2017
DOI: 10.1371/journal.pone.0187930
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Optimized approach for the identification of highly efficient correctors of nonsense mutations in human diseases

Abstract: About 10% of patients with a genetic disease carry a nonsense mutation causing their pathology. A strategy for correcting nonsense mutations is premature termination codon (PTC) readthrough, i.e. incorporation of an amino acid at the PTC position during translation. PTC-readthrough-activating molecules appear as promising therapeutic tools for these patients. Unfortunately, the molecules shown to induce PTC readthrough show low efficacy, probably because the mRNAs carrying a nonsense mutation are scarce, as th… Show more

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Cited by 26 publications
(38 citation statements)
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“…DAP contributes to the PTC-correcting activity of H7 extract. An extract (H7) prepared from the mushroom Lepista inversa (also currently called Paralepista flaccida) has recently been shown to exhibit high UAA and UGA readthrough-promoting activity 33 . To identify the compounds responsible for this activity, a semipreparative HPLC fractionation protocol was used.…”
Section: Resultsmentioning
confidence: 99%
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“…DAP contributes to the PTC-correcting activity of H7 extract. An extract (H7) prepared from the mushroom Lepista inversa (also currently called Paralepista flaccida) has recently been shown to exhibit high UAA and UGA readthrough-promoting activity 33 . To identify the compounds responsible for this activity, a semipreparative HPLC fractionation protocol was used.…”
Section: Resultsmentioning
confidence: 99%
“…Nine fractions (F7-F15) were obtained ( Fig. 1a) and tested for PTC-readthrough activity in a system using a PTC-carrying firefly luciferase mRNA subject to NMD 33 (Fig. 1b).…”
Section: Resultsmentioning
confidence: 99%
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“…In cell culture, amlexanox was able to rescue the expression of functional proteins from mRNAs containing nonsense mutations for p53, dystrophin, aspartylglucosaminidase, and type VII collagen [127,157,159]. Further potentially efficacious read-through agents include the nucleoside analog clitocine and components of fungi extracts that were identified in a recent drug screen [160,161]. Since the efficacy of these drugs is also dependent on their capability to cross the BBB, further research will be required to test if these drugs might also provide a therapy option for SSADH-D. Interestingly, the findings of Akaboshi and colleagues suggested that nonsense variants, especially Trp204X and Arg412X substitutions, are frequently present in SSADH-D [31].…”
Section: Small Molecules: Pharmacological Chaperones and Read-throughmentioning
confidence: 99%