Local Dystrophin Restoration with Antisense Oligonucleotide PRO051

doi:10.1056/NEJMoa073108

Volume 357:2677-2686		December 27, 2007		Number 26

Local Dystrophin Restoration with Antisense Oligonucleotide PRO051

Judith C. van Deutekom, Ph.D., Anneke A. Janson, B.S., Ieke B. Ginjaar, Ph.D., Wendy S. Frankhuizen, B.S., Annemieke Aartsma-Rus, Ph.D., Mattie Bremmer-Bout, B.S., Johan T. den Dunnen, Ph.D., Klaas Koop, M.D., Anneke J. van der Kooi, M.D., Ph.D., Nathalie M. Goemans, M.D., Ph.D., Sjef J. de Kimpe, Ph.D., Peter F. Ekhart, M.Sc., Edna H. Venneker, M.D., Gerard J. Platenburg, M.Sc., Jan J. Verschuuren, M.D., Ph.D., and Gert-Jan B. van Ommen, Ph.D.

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by Hoffman, E. P.

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ABSTRACT

Background Duchenne's muscular dystrophy is associated withsevere, progressive muscle weakness and typically leads to deathbetween the ages of 20 and 35 years. By inducing specific exonskipping during messenger RNA (mRNA) splicing, antisense compoundswere recently shown to correct the open reading frame of theDMD gene and thus to restore dystrophin expression in vitroand in animal models in vivo. We explored the safety, adverse-eventprofile, and local dystrophin-restoring effect of a single,intramuscular dose of an antisense oligonucleotide, PRO051,in patients with this disease.

Methods Four patients, who were selected on the basis of theirmutational status, muscle condition, and positive exon-skippingresponse to PRO051 in vitro, received a dose of 0.8 mg of PRO051injected into the tibialis anterior muscle. A biopsy was performed28 days later. Safety measures, composition of mRNA, and dystrophinexpression were assessed.

Results PRO051 injection was not associated with clinicallyapparent adverse events. Each patient showed specific skippingof exon 51 and sarcolemmal dystrophin in 64 to 97% of myofibers.The amount of dystrophin in total protein extracts ranged from3 to 12% of that found in the control specimen and from 17 to35% of that of the control specimen in the quantitative ratioof dystrophin to laminin ${alpha}$ 2.

Conclusions Intramuscular injection of antisense oligonucleotidePRO051 induced dystrophin synthesis in four patients with Duchenne'smuscular dystrophy who had suitable mutations, suggesting thatfurther studies might be feasible.

Source Information

From the Departments of Human and Clinical Genetics (J.C.D., A.A.J., I.B.G., W.S.F., A.A.-R., M.B.-B., J.T.D., G.-J.B.O.), Pathology (K.K.), and Neurology (J.J.V.), Leiden University Medical Center; and Prosensa B.V. (J.C.D., S.J.K., P.F.E., G.J.P.) — both in Leiden, the Netherlands; the Department of Neurology, Academic Medical Center, University of Amsterdam, Amsterdam (A.J.K.); the Department of Pediatric Neurology, University of Leuven, Leuven, Belgium (N.M.G.); and Afforce Healthcare, The Hague, the Netherlands (E.H.V.).

Address reprint requests to Dr. van Deutekom at Prosensa B.V., Wassenaarseweg 72, 2333 AL Leiden, the Netherlands, or at j.vandeutekom{at}prosensa.nl.

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