A ligand discovery toolbox for the WWE domain family of human E3 ligases

Author:

Münzker Lena,Kimani Serah W.ORCID,Fowkes Milan M.ORCID,Dong Aiping,Zheng Hong,Li YanjunORCID,Dasovich Morgan,Zak Krzysztof M.,Leung Anthony K. L.ORCID,Elkins Jonathan M.,Kessler DirkORCID,Arrowsmith Cheryl H.ORCID,Halabelian LevonORCID,Böttcher JarkORCID

Abstract

AbstractThe WWE domain is a relatively under-researched domain found in twelve human proteins and characterized by a conserved tryptophan-tryptophan-glutamate (WWE) sequence motif. Six of these WWE domain-containing proteins also contain domains with E3 ubiquitin ligase activity. The general recognition of poly-ADP-ribosylated substrates by WWE domains suggests a potential avenue for development of Proteolysis-Targeting Chimeras (PROTACs). Here, we present novel crystal structures of the HUWE1, TRIP12, and DTX1 WWE domains in complex with PAR building blocks and their analogs, thus enabling a comprehensive analysis of the PAR binding site structural diversity. Furthermore, we introduce a versatile toolbox of biophysical and biochemical assays for the discovery and characterization of novel WWE domain binders, including fluorescence polarization-based PAR binding and displacement assays, 15N-NMR-based binding affinity assays and 19F-NMR-based competition assays. Through these assays, we have characterized the binding of monomeric iso-ADP-ribose (iso-ADPr) and its nucleotide analogs with the aforementioned WWE proteins. Finally, we have utilized the assay toolbox to screen a small molecule fragment library leading to the successful discovery of novel ligands targeting the HUWE1 WWE domain.

Publisher

Springer Science and Business Media LLC

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