Mechanisms of natural gene therapy in dystrophic epidermolysis bullosa.

[dystrophic epidermolysis bullosa]

Revertant mosaicism has been reported in several inherited diseases , including the genetic skin fragility disorder epidermolysis bullosa (EB ). Here , we describe the largest cohort of seven patients with revertant mosaicism and dystrophic EB (DEB ), associated with mutations in the COL 7 A 1 gene , and determine the underlying molecular mechanisms . We show that revertant mosaicism occurs both in autosomal dominantly and recessively inherited DEB . We found that null mutations resulting in complete loss of collagen VII and severe disease , as well as missense or splice-site mutations associated with some preserved collagen VII function and a milder phenotype , were corrected by revertant mosaicism . The mutation , subtype , and severity of the disease are thus not decisive for the presence of revertant mosaicism . Although collagen VII is synthesized and secreted by both keratinocytes and fibroblasts , evidence for reversion was only found in keratinocytes . The reversion mechanisms included back mutations /mitotic recombinations in 70 % of the cases and second -site mutations affecting splicing in 30 %. We conclude that revertant mosaicism is more common than previously assumed in patients with DEB , and our findings will have implications for future therapeutic strategies using the patient 's naturally corrected cells as a source for cell-based therapies .