Discovery of a small-molecule inhibitor that traps Polθ on DNA and synergizes with PARP inhibitors

Author:

Fried William,Tyagi Mrityunjay,Minakhin Leonid,Chandramouly Gurushankar,Tredinnick TaylorORCID,Ramanjulu Mercy,Auerbacher William,Calbert MarissaORCID,Rusanov Timur,Hoang Trung,Borisonnik Nikita,Betsch Robert,Krais John J.ORCID,Wang Yifan,Vekariya Umeshkumar M.,Gordon John,Morton George,Kent Tatiana,Skorski Tomasz,Johnson NeilORCID,Childers Wayne,Chen Xiaojiang S.ORCID,Pomerantz Richard T.ORCID

Abstract

AbstractThe DNA damage response (DDR) protein DNA Polymerase θ (Polθ) is synthetic lethal with homologous recombination (HR) factors and is therefore a promising drug target in BRCA1/2 mutant cancers. We discover an allosteric Polθ inhibitor (Polθi) class with 4–6 nM IC50 that selectively kills HR-deficient cells and acts synergistically with PARP inhibitors (PARPi) in multiple genetic backgrounds. X-ray crystallography and biochemistry reveal that Polθi selectively inhibits Polθ polymerase (Polθ-pol) in the closed conformation on B-form DNA/DNA via an induced fit mechanism. In contrast, Polθi fails to inhibit Polθ-pol catalytic activity on A-form DNA/RNA in which the enzyme binds in the open configuration. Remarkably, Polθi binding to the Polθ-pol:DNA/DNA closed complex traps the polymerase on DNA for more than forty minutes which elucidates the inhibitory mechanism of action. These data reveal a unique small-molecule DNA polymerase:DNA trapping mechanism that induces synthetic lethality in HR-deficient cells and potentiates the activity of PARPi.

Publisher

Springer Science and Business Media LLC

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