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. These enhancers potentiate the ubiquitylation of mutant β-Catenin by β-TrCP in vitro and induce the degradation of an engineered mutant β-Catenin in a cellular system. Distinct from PROTACs, these drug-like small molecules insert into a naturally occurring PPI interface, with contacts optimized for both the substrate and ligase within the same small molecule entity. The prospective discovery of 'molecular glue' presented here provides a paradigm for the development of small molecule degraders targeting hard-to-drug proteins.
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K.R. Simonetta
Nurix (United States)
Joshua P. Taygerly
Fluxion Biosciences (United States)
Kathleen Boyle
Nurix (United States)
Nature Communications
University of California, Berkeley
Howard Hughes Medical Institute
Wilmington University
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Simonetta et al. (Fri,) studied this question.
synapsesocial.com/papers/6a028a9c4f17ebd438650845 — DOI: https://doi.org/10.1038/s41467-019-09358-9