims The randomized, double‐blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus placebo (alg+pbo) in enzyme replacement therapy (ERT)‐experienced adults with late‐onset Pompe disease (LOPD). To further assess treatment response and the effect of switching treatment from alg to cipa+mig, we conducted a within‐group effect size analysis in ERT‐experienced patients. Methods In this post hoc analysis, standardized within‐group effect sizes (Cohen's d for correlated measurements from baseline to week 52) were calculated by dividing the mean change from baseline by the corresponding standard deviation for motor function, lung function, and muscle strength outcomes; patient‐reported outcomes/quality of life; and biomarker levels (creatine kinase and hexose tetrasaccharide). Results In PROPEL, 77% of patients received ERT with alg before study entry (median ERT duration 7.4 years). ERT‐experienced patients remaining on alg+pbo (n = 30) generally showed within‐group worsening (d ≤ −0.2) or stability (−0.2 < d < 0.2) across most outcomes, while those switched to cipa+mig (n = 65) mostly showed improvement (d ≥ 0.2) or stability. Patients remaining on alg+pbo demonstrated statistically significant worsening for several lung function outcomes, biomarker levels, and significant improvement for Patient‐Reported Outcomes Measurement Information System (PROMIS)‐Dyspnea. Patients switched to cipa+mig did not demonstrate significant worsening for any outcomes and showed significant improvements for 6‐min walk distance (absolute and % predicted); upper, lower, and overall manual muscle testing; PROMIS‐Fatigue; Physician (overall score) and Subject Global Impression of Change (5/8 subdomains); and biomarker levels. Discussion ERT‐experienced patients with LOPD who switched from alg to cipa+mig treatment achieved improvements or stability in most outcomes. Trial Registration: ClinicalTrials.gov identifier: NCT03729362 ABSTRACT Introduction/Aims The randomized, double‐blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus placebo (alg+pbo) in enzyme replacement therapy (ERT)‐experienced adults with late‐onset Pompe disease (LOPD). To further assess treatment response and the effect of switching treatment from alg to cipa+mig, we conducted a within‐group effect size analysis in ERT‐experienced patients. Methods In this post hoc analysis, standardized within‐group effect sizes (Cohen's d for correlated measurements from baseline to week 52) were calculated by dividing the mean change from baseline by the corresponding standard deviation for motor function, lung function, and muscle strength outcomes; patient‐reported outcomes/quality of life; and biomarker levels (creatine kinase and hexose tetrasaccharide). Results In PROPEL, 77% of patients received ERT with alg before study entry (median ERT duration 7.4 years). ERT‐experienced patients remaining on alg+pbo (n = 30) generally showed within‐group worsening (d ≤ −0.2) or stability (−0.2 < d < 0.2) across most outcomes, while those switched to cipa+mig (n = 65) mostly showed improvement (d ≥ 0.2) or stability. Patients remaining on alg+pbo demonstrated statistically significant worsening for several lung function outcomes, biomarker levels, and significant improvement for Patient‐Reported Outcomes Measurement Information System (PROMIS)‐Dyspnea. Patients switched to cipa+mig did not demonstrate significant worsening for any outcomes and showed significant improvements for 6‐min walk distance (absolute and % predicted); upper, lower, and overall manual muscle testing; PROMIS‐Fatigue; Physician (overall score) and Subject Global Impression of Change (5/8 subdomains); and biomarker levels. Discussion ERT‐experienced patients with LOPD who switched from alg to cipa+mig treatment achieved improvements or stability in most outcomes. Trial Registration: ClinicalTrials.gov identifier: NCT03729362 A total of 95 ERT‐experienced adults with LOPD were randomized