Increased dystrophin production with golodirsen in patients with Duchenne muscular dystrophy.

Administration, Intravenous; Adolescent; Child; Dose-Response Relationship, Drug; Double-Blind Method; Dystrophin/biosynthesis/genetics; Fluorescent Antibody Technique; Humans; Male; Muscle, Skeletal/metabolism; Muscular Dystrophy, Duchenne/blood/drug therapy/genetics; Oligonucleotides/therapeutic use; Sequence Deletion/drug effects

Abstract :

[en] OBJECTIVE: To report safety, pharmacokinetics, exon 53 skipping, and dystrophin expression in golodirsen-treated patients with Duchenne muscular dystrophy (DMD) amenable to exon 53 skipping. METHODS: Part 1 was a randomized, double-blind, placebo-controlled, 12-week dose titration of once-weekly golodirsen; part 2 is an ongoing, open-label evaluation. Safety and pharmacokinetics were primary and secondary objectives of part 1. Primary biological outcome measures of part 2 were blinded exon skipping and dystrophin protein production on muscle biopsies (baseline, week 48) evaluated, respectively, using reverse transcription PCR and Western blot and immunohistochemistry. RESULTS: Twelve patients were randomized to receive golodirsen (n = 8) or placebo (n = 4) in part 1. All from part 1 plus 13 additional patients received 30 mg/kg golodirsen in part 2. Safety findings were consistent with those previously observed in pediatric patients with DMD. Most of the study drug was excreted within 4 hours following administration. A significant increase in exon 53 skipping was associated with ∼16-fold increase over baseline in dystrophin protein expression at week 48, with a mean percent normal dystrophin protein standard of 1.019% (range, 0.09%-4.30%). Sarcolemmal localization of dystrophin was demonstrated by significantly increased dystrophin-positive fibers (week 48, p < 0.001) and a positive correlation (Spearman r = 0.663; p < 0.001) with dystrophin protein change from baseline, measured by Western blot and immunohistochemistry. CONCLUSION: Golodirsen was well-tolerated; muscle biopsies from golodirsen-treated patients showed increased exon 53 skipping, dystrophin production, and correct dystrophin sarcolemmal localization. CLINICALTRIALSGOV IDENTIFIER: NCT02310906. CLASSIFICATION OF EVIDENCE: This study provides Class I evidence that golodirsen is safe and Class IV evidence that it induces exon skipping and novel dystrophin as confirmed by 3 different assays.

Disciplines :

Neurology
Pediatrics

Author, co-author :

Frank, Diane E.

Schnell, Frederick J.

Akana, Cody

El-Husayni, Saleh H.

Desjardins, Cody A.

Morgan, Jennifer

Charleston, Jay S.

Sardone, Valentina

Domingos, Joana

Dickson, George

More authors (5 more)

Language :

English

Title :

Increased dystrophin production with golodirsen in patients with Duchenne muscular dystrophy.

Publication date :

26 May 2020

Journal title :

Neurology

ISSN :

0028-3878

eISSN :

1526-632X

Publisher :

Lippincott Williams & Wilkins, United States - Maryland

Volume :

Issue :

Pages :

e2270-e2282

Peer reviewed :

Peer Reviewed verified by ORBi

Commentary :

Available on ORBi :

