Journal article

Targeted protein degradation: expanding the toolbox

Abstract:: Proteolysis-targeting chimeras (PROTACs) and related molecules that induce targeted protein degradation by the ubiquitin-proteasome system represent a new therapeutic modality and are the focus of great interest, owing to potential advantages over traditional occupancy-based inhibitors with respect to dosing, side effects, drug resistance and modulating 'undruggable' targets. However, the technology is still maturing, and the design elements for successful PROTAC-based drugs are currently being elucidated. Importantly, fewer than 10 of the more than 600 E3 ubiquitin ligases have so far been exploited for targeted protein degradation, and expansion of knowledge in this area is a key opportunity. Here, we briefly discuss lessons learned about targeted protein degradation in chemical biology and drug discovery and systematically review the expression profile, domain architecture and chemical tractability of human E3 ligases that could expand the toolbox for PROTAC discovery.

Publication status:: Published

Peer review status:: Peer reviewed

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APA Style

Schapira, M., Calabrese, M., Bullock, A., & Crews, C. (2019). Targeted protein degradation: expanding the toolbox. Nature Reviews Drug Discovery, 18, 949–963.

MLA Style

Schapira, M., et al. “Targeted Protein Degradation: Expanding the Toolbox.” Nature Reviews Drug Discovery, vol. 18, Nature Research, 2019, pp. 949–63.

Chicago Style

Schapira, M, M Calabrese, A Bullock, and C Crews. 2019. “Targeted Protein Degradation: Expanding the Toolbox.” Nature Reviews Drug Discovery 18: 949–63.
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Files:: NRDD Schapira final ms for deposition.pdf

(Preview, Accepted manuscript, pdf, 1.7MB, Terms of use)

Publisher copy:: 10.1038/s41573-019-0047-y

Authors

+ Schapira, M More by this author

Role:: Author
ORCID:: 0000-0002-1047-3309

+ Calabrese, M More by this author

Role:: Author

+ Bullock, A More by this author

Institution:: University of Oxford
Division:: MSD
Department:: NDM
Sub department:: Structural Genomics Consortium
Role:: Author
ORCID:: 0000-0001-6757-0436

+ Crews, C More by this author

Role:: Author
ORCID:: 0000-0002-8456-2005

Publisher:: Nature Research
Journal:: Nature Reviews Drug Discovery More from this journal
Volume:: 18
Pages:: 949–963
Publication date:: 2019-10-30
Acceptance date:: 2019-09-23
DOI:: 10.1038/s41573-019-0047-y
EISSN:: 1474-1784
ISSN:: 1474-1776
Pmid:: 31666732

Language:: English
Keywords:: FFR
Pubs id:: pubs:1069960
UUID:: uuid:7291c51e-b058-4f99-87c6-3085ed467c2e
Local pid:: pubs:1069960
Source identifiers:: 1069960
Deposit date:: 2019-11-27

Terms of use

Copyright holder:: Schapira et al.
Copyright date:: 2019
Rights statement:: Copyright © The Author(s) 2019.
Notes:: This is the accepted manuscript version of the article. The final version is available from Nature Research at https://doi.org/10.1038/s41573-019-0047-y

Licence:: Terms and Conditions of Use for Oxford University Research Archive

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