to switch to cipaglucosidase alfa + miglustat or remain on alglucosidase alfa treatment. After 52 weeks, patients remaining on alglucosidase alfa showed worsening or stability for most outcomes, whereas patients who switched to cipaglucosidase alfa + miglustat generally showed stability or improvement. The randomized, double-blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus placebo (alg+pbo) in enzyme replacement therapy (ERT)-experienced adults with late-onset Pompe disease (LOPD). To further assess treatment response and the effect of switching treatment from alg to cipa+mig, we conducted a within-group effect size analysis in ERT-experienced patients.INTRODUCTION/AIMSThe randomized, double-blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus placebo (alg+pbo) in enzyme replacement therapy (ERT)-experienced adults with late-onset Pompe disease (LOPD). To further assess treatment response and the effect of switching treatment from alg to cipa+mig, we conducted a within-group effect size analysis in ERT-experienced patients.In this post hoc analysis, standardized within-group effect sizes (Cohen's d for correlated measurements from baseline to week 52) were calculated by dividing the mean change from baseline by the corresponding standard deviation for motor function, lung function, and muscle strength outcomes; patient-reported outcomes/quality of life; and biomarker levels (creatine kinase and hexose tetrasaccharide).METHODSIn this post hoc analysis, standardized within-group effect sizes (Cohen's d for correlated measurements from baseline to week 52) were calculated by dividing the mean change from baseline by the corresponding standard deviation for motor function, lung function, and muscle strength outcomes; patient-reported outcomes/quality of life; and biomarker levels (creatine kinase and hexose tetrasaccharide).In PROPEL, 77% of patients received ERT with alg before study entry (median ERT duration 7.4 years). ERT-experienced patients remaining on alg+pbo (n = 30) generally showed within-group worsening (d ≤ -0.2) or stability (-0.2 < d < 0.2) across most outcomes, while those switched to cipa+mig (n = 65) mostly showed improvement (d ≥ 0.2) or stability. Patients remaining on alg+pbo demonstrated statistically significant worsening for several lung function outcomes, biomarker levels, and significant improvement for Patient-Reported Outcomes Measurement Information System (PROMIS)-Dyspnea. Patients switched to cipa+mig did not demonstrate significant worsening for any outcomes and showed significant improvements for 6-min walk distance (absolute and % predicted); upper, lower, and overall manual muscle testing; PROMIS-Fatigue; Physician (overall score) and Subject Global Impression of Change (5/8 subdomains); and biomarker levels.RESULTSIn PROPEL, 77% of patients received ERT with alg before study entry (median ERT duration 7.4 years). ERT-experienced patients remaining on alg+pbo (n = 30) generally showed within-group worsening (d ≤ -0.2) or stability (-0.2 < d < 0.2) across most outcomes, while those switched to cipa+mig (n = 65) mostly showed improvement (d ≥ 0.2) or stability. Patients remaining on alg+pbo demonstrated statistically significant worsening for several lung function outcomes, biomarker levels, and significant improvement for Patient-Reported Outcomes Measurement Information System (PROMIS)-Dyspnea. Patients switched to cipa+mig did not demonstrate significant worsening for any outcomes and showed significant improvements for 6-min walk distance (absolute and % predicted); upper, lower, and overall manual muscle testing; PROMIS-Fatigue; Physician (overall score) and Subject Global Impression of Change (5/8 subdomains); and biomarker levels.ERT-experienced patients with LOPD who switched from alg to cipa+mig treatment achieved improvements or stability in most outcomes.DISCUSSIONERT-experienced patients with LOPD who switched from alg to cipa+mig