Eteplirsen treatment for Duchenne muscular dystrophy-Reference-Cited by-同舟云学术

Eteplirsen treatment for Duchenne muscular dystrophy

Published:2018-05-11 Issue:24 Volume:90 Page:e2146-e2154
ISSN:0028-3878
Container-title:Neurology
language:en
Short-container-title:Neurology

Author:

Charleston Jay S.,Schnell Frederick J.,Dworzak Johannes,Donoghue Cas,Lewis Sarah,Chen Lei,Young G. David,Milici Anthony J.,Voss Jon,DeAlwis Uditha,Wentworth Bruce,Rodino-Klapac Louise R.,Sahenk Zarife,Frank Diane,Mendell Jerry R.

Abstract

ObjectiveTo describe the quantification of novel dystrophin production in patients with Duchenne muscular dystrophy (DMD) after long-term treatment with eteplirsen.MethodsClinical study 202 was an observational, open-label extension of the randomized, controlled study 201 assessing the safety and efficacy of eteplirsen in patients with DMD with a confirmed mutation in the DMD gene amenable to correction by skipping of exon 51. Patients received once-weekly IV doses of eteplirsen 30 or 50 mg/kg. Upper extremity muscle biopsy samples were collected at combined study week 180, blinded, and assessed for dystrophin-related content by Western blot, Bioquant software measurement of dystrophin-associated immunofluorescence intensity, and percent dystrophin-positive fibers (PDPF). Results were contrasted with matched untreated biopsies from patients with DMD. Reverse transcription PCR followed by Sanger sequencing of newly formed slice junctions was used to confirm the mechanism of action of eteplirsen.ResultsReverse transcription PCR analysis and sequencing of the newly formed splice junction confirmed that 100% of treated patients displayed the expected skipped exon 51 sequence. In treated patients vs untreated controls, Western blot analysis of dystrophin content demonstrated an 11.6-fold increase (p = 0.007), and PDPF analysis demonstrated a 7.4-fold increase (p < 0.001). The PDPF findings were confirmed in a re-examination of the sample (15.5-fold increase, p < 0.001). Dystrophin immunofluorescence intensity was 2.4-fold greater in treated patients than in untreated controls (p < 0.001).ConclusionTaken together, the 4 assays, each based on unique evaluation mechanisms, provided evidence of eteplirsen muscle cell penetration, exon skipping, and induction of novel dystrophin expression.Classification of evidenceThis study provides Class II evidence of the muscle cell penetration, exon skipping, and induction of novel dystrophin expression by eteplirsen, as confirmed by 4 assays.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Neurology (clinical)

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