James T. Rider
Amgen
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Publication
Featured researches published by James T. Rider.
Bioorganic & Medicinal Chemistry Letters | 2010
Qingping Zeng; Matthew P. Bourbeau; G. Erich Wohlhieter; Guomin Yao; Holger Monenschein; James T. Rider; Matthew R. Lee; Shiwen Zhang; Julie A. Lofgren; Daniel J. Freeman; Chun Li; Elizabeth Tominey; Xin Huang; Douglas Hoffman; Harvey Yamane; Andrew Tasker; Celia Dominguez; Vellarkad N. Viswanadhan; Randall W. Hungate; Xiaoling Zhang
A series of 2-aminothiadiazole of inhibitors of AKT1 is described. SAR relationships are discussed, along with selectivity for protein kinase A (PKA) and cyclin-dependent kinase 2 (CDK2). Moderate selectivity observed in several compounds for AKT1 versus PKA is rationalized by X-ray crystallographic analysis. Key compounds showed activity in cellular assays measuring phosphorylation of two AKT substrates, PRAS40 and FKHRL1. Compound 30 was advanced to a mouse liver PD assay, where it showed dose-dependent inhibition of AKT activity, as measured by the inhibition of phospho-PRAS40.
Bioorganic & Medicinal Chemistry Letters | 2010
Qingping Zeng; John G. Allen; Matthew P. Bourbeau; Xianghong Wang; Guomin Yao; Seifu Tadesse; James T. Rider; Chester Chenguang Yuan; Fang-Tsao Hong; Matthew R. Lee; Shiwen Zhang; Julie A. Lofgren; Daniel J. Freeman; Suijin Yang; Chun Li; Elizabeth Tominey; Xin Huang; Douglas Hoffman; Harvey Yamane; Christopher Fotsch; Celia Dominguez; Randall W. Hungate; Xiaoling Zhang
Through a combination of screening and structure-based rational design, we have discovered a series of N(1)-(5-(heterocyclyl)-thiazol-2-yl)-3-(4-trifluoromethylphenyl)-1,2-propanediamines that were developed into potent ATP competitive inhibitors of AKT. Studies of linker strand-binding adenine isosteres identified SAR trends in potency and selectivity that were consistent with binding interactions observed in structures of the inhibitors bound to AKT1 and to the counter-screening target PKA. One compound was shown to have acceptable pharmacokinetic properties and to be a potent inhibitor of AKT signaling and of in vivo xenograft tumor growth in a preclinical model of glioblastoma.
Organic Letters | 2006
Matthew P. Bourbeau and; James T. Rider
Archive | 2008
Qingping Zeng; Dawei Zhang; Guomin Yao; George E. Wohlhieter; Xianghong Wang; James T. Rider; Andreas Reichelt; Holger Monenschein; Fang-Tsao Hong; James Richard Falsey; Celia Dominguez; Matthew P. Bourbeau; John G. Allen
Archive | 2005
Qingping Zeng; Guomin Yao; George E. Wohlhieter; Vellarkad N. Viswanadhan; Andrew Tasker; James T. Rider; Holger Monenschein; Celia Dominguez; Matthew P. Bourbeau
Archive | 2007
Qingping Zeng; John G. Allen; Matthew P. Bourbeau; Celia Dominguez; Christopher Fotsch; Nianhe Han; Fang-Tsao Hong; Xin Huang; Matthew R. Lee; Aiwen Li; Qingyian Liu; James T. Rider; Seifu Tadesse; Andrew Tasker; Vellarkad N. Viswanadhan; Xianghong Wang; Kurt E. Weiler; George Eric Wohlhieter; Guomin Yao; Chester Chenguang Yuan
Archive | 2008
Qingping Zeng; Dawei Zhang; Guomin Yao; George E. Wohlhieter; Xianghong Wang; James T. Rider; Andreas Reichelt; Holger Monenschein; Fang-Tsao Hong; James Richard Falsey; Celia Dominguez; Matthew P. Bourbeau; John G. Allen
Archive | 2007
Qingping Zeng; John G. Allen; Matthew P. Bourbeau; Celia Dominguez; Christopher Fotsch; Nianhe Han; Fang-Tsao Hong; Xin Huang; Matthew R. Lee; Aiwen Li; Qingyian Liu; James T. Rider; Seifu Tadesse; Andrew Tasker; Vellarkad N. Viswanadhan; Xianghong Wang; Kurt E. Weiler; George E. Wohlhieter; Guomin Yao; Chester Chenguang Yuan
Archive | 2007
Qingping Zeng; John G. Allen; Matthew P. Bourbeau; Celia Dominguez; Christopher Fotsch; Nianhe Han; Fang-Tsao Hong; Xin Huang; Matthew R. Lee; Aiwen Li; Qingyian Liu; James T. Rider; Seifu Tadesse; Andrew Tasker; Vellarkad N. Viswanadhan; Xianghong Wang; Kurt E. Weiler; George E. Wohlhieter; Guomin Yao; Chester Chenguang Yuan
Archive | 2005
Qingping Zeng; Guomin Yao; George E. Wohlhieter; Vellarkad N. Viswanadhan; Andrew Tasker; James T. Rider; Holger Monenschein; Celia Dominguez; Matthew P. Bourbeau