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Optimization of the physicochemical and pharmacokinetic attributes in a 6-azauracil series of P2X7 receptor antagonists leading to the discovery of the clinical candidate CE-224,535 |
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| Authors: | Duplantier Allen J Dombroski Mark A Subramanyam Chakrapani Beaulieu Aimee M Chang Shang-Poa Gabel Christopher A Jordan Crystal Kalgutkar Amit S Kraus Kenneth G Labasi Jeff M Mussari Christopher Perregaux David G Shepard Rick Taylor Timothy J Trevena Kristen A Whitney-Pickett Carrie Yoon Kwansik |
| Affiliation: | Pfizer Global Research and Development, Groton Laboratories, Eastern Point Road, Groton, CT 06340, USA |
| Abstract: | High throughput screening (HTS) of our compound file provided an attractive lead compound with modest P2X7 receptor antagonist potency and high selectivity against a panel of receptors and channels, but also with high human plasma protein binding and a predicted short half-life in humans. Multi-parameter optimization was used to address the potency, physicochemical and pharmacokinetic properties which led to potent P2X7R antagonists with good disposition properties. Compound 33 (CE-224,535) was advanced to clinical studies for the treatment of rheumatoid arthritis. |
| Keywords: | P2X7 Antagonist Rheumatoid arthritis 6-Azauracil Pharmacokinetic Log P |
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