treatment achieved improvements or stability in most outcomes.ClinicalTrials.gov identifier: NCT03729362.TRIAL REGISTRATIONClinicalTrials.gov identifier: NCT03729362. The randomized, double-blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus placebo (alg+pbo) in enzyme replacement therapy (ERT)-experienced adults with late-onset Pompe disease (LOPD). To further assess treatment response and the effect of switching treatment from alg to cipa+mig, we conducted a within-group effect size analysis in ERT-experienced patients. In this post hoc analysis, standardized within-group effect sizes (Cohen's d for correlated measurements from baseline to week 52) were calculated by dividing the mean change from baseline by the corresponding standard deviation for motor function, lung function, and muscle strength outcomes; patient-reported outcomes/quality of life; and biomarker levels (creatine kinase and hexose tetrasaccharide). In PROPEL, 77% of patients received ERT with alg before study entry (median ERT duration 7.4 years). ERT-experienced patients remaining on alg+pbo (n = 30) generally showed within-group worsening (d ≤ -0.2) or stability (-0.2 < d < 0.2) across most outcomes, while those switched to cipa+mig (n = 65) mostly showed improvement (d ≥ 0.2) or stability. Patients remaining on alg+pbo demonstrated statistically significant worsening for several lung function outcomes, biomarker levels, and significant improvement for Patient-Reported Outcomes Measurement Information System (PROMIS)-Dyspnea. Patients switched to cipa+mig did not demonstrate significant worsening for any outcomes and showed significant improvements for 6-min walk distance (absolute and % predicted); upper, lower, and overall manual muscle testing; PROMIS-Fatigue; Physician (overall score) and Subject Global Impression of Change (5/8 subdomains); and biomarker levels. ERT-experienced patients with LOPD who switched from alg to cipa+mig treatment achieved improvements or stability in most outcomes. ClinicalTrials.gov identifier: NCT03729362.
Author	Toscano, Antonio Díaz‐Manera, Jordi Claeys, Kristl G. Goldman, Mitchell Sitaraman Das, Sheela Laforêt, Pascal Castelli, Jeff Schoser, Benedikt Holdbrook, Fred Kushlaf, Hani Kishnani, Priya S. Byrne, Barry J. Dimachkie, Mazen M. Mozaffar, Tahseen Bratkovic, Drago Roberts, Mark Clemens, Paula R.
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publication-title: Lancet Neurology – volume: 31 issue: 9 year: 2024 article-title: Start, Switch and Stop (Triple‐S) Criteria for Enzyme Replacement Therapy of Late‐Onset Pompe Disease: European Pompe Consortium Recommendation Update 2024 publication-title: European Journal of Neurology – volume: 268 start-page: 2482 issue: 7 year: 2021 end-page: 2492 article-title: STIG Study: Real‐World Data of Long‐Term Outcomes of Adults With Pompe Disease Under Enzyme Replacement Therapy With Alglucosidase Alfa publication-title: Journal of Neurology – volume: 15 year: 2024 article-title: Cipaglucosidase Alfa Plus Miglustat: Linking Mechanism of Action to Clinical Outcomes in Late‐Onset Pompe Disease publication-title: Frontiers in Neurology – volume: 296 year: 2021 article-title: Endolysosomal N‐Glycan Processing Is Critical to Attain the Most Active Form of the Enzyme Acid Alpha‐Glucosidase publication-title: Journal of Biological Chemistry – volume: 4 start-page: 279 issue: 3 year: 2012 end-page: 282 article-title: Using Effect Size‐Or Why the P Value Is Not Enough publication-title: Journal of Graduate Medical Education – volume: 114 start-page: S49 issue: 2 year: 2015 article-title: Novel Recombinant Human Acid α‐Glucosidase With Optimal Glycosylation Is Significantly Better Than Standard of Care Enzyme Replacement for Glycogen Clearance in Skeletal Muscles of GAA Knock‐Out Mice publication-title: Molecular Genetics and Metabolism – volume: 27 year: 2021 article-title: Carrier Frequency and Predicted Genetic Prevalence of Pompe