Use of 2,6-diaminopurine as a potent suppressor of UGA premature stop codons in cystic fibrosis

Publication date

2023-04-05

Authors

Leroy, Catherine
Spelier, Sacha
Essonghe, Nadège Charlene
Poix, Virginie
Kong, Rebekah
Gizzi, Patrick
Bourban, Claire
Amand, Séverine
Bailly, Christine
Guilbert, Romain

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Document Type

Article

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Abstract

Nonsense mutations are responsible for around 10% of cases of genetic diseases, including cystic fibrosis. 2,6-diaminopurine (DAP) has recently been shown to promote efficient readthrough of UGA premature stop codons. In this study, we show that DAP can correct a nonsense mutation in the Cftr gene in vivo in a new CF mouse model, in utero, and through breastfeeding, thanks, notably, to adequate pharmacokinetic properties. DAP turns out to be very stable in plasma and is distributed throughout the body. The ability of DAP to correct various endogenous UGA nonsense mutations in the CFTR gene and to restore its function in mice, in organoids derived from murine or patient cells, and in cells from patients with cystic fibrosis reveals the potential of such readthrough-stimulating molecules in developing a therapeutic approach. The fact that correction by DAP of certain nonsense mutations reaches a clinically relevant level, as judged from previous studies, makes the use of this compound all the more attractive.

Keywords

2,6-diaminopurine, cystic fibrosis, mouse model, nonsense mutation, readthrough molecule, Molecular Medicine, Molecular Biology, Genetics, Pharmacology, Drug Discovery

Citation

Leroy, C, Spelier, S, Essonghe, N C, Poix, V, Kong, R, Gizzi, P, Bourban, C, Amand, S, Bailly, C, Guilbert, R, Hannebique, D, Persoons, P, Arhant, G, Prévotat, A, Reix, P, Hubert, D, Gérardin, M, Chamaillard, M, Prevarskaya, N, Rebuffat, S, Shapovalov, G, Beekman, J & Lejeune, F 2023, 'Use of 2,6-diaminopurine as a potent suppressor of UGA premature stop codons in cystic fibrosis', Molecular Therapy, vol. 31, no. 4, pp. 970-985. https://doi.org/10.1016/j.ymthe.2023.01.014