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Structural insights into WRN helicase reveal conformational states and opportunities for MSI-H cancer drug discovery
Journal article   Open access   Peer reviewed

Structural insights into WRN helicase reveal conformational states and opportunities for MSI-H cancer drug discovery

Catherine T. Fletcher, Abigail A. Mornement, Charlotte Barrett, Peter Canning, Prakash Rucktooa, Sophie Huber, Christopher D. O. Cooper, Conor C. G. Scully, Andrew S. Doré, Daniel Rohle, …
Communications biology, Vol.9(1), p.334
28/01/2026
PMID: 41606312

Abstract

13/1 38/91 631/45/173 631/535/1266 631/57/2272 631/67/1059/602 82/103 82/16 Article Biomedical and Life Sciences General Life Sciences
Werner syndrome helicase (WRN) is a RecQ-family DNA helicase essential for genome maintenance and is a synthetic lethal target in microsatellite instability-high (MSI-H) cancers. Despite its therapeutic promise, the conformational dynamics that enable WRN to unwind DNA, and how inhibitors disrupt this activity, remains poorly understood. Here, we present crystal structures of apo WRN and WRN bound to single-stranded DNA (ssDNA), capturing key conformations in the helicase catalytic cycle. These structures reveal how WRN engages DNA through conserved polar and aromatic interactions, and how domain rearrangements, including an ordering of the aromatic-rich loop (ARL), drive directional translocation. Biochemical and biophysical data demonstrate how nucleotide and inhibitor binding remodel these conformations and suggest that known clinical inhibitors (HRO761 and VVD-133214) function by locking WRN in inactive, ‘off-DNA’ states. Resistance emerged rapidly in vitro, through acquired point mutations as well as altered WRN expression. Together, our findings provide a structural framework for the WRN structural cycle and support the development of next-generation ‘on-DNA’ inhibitors to overcome resistance. In this study, Kennedy et al. combine crystallography, biophysical measurements and biochemical assays to define a structural cycle for Werner syndrome helicase (WRN) and reveal how nucleotide binding and ssDNA engagement lead to conformational transitions.
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https://doi.org/10.1038/s42003-026-09584-0View
Published (Version of record) Open CC BY V4.0

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