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Synergistic Rescue of Nonsense Mutant Tumor Suppressor p53 by Combination Treatment with Aminoglycosides and Mdm2 Inhibitors.

Front Oncol. 2017; 
ZhangMeiqiongzi,HeldinAngelos,Palomar-SilesMireia,ÖhlinSusanne,BykovVladimir J N,WimanKl
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摘要

The tumor suppressor gene is inactivated by mutation in a large fraction of human tumors. Around 10% of mutations are nonsense mutations that lead to premature termination of translation and expression of truncated unstable and non-functional p53 protein. Aminoglycosides G418 (geneticin) and gentamicin have been shown to induce translational readthrough and expression of full-length p53. However, aminoglycosides have severe side effects that limit their clinical use. Here, we show that combination treatment with a proteasome inhibitor or compounds that disrupt p53-Mdm2 binding can synergistically enhance levels of full-length p53 upon aminoglycoside-induced readthrough of R213X nonsense mutant p53. Full-l... More

关键词

MDM2 inhibitors,aminoglycosides,nonsense mutation,p53,readthr