Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene

Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene

Protein-truncating mutations in the dystrophin gene lead to the progressive muscle wasting disorder Duchenne muscular dystrophy, whereas in-frame deletions typically manifest as the milder allelic condition, Becker muscular dystrophy. Antisense oligomer-induced exon skipping can modify dystrophin ge...

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Bibliographic Details
Main Authors: Sue Fletcher, Carl F. Adkin, Penny Meloni, Brenda Wong, Francesco Muntoni, Ryszard Kole, Clayton Fragall, Kane Greer, Russell Johnsen, Steve D. Wilton
Format: Article
Language:English
Published: Elsevier 2012-01-01
Series:Molecular Therapy: Nucleic Acids
Subjects:
antisense oligomers
Duchenne muscular dystrophy
exon skipping
personalized genetic therapy
splice-switching
Online Access:http://www.sciencedirect.com/science/article/pii/S2162253116301068
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spelling doaj-bef9514bacf54e2886ea174f3e8695342020-11-24T23:17:13ZengElsevierMolecular Therapy: Nucleic Acids2162-25312012-01-011C10.1038/mtna.2012.40Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin GeneSue Fletcher0Carl F. Adkin1Penny Meloni2Brenda Wong3Francesco Muntoni4Ryszard Kole5Clayton Fragall6Kane Greer7Russell Johnsen8Steve D. Wilton9Centre for Neuromuscular and Neurological Disorders, University of Western Australia, Perth, AustraliaCentre for Neuromuscular and Neurological Disorders, University of Western Australia, Perth, AustraliaCentre for Neuromuscular and Neurological Disorders, University of Western Australia, Perth, AustraliaDepartment of Pediatrics, Cincinnati Children's Hospital Medical Centre and University of Cincinnati College of Medicine, Cincinnati, Ohio, USAThe Dubowitz Neuromuscular Centre, University College London, Institute of Child Health London, UKAVI Biopharma, Bothell, Washington, USASchool of Pathology and Laboratory Medicine, University of Western Australia, Perth, AustraliaCentre for Neuromuscular and Neurological Disorders, University of Western Australia, Perth, AustraliaCentre for Neuromuscular and Neurological Disorders, University of Western Australia, Perth, AustraliaCentre for Neuromuscular and Neurological Disorders, University of Western Australia, Perth, AustraliaProtein-truncating mutations in the dystrophin gene lead to the progressive muscle wasting disorder Duchenne muscular dystrophy, whereas in-frame deletions typically manifest as the milder allelic condition, Becker muscular dystrophy. Antisense oligomer-induced exon skipping can modify dystrophin gene expression so that a disease-associated dystrophin pre-mRNA is processed into a Becker muscular dystrophy-like mature transcript. Despite genomic deletions that may encompass hundreds of kilobases of the gene, some dystrophin mutations appear “leaky”, and low levels of high molecular weight, and presumably semi-functional, dystrophin are produced. A likely causative mechanism is endogenous exon skipping, and Duchenne individuals with higher baseline levels of dystrophin may respond more efficiently to the administration of splice-switching antisense oligomers. We optimized excision of exons 8 and 9 in normal human myoblasts, and evaluated several oligomers in cells from eight Duchenne muscular dystrophy patients with deletions in a known “leaky” region of the dystrophin gene. Inter-patient variation in response to antisense oligomer induced skipping in vitro appeared minimal. We describe oligomers targeting exon 8, that unequivocally increase dystrophin above baseline in vitro, and propose that patients with leaky mutations are ideally suited for participation in antisense oligomer mediated splice-switching clinical studies.http://www.sciencedirect.com/science/article/pii/S2162253116301068antisense oligomersDuchenne muscular dystrophyexon skippingpersonalized genetic therapysplice-switching
collection DOAJ
language English
format Article
sources DOAJ
author Sue Fletcher
Carl F. Adkin
Penny Meloni
Brenda Wong
Francesco Muntoni
Ryszard Kole
Clayton Fragall
Kane Greer
Russell Johnsen
Steve D. Wilton
spellingShingle Sue Fletcher
Carl F. Adkin
Penny Meloni
Brenda Wong
Francesco Muntoni
Ryszard Kole
Clayton Fragall
Kane Greer
Russell Johnsen
Steve D. Wilton
Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene
Molecular Therapy: Nucleic Acids
antisense oligomers
Duchenne muscular dystrophy
exon skipping
personalized genetic therapy
splice-switching
author_facet Sue Fletcher
Carl F. Adkin
Penny Meloni
Brenda Wong
Francesco Muntoni
Ryszard Kole
Clayton Fragall
Kane Greer
Russell Johnsen
Steve D. Wilton
author_sort Sue Fletcher
title Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene
title_short Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene
title_full Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene
title_fullStr Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene
title_full_unstemmed Targeted Exon Skipping to Address “Leaky” Mutations in the Dystrophin Gene
title_sort targeted exon skipping to address “leaky” mutations in the dystrophin gene
publisher Elsevier
series Molecular Therapy: Nucleic Acids
issn 2162-2531
publishDate 2012-01-01
description Protein-truncating mutations in the dystrophin gene lead to the progressive muscle wasting disorder Duchenne muscular dystrophy, whereas in-frame deletions typically manifest as the milder allelic condition, Becker muscular dystrophy. Antisense oligomer-induced exon skipping can modify dystrophin gene expression so that a disease-associated dystrophin pre-mRNA is processed into a Becker muscular dystrophy-like mature transcript. Despite genomic deletions that may encompass hundreds of kilobases of the gene, some dystrophin mutations appear “leaky”, and low levels of high molecular weight, and presumably semi-functional, dystrophin are produced. A likely causative mechanism is endogenous exon skipping, and Duchenne individuals with higher baseline levels of dystrophin may respond more efficiently to the administration of splice-switching antisense oligomers. We optimized excision of exons 8 and 9 in normal human myoblasts, and evaluated several oligomers in cells from eight Duchenne muscular dystrophy patients with deletions in a known “leaky” region of the dystrophin gene. Inter-patient variation in response to antisense oligomer induced skipping in vitro appeared minimal. We describe oligomers targeting exon 8, that unequivocally increase dystrophin above baseline in vitro, and propose that patients with leaky mutations are ideally suited for participation in antisense oligomer mediated splice-switching clinical studies.
topic antisense oligomers
Duchenne muscular dystrophy
exon skipping
personalized genetic therapy
splice-switching
url http://www.sciencedirect.com/science/article/pii/S2162253116301068
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