Discovery of Bioavailable 4,4-Disubstituted Piperidines as Potent Ligands of the Chemokine Receptor 5 and Inhibitors of the Human Immunodeficiency Virus-1

被引:32
|
作者
Kazmierski, Wieslaw M. [1 ]
Aquino, Christopher [6 ]
Chauder, Brian A. [6 ]
Deanda, Felix [3 ]
Ferris, Robert [1 ]
Jones-Hertzog, Deborah K. [4 ]
Kenakin, Terrence [2 ]
Koble, Cecilia S. [6 ]
Watson, Christian [2 ]
Wheelan, Pat [5 ]
Yang, Hanbiao
Youngman, Michael [1 ]
机构
[1] GlaxoSmithKline Inc, Infect Dis Ctr Excellence Drug Discovery, Res Triangle Pk, NC 27709 USA
[2] GlaxoSmithKline Inc, Mol Discovery Res, Res Triangle Pk, NC 27709 USA
[3] GlaxoSmithKline Inc, Computat & Struct Chem, Res Triangle Pk, NC 27709 USA
[4] GlaxoSmithKline Inc, Drug Discovery IT, Res Triangle Pk, NC 27709 USA
[5] GlaxoSmithKline Inc, ID DMPK, Res Triangle Pk, NC 27709 USA
[6] GlaxoSmithKline Inc, Metab Pathways Ctr Excellence Drug Discovery, Res Triangle Pk, NC 27709 USA
来源
JOURNAL OF MEDICINAL CHEMISTRY | 2008年 / 51卷 / 20期
关键词
D O I
10.1021/jm800598a
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
We describe robust chemical approaches toward putative CCR5 scaffolds designed in our laboratories. Evaluation of analogues in the (125)I-[MIP-1 beta] binding and Ba-L-HOS antiviral assays resulted in the discovery of 64 and 68 in the 4,4-disubstitited piperidine class H, both potent CCR5 ligands (pIC(50) = 8.30 and 9.00, respectively) and HIV-1 inhibitors (pIC(50) = 7.80 and 7.84, respectively, in Ba-L-HOS assay). In addition, 64 and 68 were bioavailable in rodents, establishing them as lead molecules for further optimization toward CCR5 clinical candidates.
引用
收藏
页码:6538 / 6546
页数:9
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