Synthesis and biological evaluation of phenyl piperidine derivatives as CCR2 antagonists |
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| Authors: | Xia Mingde Hou Cuifen Pollack Scott Brackley James DeMong Duane Pan Meng Singer Monica Matheis Michele Olini Gil Cavender Druie Wachter Michael |
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| Affiliation: | Drug Discovery, Johnson & Johnson Pharmaceutical Research and Development, LLC, 8 Clarke Drive, Cranbury, NJ 08512, USA. mxia@prdus.jnj.com |
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| Abstract: | A series of phenyl piperidine derivatives possessing potent and selective CCR2 antagonist activity is reported. Structure-activity relationship (SAR) studies have established that incorporation of a second ring system adjacent to the aryl piperidine plays an important role in determining the CCR2 potency. Both a second piperidine ring and a 1,3-substituted cyclopentylamine have been probed as linkers. For the cyclopentylamine series, the 1S,3R-configuration exhibits much higher affinity for hCCR2 than the 1R,3S-configuration. Compound 3g shows good selectivity over CCR1, CCR3, 5-HT and has an excellent P450 profile. |
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