Disease Based on a General Population Database publication-title: Molecular Genetics and Metabolism Reports – volume: 4 issue: 5 year: 2019 article-title: Improved Efficacy of a Next‐Generation ERT in Murine Pompe Disease publication-title: JCI Insight – volume: 26 start-page: 45 issue: 1 year: 2007 end-page: 48 article-title: Role of Autophagy in the Pathogenesis of Pompe Disease publication-title: Acta Myologica – volume: 7 start-page: 284 issue: 13 year: 2019 article-title: Multisystem Late Onset Pompe Disease (LOPD): An Update on Clinical Aspects publication-title: Annals of Translational Medicine – volume: 45 start-page: 319 issue: 3 year: 2012 end-page: 333 article-title: Consensus Treatment Recommendations for Late‐Onset Pompe Disease publication-title: Muscle & Nerve – year: 2002 – year: 1988 – volume: 31 issue: 5 year: 2024 article-title: Establishing How Much Improvement in Lung Function and Distance Walked Is Clinically Important for Adult Patients With Pompe Disease publication-title: European Journal of Neurology – volume: 19 start-page: 154 issue: 1 year: 2024 article-title: Minimal Clinically Important Differences in Six‐Minute Walking Distance in Late‐Onset Pompe Disease publication-title: Orphanet Journal of Rare Diseases – volume: 362 start-page: 1396 issue: 15 year: 2010 end-page: 1406 article-title: A Randomized Study of Alglucosidase Alfa in Late‐Onset Pompe's Disease publication-title: New England Journal of Medicine – volume: 20 start-page: 1027 issue: 12 year: 2021 end-page: 1037 article-title: 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 publication-title: Lancet Neurology – volume: 8 start-page: 132 issue: 1 year: 2024 article-title: Switching Treatment to Cipaglucosidase Alfa Plus Miglustat Positively Affects Patient‐Reported Outcome Measures in Patients With Late‐Onset Pompe Disease publication-title: J Patient Rep Outcomes – ident: e_1_2_11_9_1 doi: 10.21037/atm.2019.04.15 – ident: e_1_2_11_22_1 doi: 10.1186/1755-8417-1-6 – ident: e_1_2_11_10_1 doi: 10.1016/j.jbc.2021.100769 – ident: e_1_2_11_3_1 doi: 10.1097/01.gim.0000218152.87434.f3 – ident: e_1_2_11_20_1 doi: 10.1016/j.ymgme.2014.12.096 – volume: 26 start-page: 45 issue: 1 year: 2007 ident: e_1_2_11_21_1 article-title: Role of Autophagy in the Pathogenesis of Pompe Disease publication-title: Acta Myologica – ident: e_1_2_11_6_1 doi: 10.1002/mus.22329 – ident: e_1_2_11_25_1 doi: 10.1111/ene.16223 – ident: e_1_2_11_24_1 doi: 10.1186/s13023-024-03156-3 – ident: e_1_2_11_7_1 doi: 10.1056/NEJMoa0909859 – volume-title: It's the Effect Size, Stupid. 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Snippet	ABSTRACT Introduction/Aims The randomized, double‐blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus... The randomized, double-blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus alglucosidase alfa plus... Introduction/Aims The randomized, double‐blind PROPEL study (NCT03729362) suggested benefits for cipaglucosidase alfa plus miglustat (cipa+mig) versus...
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SubjectTerms	1-Deoxynojirimycin - administration & dosage 1-Deoxynojirimycin - analogs & derivatives 1-Deoxynojirimycin - therapeutic use Adult Aged alpha-Glucosidases - therapeutic use Biomarkers cipaglucosidase alfa Creatine Creatine kinase Double-Blind Method Dyspnea Enzyme Replacement Therapy - methods Enzymes Fatigue tests Female Glycogen Storage Disease Type II - drug therapy Health services Human motion Humans Kinases late‐onset Pompe disease Lungs Male Middle Aged miglustat Muscle strength Muscle Strength - drug effects Muscular fatigue Patients Quality of Life Respiration Respiratory function Stability Statistical analysis Treatment Outcome
Title	Switching Enzyme Replacement Therapy for Late‐Onset Pompe Disease From Alglucosidase Alfa to Cipaglucosidase Alfa Plus Miglustat: Post Hoc Effect Size Analysis of PROPEL
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