Jerry Andrew Taylor
Merck & Co.
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Publication
Featured researches published by Jerry Andrew Taylor.
Journal of Medicinal Chemistry | 2009
Jeffrey Bagdanoff; Michael S. Donoviel; Amr Nouraldeen; James Tarver; Qinghong Fu; Marianne Carlsen; Theodore C. Jessop; Haiming Zhang; Jill Hazelwood; Huy H. Nguyen; Simon D.P. Baugh; Michael Gardyan; Kristen M. Terranova; Joseph Barbosa; Jack Yan; Mark S. Bednarz; Suman Layek; Lawrence F. Courtney; Jerry Andrew Taylor; Ann Marie Digeorge-Foushee; Suma Gopinathan; Debra Bruce; Traci Smith; Liam Moran; Emily O’Neill; Jeffrey A. Kramer; Zhong Lai; S. David Kimball; Qingyun Liu; Weimei Sun
During nearly a decade of research dedicated to the study of sphingosine signaling pathways, we identified sphingosine-1-phosphate lyase (S1PL) as a drug target for the treatment of autoimmune disorders. S1PL catalyzes the irreversible decomposition of sphingosine-1-phosphate (S1P) by a retro-aldol fragmentation that yields hexadecanaldehyde and phosphoethanolamine. Genetic models demonstrated that mice expressing reduced S1PL activity had decreased numbers of circulating lymphocytes due to altered lymphocyte trafficking, which prevented disease development in multiple models of autoimmune disease. Mechanistic studies of lymphoid tissue following oral administration of 2-acetyl-4(5)-(1(R),2(S),3(R),4-tetrahydroxybutyl)-imidazole (THI) 3 showed a clear relationship between reduced lyase activity, elevated S1P levels, and lower levels of circulating lymphocytes. Our internal medicinal chemistry efforts discovered potent analogues of 3 bearing heterocycles as chemical equivalents of the pendant carbonyl present in the parent structure. Reduction of S1PL activity by oral administration of these analogues recapitulated the phenotype of mice with genetically reduced S1PL expression.
Bioorganic & Medicinal Chemistry Letters | 2017
Amjad Ali; D. Jonathan Bennett; Jaiqiang Cai; Emma Carswell; Andrew John Cooke; Scott B. Hoyt; Michael Lo; Clare London; John Maclean; Min K. Park; Paul Ratcliffe; Jerry Andrew Taylor; Brent Whitehead; Yusheng Xiong
The inhibition of aldosterone synthase (CYP11B2) may be an effective treatment of hypertension and heart failure, among other ailments. Previously reported benzimidazole CYP11B2 inhibitors led the way for bioisosteric imidazopyridines that are both potent and selective over CYP11B1.
Bioorganic & Medicinal Chemistry Letters | 2009
Theodore C. Jessop; James Tarver; Marianne Carlsen; Amy Xu; Jason P. Healy; Alexander Heim-Riether; Qinghong Fu; Jerry Andrew Taylor; David J. Augeri; Min Shen; Terry R. Stouch; Ronald V. Swanson; Leslie W. Tari; Isaac D. Hoffman; Philip E. Keyes; Xuan Chuan Yu; Maricar Miranda; Qingyun Liu; Jonathan Swaffield; S. David Kimball; Amr Nouraldeen; Alan Wilson; Ann Marie DiGeorge Foushee; Kanchan Jhaver; Rick A. Finch; Steve Anderson; Tamas Oravecz; Kenneth G. Carson
A series of deoxycytidine kinase inhibitors was simultaneously optimized for potency and PK properties. A co-crystal structure then allowed merging this series with a high throughput screening hit to afford a highly potent, selective and orally bioavailable inhibitor, compound 10. This compound showed dose dependent inhibition of deoxycytidine kinase in vivo.
Bioorganic & Medicinal Chemistry Letters | 2009
James Tarver; Theodore C. Jessop; Marianne Carlsen; David J. Augeri; Qinghong Fu; Jason P. Healy; Alexander Heim-Riether; Amy Xu; Jerry Andrew Taylor; Min Shen; Philip E. Keyes; S. David Kimball; Xuan Chuan Yu; Maricar Miranda; Qingyun Liu; Jonathan Swaffield; Amr Nouraldeen; Alan Wilson; Rick A. Finch; Kanchan Jhaver; Ann Marie DiGeorge Foushee; Steve Anderson; Tamas Oravecz; Kenneth G. Carson
A series of potent piperidine-linked cytosine derivatives were prepared as inhibitors of deoxycytidine kinase (dCK). Compound 9h was discovered to be a potent inhibitor of dCK and shows a good combination of cellular potency and pharmacokinetic parameters. Compound 9h blocks the incorporation of radiolabeled cytosine into mouse T-cells in vitro, as well as in vivo in mice following a T-cell challenge.
Bioorganic & Medicinal Chemistry Letters | 2017
Scott B. Hoyt; Jerry Andrew Taylor; Clare London; Amjad Ali; Feroze Ujjainwalla; Jim Tata; Mary Struthers; Doris F. Cully; Tom Wisniewski; Ning Ren; Charlene Bopp; Andrea Sok; Andreas Verras; Daniel R. McMasters; Qing Chen; Elaine Tung; Wei Tang; Gino Salituro; Joe Clemas; Gaochao Zhou; Douglas J. MacNeil; Ruth Duffy; Yusheng Xiong
We report the discovery and hit-to-lead optimization of a structurally novel indazole series of CYP11B2 inhibitors. Benchmark compound 34 from this series displays potent inhibition of CYP11B2, high selectivity versus related steroidal and hepatic CYP targets, and lead-like physical and pharmacokinetic properties. On the basis of these and other data, the indazole series was progressed to lead optimization for further refinement.
ACS Medicinal Chemistry Letters | 2013
Scott B. Hoyt; Whitney Lane Petrilli; Clare London; Yusheng Xiong; Jerry Andrew Taylor; Amjad Ali; Michael Man-Chu Lo; Timothy J. Henderson; Qingzhong Hu; Rolf Hartmann; Lina Yin; Ralf Heim; Emmanuel Bey; Rohit Saxena; Swapan Kumar Samanta; Bheemashankar A. Kulkarni
Archive | 2007
David J. Augeri; Marianne Carlsen; Kenneth G. Carson; Qinghong Fu; Jason P. Healy; Alexander Heim-Riether; Theodore C. Jessop; Philip E. Keyes; Min Shen; James Tarver; Jerry Andrew Taylor; Xiaolian Xu
Archive | 2007
David J. Augeri; Marianne Carlsen; Kenneth G. Carson; Qinghong Fu; Alexander Heim-Riether; Theodore C. Jessop; James E. Tarver; Jerry Andrew Taylor
Archive | 2007
David J. Augeri; Marianne Carlsen; Kenneth G. Carson; Qinghong Fu; Jason P. Healy; Alexander Heim-Riether; Theodore C. Jessop; Philip E. Keyes; Min Shen; James E. Tarver; Jerry Andrew Taylor; Xiaolian Xu
Archive | 2014
Scott B. Hoyt; Jerry Andrew Taylor; Clare London; Yusheng Xiong; Andrew John Cooke
