Readthrough compounds for nonsense mutations: bridging the translational gap

Publication date

2023-04

Authors

Spelier, Sacha
van Doorn, Eveline P.M.
van der Ent, KorsISNI 0000000388008551
Beekman, JMISNI 0000000388915338
Koppens, Martijn A J

Editors

Advisors

Supervisors

Document Type

Article

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License

cc_by_nc_nd

Abstract

Approximately 10% of all pathological mutations are nonsense mutations that are responsible for several severe genetic diseases for which no treatment regimens are currently available. The most widespread strategy for treating nonsense mutations is by enhancing ribosomal readthrough of premature termination codons (PTCs) to restore the production of the full-length protein. In the past decade several compounds with readthrough potential have been identified. However, although preclinical results on these compounds are promising, clinical studies have not yielded positive outcomes. We review preclinical and clinical research related to readthrough compounds and characterize factors that contribute to the observed translational gap.

Keywords

nonsense mutations, nonsense-mediated decay, rare diseases, readthrough, translational gap, Molecular Medicine, Molecular Biology

Citation

Spelier, S, van Doorn, E P M, van der Ent, C K, Beekman, J M & Koppens, M A J 2023, 'Readthrough compounds for nonsense mutations : bridging the translational gap', Trends in molecular medicine, vol. 29, no. 4, pp. 297-314. https://doi.org/10.1016/j.molmed.2023.01.004