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Regulation of p53 by the 14-3-3 protein interaction network: new opportunities for drug discovery in cancer

Authors :
Richard G. Doveston
Jake A. Ward
Salvador Macip
Marta Falcicchio
Source :
Cell Death Discovery, Vol 6, Iss 1, Pp 1-21 (2020), Cell Death Discovery
Publication Year :
2020
Publisher :
Nature Publishing Group, 2020.

Abstract

Most cancers evolve to disable the p53 pathway, a key tumour suppressor mechanism that prevents transformation and malignant cell growth. However, only ~50% exhibit inactivating mutations of p53, while in the rest its activity is suppressed by changes in the proteins that modulate the pathway. Therefore, restoring p53 activity in cells in which it is still wild type is a highly attractive therapeutic strategy that could be effective in many different cancer types. To this end, drugs can be used to stabilise p53 levels by modulating its regulatory pathways. However, despite the emergence of promising strategies, drug development has stalled in clinical trials. The need for alternative approaches has shifted the spotlight to the 14-3-3 family of proteins, which strongly influence p53 stability and transcriptional activity through direct and indirect interactions. Here, we present the first detailed review of how 14-3-3 proteins regulate p53, with special emphasis on the mechanisms involved in their binding to different members of the pathway. This information will be important to design new compounds that can reactivate p53 in cancer cells by influencing protein–protein interactions. The intricate relationship between the 14-3-3 isoforms and the p53 pathway suggests that many potential drug targets for p53 reactivation could be identified and exploited to design novel antineoplastic therapies with a wide range of applications.

Details

Language :
English
ISSN :
20587716
Volume :
6
Issue :
1
Database :
OpenAIRE
Journal :
Cell Death Discovery
Accession number :
edsair.doi.dedup.....990efe3f2a48e81b06d629c501c4ed07