2. Academic Validation
  3. Validation, Key Pharmacophores, and X-ray Cocrystal Structures of Novel Biochemically and Cellularly Active WRN Inhibitors Derived from a DNA-Encoded Library Screen

Validation, Key Pharmacophores, and X-ray Cocrystal Structures of Novel Biochemically and Cellularly Active WRN Inhibitors Derived from a DNA-Encoded Library Screen

  • J Med Chem. 2025 Jun 26;68(12):12434-12456. doi: 10.1021/acs.jmedchem.4c03029.
Yunsong Tong 1 Kenton A Baker 1 Alex M Chapman 1 Nathaniel L Elsen 1 Faith Fowler 2 Mariam D George 1 Nathan J Gesmundo 1 Harry Hatton 3 Michael Hickey 3 Charles W Hutchins 1 Cynthia L Jeffries 1 Aileen Kelly 1 Alla Korepanova 1 Iain R Miller 3 Boguslaw Nocek 1 Sanjay C Panchal 1 Orville A Pemberton 1 Wei Qiu 1 Nari N Talaty 1 Henry Yue Hin Tang 1 Danli Towne 1 Maomao Zhang 2 Yiming Zhao 3 Sujatha M Gopalakrishnan 1 Chaohong Sun 1 Michael E Kort 1 Michael J Dart 1 Ari J Firestone 2
Affiliations

Affiliations

  • 1 Abbvie, 1 North Waukegan Road, North Chicago, Illinois 60064, United States.
  • 2 Calico Life Sciences,1130 Veterans Boulevard, South San Francisco, California 94080, United States.
  • 3 Sygnature Discovery, Biocity, Pennyfoot Street, Nottingham NG1 1GR, United Kingdom.
PMID: 40472162 DOI: 10.1021/acs.jmedchem.4c03029
Abstract

A novel class of selective and potent WRN helicase antagonists identified via a DNA-encoded library screen was rigorously validated by various biophysical assays including ASMS, TSA, and SPR. Preliminary structure-activity-relationship studies identified the key pharmacophores and advanced the biochemical potency to single digit nanomolar. Potent analogs demonstrated anti-proliferative activities specifically in cell lines with a WRN genetic dependency. A crystal structure of a ligand-WRN complex revealed an unexpected large shift of the helicase domain compared to the apo WRN structure with ADP. These structural insights led to the successful design of covalent inhibitors and the identification of compound resistant WRN mutants that confirmed on-mechanism cellular activity. The covalent interaction between the ligand and at WRN Cys727 was confirmed by intact mass spectrometry and a bound crystal structure. The discovery of these unique WRN inhibitors provides more insight into the field and offers an opportunity to further optimize such molecules.

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