Uncovering an allosteric mode of action for a selective inhibitor of human Bloom syndrome protein

Author:

Chen X.ORCID,Ali Y.,Fisher C.E.L.,Arribas-Bosacoma R.ORCID,Rajasekaran M.B.,Williams G.,Walker S.,Booth J.R.,Hudson J.J.R.ORCID,Roe S.M.ORCID,Pearl L. H.ORCID,Ward S. E.ORCID,Pearl F. M. G.ORCID,Oliver A.W.ORCID

Abstract

ABSTRACTBLM (Bloom syndrome protein) is a RECQ-family helicase involved in the dissolution of complex DNA structures and repair intermediates. Synthetic lethality analysis implicates BLM as a promising target in a range of cancers with defects in the DNA damage response, however selective small molecule inhibitors of defined mechanism are currently lacking. Here we identify and characterise a specific inhibitor of BLM’s ATPase-coupled DNA helicase activity, by allosteric trapping of a DNA-bound translocation intermediate. Crystallographic structures of BLM-DNA-ADP-inhibitor complexes identify a hitherto unknown interdomain interface, whose opening and closing are integral to translocation of ssDNA, and which provides a highly selective pocket for drug discovery. Comparison with structures of other RECQ helicases provides a model for branch migration of Holliday junctions by BLM.

Publisher

Cold Spring Harbor Laboratory

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