TABLE 3.
Gene therapy strategies and application to hiPSC-CM models to restore dystrophin function.
| Approach | Target mutation type | Dystrophin product | Strengths | Challenges | hiPSC-CM |
| Stop codon readthrough | Nonsense point mutations | Complete | • Well-tolerated (PTC124 or ataluren) | • Low efficiency in the heart • Low prevalence of amenable mutations • Frequent re-dosing | ? |
| AON-mediated exon skipping | Frameshift mutations | Lacking existing deletion and additional exon(s) | • Well-tolerated • Effective at cell level | • Poor cardiac uptake of PMO • Frequent re-dosing • Low number of amenable mutations for each AON drug | • Efficacy • Reduced arrhythmias (Liang et al., 2019) |
| AAV micro-dystrophin | not interacting with endogenous gene) | Extensively truncated but functional | • High efficacy in heart • High efficacy in skeletal muscle • Lasting (multiple years) | • Potentially immunogenic • Potential for null effect with pre-existing immunity | ? |
| CRISPR-Cas9 | Frameshift, insertion, and nonsense mutations | Depends on editing strategy [ranging from complete to lacking deletion and additional exon(s)] | • High efficacy in heart and skeletal muscle • Versatile • Genomic correction is life-long (theoretically) | • Potentially immunogenic • Risk of off-target editing • Low number of amenable mutations for each CRISPR drug | • Efficacy • Restored contractile force of EHTs (Kyrychenko et al., 2017; Long et al., 2018; Min et al., 2019; Zhang et al., 2017) |