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Literature DB >> 24900329

Discovery of INCB3284, a Potent, Selective, and Orally Bioavailable hCCR2 Antagonist.

Chu-Biao Xue¹, Hao Feng¹, Ganfeng Cao¹, Taisheng Huang¹, Joseph Glenn¹, Rajan Anand¹, David Meloni¹, Ke Zhang¹, Lingquan Kong¹, Anlai Wang¹, Yingxin Zhang¹, Changsheng Zheng¹, Michael Xia¹, Lihua Chen¹, Hiroyuki Tanaka¹, Qi Han¹, D J Robinson¹, Dilip Modi¹, Lou Storace¹, Lixin Shao¹, Vaqar Sharief¹, Mei Li¹, Laurine G Galya¹, Maryanne Covington¹, Peggy Scherle¹, Sharon Diamond¹, Tom Emm¹, Swamy Yeleswaram¹, Nancy Contel¹, Kris Vaddi¹, Robert Newton¹, Greg Hollis¹, Steven Friedman¹, Brian Metcalf¹.

Abstract

We report the identification of 13 (INCB3284) as a potent human CCR2 (hCCR2) antagonist. INCB3284 exhibited an IC50 of 3.7 nM in antagonism of monocyte chemoattractant protein-1 binding to hCCR2, an IC50 of 4.7 nM in antagonism of chemotaxis activity, an IC50 of 84 μM in inhibition of the hERG potassium current, a free fraction of 58% in protein binding, high selectivity over other chemokine receptors and G-protein-coupled receptors, and acceptable oral bioavailability in rodents and primates. In human clinical trials, INCB3284 exhibited a pharmacokinetic profile suitable for once-a-day dosing (T 1/2 = 15 h).

Entities: Chemical Gene Species

Keywords: CCR2; antagonist; chemokine; hERG; oral absorption

Year: 2011 PMID： 24900329 PMCID： PMC4018154 DOI： 10.1021/ml200030q

Source DB: PubMed Journal: ACS Med Chem Lett ISSN： 1948-5875 Impact factor: 4.345

10 in total

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