Christopher J. Brown scite author profile

Currently, around 11 million people are living with a tumour that contains an inactivating mutation of TP53 (the human gene that encodes p53) and another 11 million have tumours in which the p53 pathway is partially abrogated through the inactivation of other signalling or effector components. The p53 pathway is therefore a prime target for new cancer drug development, and several original approaches to drug discovery that could have wide applications to drug development are being used. In one approach, molecules that activate p53 by blocking protein-protein interactions with MDM2 are in early clinical development. Remarkable progress has also been made in the development of p53-binding molecules that can rescue the function of certain p53 mutants. Finally, cell-based assays are being used to discover compounds that exploit the p53 pathway by either seeking targets and compounds that show synthetic lethality with TP53 mutations or by looking for non-genotoxic activators of the p53 response.

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Stapled Peptides with Improved Potency and Specificity That Activate p53

Brown

et al. 2012

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By using a phage display derived peptide as an initial template, compounds have been developed that are highly specific against Mdm2/Mdm4. These compounds exhibit greater potency in p53 activation and protein-protein interaction assays than a compound derived from the p53 wild-type sequence. Unlike Nutlin, a small molecule inhibitor of Mdm2/Mdm4, the phage derived compounds can arrest cells resistant to p53 induced apoptosis over a wide concentration range without cellular toxicity, suggesting they are highly suitable for cyclotherapy.

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Functionalised staple linkages for modulating the cellular activity of stapled peptides

et al. 2014

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Reactivation of p53: from peptides to small molecules

Brown

Cheok

Verma

et al. 2011

Trends in Pharmacological Sciences

122

118

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Differential binding of p53 and nutlin to MDM2 and MDMX: Computational studies

Joseph

Madhumalar²,

Brown³

et al. 2010

Cell Cycle

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