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2-Guanidino-quinazoline promotes the readthrough of nonsense mutations underlying human genetic diseases

Laure Bidou, Olivier Bugaud, Goulven Merer, Matthieu Coupet, Isabelle Hatin, Egor Chirkin, Sabrina Karri, Stéphane Demais, Pauline François, Jean‐Christophe Cintrat, Olivier Namy

2022Proceedings of the National Academy of Sciences16 citationsDOIOpen Access PDF

Abstract

Premature termination codons (PTCs) account for 10 to 20% of genetic diseases in humans. The gene inactivation resulting from PTCs can be counteracted by the use of drugs stimulating PTC readthrough, thereby restoring production of the full-length protein. However, a greater chemical variety of readthrough inducers is required to broaden the medical applications of this therapeutic strategy. In this study, we developed a reporter cell line and performed high-throughput screening (HTS) to identify potential readthrough inducers. After three successive assays, we isolated 2-guanidino-quinazoline (TLN468). We assessed the clinical potential of this drug as a potent readthrough inducer on the 40 PTCs most frequently responsible for Duchenne muscular dystrophy (DMD). We found that TLN468 was more efficient than gentamicin, and acted on a broader range of sequences, without inducing the readthrough of normal stop codons (TC).

Topics & Concepts

Nonsense mutationBiologyGeneDuchenne muscular dystrophyInducerGeneticsMutationTranslation (biology)Genetic screenStop codonQuinazolineComputational biologyMutantMessenger RNAChemistryCombinatorial chemistryMissense mutationRNA and protein synthesis mechanismsCRISPR and Genetic EngineeringRNA Interference and Gene Delivery
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