Peptide-conjugated phosphodiamidate oligomer-mediated exon skipping has benefits for cardiac function in mdx and Cmah-/-mdx mouse models of Duchenne muscular dystrophy.

Alison M Blain,Matthew J Wood,Corinne A Betts,Caroline Godfrey,Thibault Coursindel,Raquel Manzano,Graham Mcclorey,Liz O’Donovan,Elizabeth Greally,Guy A Macgowan,Mike J Gait,Volker W Straub

doi:10.1371/journal.pone.0198897

Abstract

Cardiac failure is a major cause of mortality in patients with Duchenne muscular dystrophy (DMD). Antisense-mediated exon skipping has the ability to correct out-of-frame mutations in DMD to produce truncated but functional dystrophin. Traditional antisense approaches have however been limited by their poor uptake into cardiac muscle. The addition of cell-penetrating peptides to antisense molecules has increased their potency and improved their uptake into all muscles, including the heart. We have investigated the efficacy of the Peptide-conjugated phosphodiamidate morpholino oligomer (P-PMO) Pip6a-PMO, for restoration of cardiac dystrophin and functional rescue in DMD mice- the mdx mouse and the less well characterised Cmah-/-mdx mouse (which carry a human-like mutation in the mouse Cmah gene as well as a mutation in DMD). In our first study male mdx mice were administered Pip6a-PMO, i.v, fortnightly from 12 to 30 weeks of age alongside mock-injected age-matched mdx and C57BL10 controls. Mice received 4 doses of 18 mg/kg followed by 8 doses of 12.5 mg/kg. The cardiac function of the mice was analysed 2 weeks after their final injection by MRI followed by conductance catheter and their muscles were harvested for dystrophin quantification. In the second study, male Cmah-/-mdx mice, received 12.5 mg/kg Pip6a-PMO, i.v fortnightly from 8 to 26 weeks and assessed by MRI at 3 time points (12, 18 and 28 weeks) alongside mock-injected age-matched mdx, C57BL10 and Cmah-/-mdx controls. The mice also underwent MEMRI and conductance catheter at 28 weeks. This allowed us to characterise the cardiac phenotype of Cmah-/-mdx mice as well as assess the effects of P-PMO on cardiac function. Pip6a-PMO treatment resulted in significant restoration of dystrophin in mdx and Cmah-/-mdx mice (37.5% and 51.6%, respectively), which was sufficient to significantly improve cardiac function, ameliorating both right and left ventricular dysfunction. Cmah-/-mdx mice showed an abnormal response to dobutamine stress test and this was completely ameliorated by PIP6a-PMO treatment. These encouraging data suggest that total restoration of dystrophin may not be required to significantly improve cardiac outcome in DMD patients and that it may be realistic to expect functional improvements with modest levels of dystrophin restoration which may be very achievable in future clinical trials.

Highlights

Duchenne muscular dystrophy (DMD) is a degenerative genetic muscle disease that occurs in around 1 in 3500 live male births [1]
The condition is caused by mutations in a large 79-exon gene encoding the 427 kDa cytoskeletal protein dystrophin, which forms a critical part of the dystrophin-associated glycoprotein complex (DGC) [2,3]
No deaths were seen in the mock injected mice suggesting that the deaths in the phosphodiamidate morpholino oligomer (P-phosphodiamidate morpholino oligomer (PMO)) mice were not due to repeated anaesthesia or volume overload

Summary

Introduction

Duchenne muscular dystrophy (DMD) is a degenerative genetic muscle disease that occurs in around 1 in 3500 live male births [1]. The role of the DGC is best characterised in muscle where it stabilises the muscle membrane and protects the muscle from contraction-induced damage. Loss of dystrophin from the muscle membrane results in sarcolemmal instability, dysregulation of calcium signalling and a cycle of events which culminates in fatty replacement of muscle and reduced strength. Patients with DMD commonly harbour out-of-frame or nonsense mutations which result in a complete loss of dystrophin [4]. Evidence from patients with the milder allelic form of the disease, Becker muscular dystrophy (BMD), suggests that dystrophin can be partially functional, even with the presence of an internal deletion, if the “reading frame” is preserved [5,6]. The concept of exon skipping therapy for DMD (whereby a mutation-specific antisense oligonucleotide induces ‘skipping’ of the mutated exon during translation) was conceived over a decade ago and remains one of the most rational therapeutic strategies under development [7]

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