Structure Report for: 8BTA

Zhao, Y.,Jones, E.Y.,Fish, P.

Title: Designed switch from covalent to non-covalent inhibitors of carboxylesterase Notum activity
Atkinson BN, Willis NJ, Zhao Y, Patel C, Frew S, Costelloe K, Magno L, Svensson F, Jones EY, Fish PV
Ref: Eur Journal of Medicinal Chemistry, 251:115132, 2023 : PubMed
Abstract


ESTHER: Atkinson_2023_Eur.J.Med.Chem_251_115132
PubMedSearch: Atkinson 2023 Eur.J.Med.Chem 251 115132
PubMedID: 36934521
Inhibitor(s) related to this paper: ARUK3004048, ARUK3004308, ARUK3004558, ARUK3005522, ARUK3005518, ARUK3004876

Abstract

N-Acyl indolines 4 are potent, non-covalent Notum inhibitors developed from a covalent virtual screening hit 2a. The lead compounds were simple to synthesise, achieved excellent potency in a biochemical Notum-OPTS assay and restored Wnt signalling in a cell-based TCF/LEF reporter assay. Multiple high resolution X-ray structures established a common binding mode of these inhibitors with the indoline bound centred in the palmiteolate pocket with key interactions being aromatic stacking and a water mediated hydrogen bond to the oxyanion hole. These N-acyl indolines 4 will be useful tools for use in vitro studies to investigate the role of Notum in disease models, especially when paired with a structurally related covalent inhibitor (e.g. 4w and 2a). Overall, this study highlights the designed switch from covalent to non-covalent Notum inhibitors and so illustrates a complementary approach for hit generation and target inhibition.