since 01 February 2021

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Bibliography

Bushby K, Finkel R, Birnkrant DJ, et al. Diagnosis and management of Duchenne muscular dystrophy, part 1: diagnosis, and pharmacological and psychosocial management. Lancet Neurol 2010; 9: 77-93.
Emery AE,. Population frequencies of inherited neuromuscular diseases: a world survey. Neuromuscul Disord 1991; 1: 19-29.
Mendell JR, Shilling C, Leslie ND, et al. Evidence-based path to newborn screening for Duchenne muscular dystrophy. Ann Neurol 2012; 71: 304-313.
Mah JK, Korngut L, Dykeman J, Day L, Pringsheim T, Jette N,. A systematic review and meta-analysis on the epidemiology of Duchenne and Becker muscular dystrophy. Neuromuscul Disord 2014; 24: 482-491.
Kobayashi YM, Campbell KP,. Skeletal muscle dystrophin-glycoprotein complex and muscular dystrophy. In: Hill JA, Olson EN, eds. Muscle: Fundamental Biology and Mechanisms of Disease, vol. 2. New York: Academic Press; 2012: 935-942.
Emery AE,. The muscular dystrophies. Lancet 2002; 359: 687-695.
Monaco AP, Bertelson CJ, Liechti-Gallati S, Moser H, Kunkel LM,. An explanation for the phenotypic differences between patients bearing partial deletions of the DMD locus. Genomics 1988; 2: 90-95.
Allen DG, Whitehead NP, Froehner SC,. Absence of dystrophin disrupts skeletal muscle signaling: roles of Ca2+, reactive oxygen species, and nitric oxide in the development of muscular dystrophy. Physiol Rev 2016; 96: 253-305.
Rando TA,. The dystrophin-glycoprotein complex, cellular signaling, and the regulation of cell survival in the muscular dystrophies. Muscle Nerve 2001; 24: 1575-1594.
Mah JK,. Current and emerging treatment strategies for Duchenne muscular dystrophy. Neuropsychiatr Dis Treat 2016; 12: 1795-1807.
Falzarano MS, Scotton C, Passarelli C, Ferlini A,. Duchenne muscular dystrophy: from diagnosis to therapy. Molecules 2015; 20: 18168-18184.
Wilton SD, Fall AM, Harding PL, McClorey G, Coleman C, Fletcher S,. Antisense oligonucleotide-induced exon skipping across the human dystrophin gene transcript. Mol Ther 2007; 15: 1288-1296.
Wilton SD, Fletcher S,. RNA splicing manipulation: strategies to modify gene expression for a variety of therapeutic outcomes. Curr Gene Ther 2011; 11: 259-275.
Wilton SD, Lloyd F, Carville K, et al. Specific removal of the nonsense mutation from the mdx dystrophin mRNA using antisense oligonucleotides. Neuromuscul Disord 1999; 9: 330-338.
Popplewell LJ, Trollet C, Dickson G, Graham IR,. Design of phosphorodiamidate morpholino oligomers (PMOs) for the induction of exon skipping of the human DMD gene. Mol Ther 2009; 17: 554-561.
Exondys 51 [package insert]. Cambridge: Sarepta Therapeutics, Inc.; 2016.
Cirak S, Arechavala-Gomeza V, Guglieri M, et al. Exon skipping and dystrophin restoration in patients with Duchenne muscular dystrophy after systemic phosphorodiamidate morpholino oligomer treatment: an open-label, phase 2, dose-escalation study. Lancet 2011; 378: 595-605.
Mendell JR, Goemans N, Lowes LP, et al. Longitudinal effect of eteplirsen versus historical control on ambulation in Duchenne muscular dystrophy. Ann Neurol 2016; 79: 257-271.
Aartsma-Rus A, Fokkema I, Verschuuren J, et al. Theoretic applicability of antisense-mediated exon skipping for Duchenne muscular dystrophy mutations. Hum Mutat 2009; 30: 293-299.
Frank D, Dworzak J, Lawlor M, et al. Optimization and implementation of best practices for collection and preparation of muscle biopsies for analysis during clinical trials of neuromuscular disease therapeutics [poster]. International Annual Congress of the World Muscle Society; October 3-7, 2017; Saint Malo, France.
Charleston JS, Schnell FJ, Dworzak J, et al. Eteplirsen treatment for Duchenne muscular dystrophy: exon skipping and dystrophin production. Neurology 2018; 90: e2146-e2154.
Guidance for Industry. Duchenne muscular dystrophy and related dystrophinopathies: developing drugs for treatment. 2018. Available at: fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/UCM450229.pdf. Accessed February 5, 2019.
Mendell JR, Rodino-Klapac LR, Sahenk Z, et al. Eteplirsen for the treatment of Duchenne muscular dystrophy. Ann Neurol 2013; 74: 637-647.
Alter J, Lou F, Rabinowitz A, et al. Systemic delivery of morpholino oligonucleotide restores dystrophin expression bodywide and improves dystrophic pathology. Nat Med 2006; 12: 175-177.
Yokota T, Lu QL, Partridge T, et al. Efficacy of systemic morpholino exon-skipping in Duchenne dystrophy dogs. Ann Neurol 2009; 65: 667-676.
van Putten M, Hulsker M, Young C, et al. Low dystrophin levels increase survival and improve muscle pathology and function in dystrophin/utrophin double-knockout mice. FASEB J 2013; 27: 2484-2495.
Anthony K, Arechavala-Gomeza V, Ricotti V, et al. Biochemical characterization of patients with in-frame or out-of-frame DMD deletions pertinent to exon 44 or 45 skipping. JAMA Neurol 2014; 71: 32-40.
Bello L, Morgenroth LP, Gordish-Dressman H, Hoffman EP, McDonald CM, Cirak S,. DMD genotypes and loss of ambulation in the CINRG Duchenne natural history study. Neurology 2016; 87: 401-409.
Moon D, Hu S, Bange J, et al. Genotype-phenotype associations in a large cohort of Duchenne muscular dystrophy patients. Neuromuscul Disord 2017; 27 (suppl 2): S104-S105.
Waldrop MA, Gumienny F, El Husayni S, Frank DE, Weiss RB, Flanigan KM,. Low-level dystrophin expression attenuating the dystrophinopathy phenotype. Neuromuscul Disord 2018; 28: 116-121.
Brogna C, Coratti G, Pane M, et al; on behalf on the International DMD Group. Long-term natural history data in Duchenne muscular dystrophy ambulant patients with mutations amenable to skip exons 44, 45, 51 and 53. PLoS One 2019; 14: e0218683.
Khan N, Eliopoulos H, Han L, et al. Eteplirsen treatment attenuates respiratory decline in ambulatory and non-ambulatory patients with Duchenne muscular dystrophy. J Neuromuscul Dis 2019; 6: 213-225.
Godfrey C, Muses S, McClorey G, et al. How much dystrophin is enough: the physiological consequences of different levels of dystrophin in the mdx mouse. Hum Mol Genet 2015; 24: 4225-4237.
Bello L, Flanigan KM, Weiss RB, et al. Association study of exon variants in the NF-B and TGFβ pathways identifies CD40 as a modifier of Duchenne muscular dystrophy. Am J Hum Genet 2016; 99: 1163-1171.
Flanigan KM, Ceco E, Lamar KM, et al. LTBP4 genotype predicts age of ambulatory loss in Duchenne muscular dystrophy. Ann Neurol 2013; 73: 481-488.
European Medicines Agency. Guideline on the clinical investigation of medicinal products for the treatment of Duchenne and Becker muscular dystrophy. Available at: ema.europa.eu/docs/en_GB/document_library/Scientific_guideline/2015/12/WC500199239.pdf. Accessed November 5, 2018.