| Literature DB >> 34570508 |
Jeffrey W Johannes1, Amber Balazs1, Derek Barratt2, Michal Bista2, Matthew D Chuba1, Sabina Cosulich3, Susan E Critchlow4, Sébastien L Degorce1, Paolo Di Fruscia2, Scott D Edmondson1, Kevin Embrey2, Stephen Fawell5, Avipsa Ghosh1, Sonja J Gill6, Anders Gunnarsson7, Sudhir M Hande1, Tom D Heightman8, Paul Hemsley2, Giuditta Illuzzi4, Jordan Lane2, Carrie Larner6, Elisabetta Leo4, Lina Liu9, Andrew Madin2, Scott Martin10, Lisa McWilliams2, Mark J O'Connor4, Jonathan P Orme2, Fiona Pachl11, Martin J Packer12, Xiaohui Pei9, Andrew Pike10, Marianne Schimpl2, Hongyao She9, Anna D Staniszewska4, Verity Talbot2, Elizabeth Underwood2, Jeffrey G Varnes1, Lin Xue9, Tieguang Yao9, Ke Zhang9, Andrew X Zhang11, Xiaolan Zheng1.
Abstract
Poly-ADP-ribose-polymerase (PARP) inhibitors have achieved regulatory approval in oncology for homologous recombination repair deficient tumors including BRCA mutation. However, some have failed in combination with first-line chemotherapies, usually due to overlapping hematological toxicities. Currently approved PARP inhibitors lack selectivity for PARP1 over PARP2 and some other 16 PARP family members, and we hypothesized that this could contribute to toxicity. Recent literature has demonstrated that PARP1 inhibition and PARP1-DNA trapping are key for driving efficacy in a BRCA mutant background. Herein, we describe the structure- and property-based design of 25 (AZD5305), a potent and selective PARP1 inhibitor and PARP1-DNA trapper with excellent in vivo efficacy in a BRCA mutant HBCx-17 PDX model. Compound 25 is highly selective for PARP1 over other PARP family members, with good secondary pharmacology and physicochemical properties and excellent pharmacokinetics in preclinical species, with reduced effects on human bone marrow progenitor cells in vitro.Entities:
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Year: 2021 PMID: 34570508 DOI: 10.1021/acs.jmedchem.1c01012
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446