Differential PROTAC substrate specificity dictated by orientation of recruited E3 ligase

Smith, Blake E.; Wang, Stephen L.; Jaime‐Figueroa, Saul; Harbin, Alicia; Wang, Jing; Hamman, Brian D.; Crews, Craig M.

doi:10.1038/s41467-018-08027-7

articleNature CommunicationsJan 4, 2019GOLD OA

Differential PROTAC substrate specificity dictated by orientation of recruited E3 ligase

BEBlake E. Smith SLStephen L. Wang SJSaul Jaime‐Figueroa AHAlicia Harbin JWJing Wang

Yale University · Arvinas (United States)

PubMed

Indexed incrossrefdoajpubmed

Abstract

PROteolysis-TArgeting Chimeras (PROTACs) are hetero-bifunctional molecules that recruit an E3 ubiquitin ligase to a given substrate protein resulting in its targeted degradation. Many potent PROTACs with specificity for dissimilar targets have been developed; however, the factors governing degradation selectivity within closely-related protein families remain elusive. Here, we generate isoform-selective PROTACs for the p38 MAPK family using a single warhead (foretinib) and recruited E3 ligase (von Hippel-Lindau). Based on their distinct linker attachments and lengths, these two PROTACs differentially recruit VHL, resulting in degradation of p38α or p38δ. We characterize the role of ternary complex formation in…

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Topics & keywords

Topics

Keywords

Ubiquitin ligase
Ubiquitin
Ternary complex
Cell biology
DNA ligase
Protein degradation
Chemistry
Proteolysis

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Funding

NI
National Institutes of Health
Award: R35CA197589