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Mitigation of Acetylcholine Esterase Activity in the 1,7-Diazacarbazole Series of Inhibitors of Checkpoint Kinase 1

Checkpoint kinase 1 (ChK1) plays a key role in the DNA damage response, facilitating cell-cycle arrest to provide sufficient time for lesion repair. This leads to the hypothesis that inhibition of ChK1 might enhance the effectiveness of DNA-damaging therapies in the treatment of cancer. Lead compound 1 (GNE-783), the prototype of the 1,7-diazacarbazole class of ChK1 inhibitors, was found to be a highly potent inhibitor of acetylcholine esterase (AChE) and unsuitable for development. A campaign of analogue synthesis established SAR delineating ChK1 and AChE activities and allowing identification of new leads with improved profiles. In silico docking using a model of AChE permitted rationalization of the observed SAR. Compounds 19 (GNE-900) and 30 (GNE-145) were identified as selective, orally bioavailable ChK1 inhibitors offering excellent in vitro potency with significantly reduced AChE activity. In combination with gemcitabine, these compounds demonstrate an in vivo pharmacodynamic effect and are efficacious in a mouse p53 mutant xenograft model

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Identification of C‑2 Hydroxyethyl Imidazopyrrolopyridines as Potent JAK1 Inhibitors with Favorable Physicochemical Properties and High Selectivity over JAK2

Author: Adam Johnson (243334)
Anne van Abbema (1947484)
Austin Reeve (1947670)
Barbara Avitabile-Woo (1947640)
Charles Eigenbrot (1346406)
Charles Ellwood (1577416)
Chris Hamman (1947652)
Christine Chang (111265)
Christopher A. Hurley (1947685)
Eric Harstad (1947643)
Gauri Deshmukh (1503163)
Ignacio Aliagas (1465009)
Jane R. Kenny (1947679)
Janusz J. Kulagowski (1947664)
Jason DeVoss (1593535)
Jiangpeng Liao (1947631)
Jing Yang (13969)
Kathy Barrett (1600633)
Mark Zak (1845538)
Marya Liimatta (1638922)
Mercedesz Balazs (178787)
Micah Steffek (114377)
Michael F. T. Koehler (1443895)
Nico Ghilardi (201347)
Paroma Chakravarty (1891471)
Paul Gibbons (114343)
Pawan Bir Kohli (1947676)
Peter S. Dragovich (1947655)
Peter Crackett (1577431)
Peter Gribling (1947634)
Peter Hewitt (1947628)
Philippe Bergeron (1443877)
Raman Narukulla (8829)
Rebecca Pulk (1947646)
Richard Bull (1947649)
Rohan Mendonca (1947673)
Savita Ubhayakar (1947682)
Scott Savage (1702459)
Sharada Labadie (1947658)
Simon Gaines (1508116)
Stefan Gradl (1947637)
Steven Shia (1947469)
Stuart I. Ward (1947667)
Tony Johnson (1947625)
Wade S. Blair (235574)
Wyne P. Lee (1947661)
Yisong Xiao (1845745)
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Herein we report on the structure-based discovery of a C-2 hydroxyethyl moiety which provided consistently high levels of selectivity for JAK1 over JAK2 to the imidazopyrrolopyridine series of JAK1 inhibitors. X-ray structures of a C-2 hydroxyethyl analogue in complex with both JAK1 and JAK2 revealed differential ligand/protein interactions between the two isoforms and offered an explanation for the observed selectivity. Analysis of historical data from related molecules was used to develop a set of physicochemical compound design parameters to impart desirable properties such as acceptable membrane permeability, potent whole blood activity, and a high degree of metabolic stability. This work culminated in the identification of a highly JAK1 selective compound (31) exhibiting favorable oral bioavailability across a range of preclinical species and robust efficacy in a rat CIA model

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