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Review
. 2010 Feb;20(1):40-5.
doi: 10.1016/j.semcancer.2010.02.007. Epub 2010 Mar 4.

The discovery of nongenotoxic activators of p53: building on a cell-based high-throughput screen

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Review

The discovery of nongenotoxic activators of p53: building on a cell-based high-throughput screen

Anna R McCarthy et al. Semin Cancer Biol. 2010 Feb.

Abstract

The reactivation of mutant forms of the transcriptional regulator p53 or artificially raising activated p53 levels in a controlled nongenotoxic manner are seen as two of the grand challenges in anti-cancer drug discovery. Recent reports suggest that these demanding goals are achievable. This review article focuses on the use of cell-based high-throughput screening to discover novel nongenotoxic activators of endogenous p53. This challenging approach to the early phases of drug discovery prioritises the discovery of compounds with activity in cells in the hope that the compounds discovered will ultimately be of more direct relevance to therapeutic development. However, this approach also requires that protein target identification studies are carried out. We, and others, have shown that whilst a sometimes daunting proposition, it is possible to identify the targets of compounds that activate p53.

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