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Discovery of BMS-753426: A Potent Orally Bioavailable Antagonist of CC Chemokine Receptor 2 |
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| Authors: | Michael G. Yang Zili Xiao Rulin Zhao Andrew J. Tebben Bei Wang Robert J. Cherney Douglas G. Batt Gregory D. Brown Mary Ellen Cvijic John V. Duncia Michael A. Gallela Daniel S. Gardner Purnima Khandelwal Mary F. Malley Jian Pang Anne V. Rose Joseph B. Santella III Amy A. Sarjeant Songmei Xu Arvind Mathur Sandhya Mandlekar Ragini Vuppugalla Qihong Zhao Percy H. Carter |
| Affiliation: | Research and Development, Bristol Myers Squibb Company, Princeton, New Jersey 08543-4000, United States |
| Abstract: | To improve the metabolic stability profile of BMS-741672 (1a), we undertook a structure–activity relationship study in our trisubstituted cyclohexylamine series. This ultimately led to the identification of 2d (BMS-753426) as a potent and orally bioavailable antagonist of CCR2. Compared to previous clinical candidate 1a, the tert-butyl amine 2d showed significant improvements in pharmacokinetic properties, with lower clearance and higher oral bioavailability. Furthermore, compound 2d exhibited improved affinity for CCR5 and good activity in models of both monocyte migration and multiple sclerosis in the hCCR2 knock-in mouse. The synthesis of 2d was facilitated by the development of a simplified approach to key intermediate (4R)-9b that deployed a stereoselective reductive amination which may prove to be of general interest. |
| Keywords: | CC chemokine receptor 2 (CCR2) CCR2 antagonist Monocyte chemoattractant protein-1 Multiple sclerosis |