Cell-Active Small Molecule Inhibitors of the DNA-Damage Repair Enzyme Poly(ADP-ribose) Glycohydrolase (PARG): Discovery and Optimization of Orally Bioavailable Quinazolinedione Sulfonamides | Zendy

Bohdan Waszkowycz | Zendy; Kate M. Smith | Zendy; Alison E. McGonagle | Zendy; Allan M. Jordan | Zendy; Ben Acton | Zendy; Emma Fairweather | Zendy; Louise A. Griffiths | Zendy; Niall M. Hamilton | Zendy; Nicola Hamilton | Zendy; James R. Hitchin | Zendy; Colin Hutton | Zendy; Dominic I. James | Zendy; Clifford D. Jones | Zendy; Stuart Jones | Zendy; Daniel P. Mould | Zendy; Helen Small | Zendy; Alexandra Stowell | Zendy; Julie A. Tucker | Zendy; Ian D. Waddell | Zendy; Donald Ogilvie | Zendy

Open Access

Cell-Active Small Molecule Inhibitors of the DNA-Damage Repair Enzyme Poly(ADP-ribose) Glycohydrolase (PARG): Discovery and Optimization of Orally Bioavailable Quinazolinedione Sulfonamides

Author(s) -

Bohdan Waszkowycz,

Kate M. Smith,

Alison E. McGonagle,

Allan M. Jordan,

Ben Acton,

Emma Fairweather,

Louise A. Griffiths,

Niall M. Hamilton,

Nicola Hamilton,

James R. Hitchin,

Colin Hutton,

Dominic I. James,

Clifford D. Jones,

Stuart Jones,

Daniel P. Mould,

Helen Small,

Alexandra Stowell,

Julie A. Tucker,

Ian D. Waddell,

Donald Ogilvie

Publication year - 2018

Publication title -

journal of medicinal chemistry

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.01

H-Index - 261

eISSN - 1520-4804

pISSN - 0022-2623

DOI - 10.1021/acs.jmedchem.8b01407

Subject(s) - chemistry , enzyme , in vivo , dna repair , small molecule , dna damage , poly adp ribose polymerase , active site , biochemistry , drug discovery , dna , biology , polymerase , microbiology and biotechnology

DNA damage repair enzymes are promising targets in the development of new therapeutic agents for a wide range of cancers and potentially other diseases. The enzyme poly(ADP-ribose) glycohydrolase (PARG) plays a pivotal role in the regulation of DNA repair mechanisms; however, the lack of potent drug-like inhibitors for use in cellular and in vivo models has limited the investigation of its potential as a novel therapeutic target. Using the crystal structure of human PARG in complex with the weakly active and cytotoxic anthraquinone 8a, novel quinazolinedione sulfonamides PARG inhibitors have been identified by means of structure-based virtual screening and library design. 1-Oxetan-3-ylmethyl derivatives 33d and 35d were selected for preliminary investigations in vivo. X-ray crystal structures help rationalize the observed structure-activity relationships of these novel inhibitors.

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