David A. Favor
Pfizer
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Publication
Featured researches published by David A. Favor.
Bioorganic & Medicinal Chemistry Letters | 2011
Douglas S. Johnson; Chung Choi; Lorraine Kathleen Fay; David A. Favor; Joseph Thomas Repine; Andrew David White; Hyacinth Akunne; Lawrence W. Fitzgerald; Kim Nicholls; Bradley Snyder; Steven Z. Whetzel; Liming Zhang; Kevin A. Serpa
The synthesis and structure-activity relationship (SAR) of a novel series of aryl piperazine napthyridinone D(2) partial agonists is described. Our goal was to optimize the affinities for the D(2), 5-HT(2A) and 5-HT(1A) receptors, such that the D(2)/5-HT(2A) ratio was greater than 5 to ensure maximal occupancy of these receptors when the D(2) occupancy reached efficacious levels. This strategy led to identification of PF-00217830 (2) with robust inhibition of sLMA (MED=0.3mg/kg) and DOI-induced head twitches in rats (31% and 78% at 0.3 and 1mg/kg) with no catalepsy observed at the highest dose tested (10 mg/kg).
Bioorganic & Medicinal Chemistry Letters | 2013
Alan Daniel Brown; David Ellis; David A. Favor; Tony Kirkup; Wolfgang Klute; Malcolm MacKenny; Gordon McMurray; Adam Stennett
A new series of 2-(benzyloxy)benzamides are presented that are potent functional antagonists of TRPM8 and possess improved LipE and LE compared to the original lead. They were discovered through a series of compound libraries and we present a powerful visualization method for the chemical space explored with each library. Remarkably this new series originated from the highest risk design strategy where compounds were synthesised with the least degree of similarity to the lead structure.
Bioorganic & Medicinal Chemistry Letters | 2011
Lee R. Roberts; Duncan Armor; Carolyn M. Barker; Andrew Bent; Kirstin Bess; Alan Daniel Brown; David A. Favor; David Ellis; Stephen L. Irving; Malcolm MacKenny; Christopher Phillips; Nick Pullen; Adam Stennett; Linda Strand; Michelle Leanne Styles
A series of p-hydroxybenzenesulphonamides ERβ receptor agonists were discovered and several compounds identified had excellent selectivity over the related ERα receptor. One of these, compound 11, had an interesting binding conformation determined by X-ray and represents an excellent starting point in the quest for further selective ERβ agonists.
Bioorganic & Medicinal Chemistry Letters | 2010
David A. Favor; James J. Powers; Andrew David White; Lawrence W. Fitzgerald; Vincent E. Groppi; Kevin A. Serpa
A series of 6-alkoxyisoindolin-1-ones with a magic shotgun pharmacological profile are presented as potential antipsychotics. The in vitro pharmacological profile includes D(2) partial agonism (30-55%), 5-HT(1A) partial agonism (60-90%), and 5-HT(2A) antagonism. Selected compounds in this series displayed good in vivo activity and potency.
Archive | 2004
Jerry D. Clark; Jamie M. Davis; David A. Favor; Lorraine Kathleen Fay; Lloyd Franklin; Kevin Henegar; Douglas S. Johnson; Brian Nichelson; Ligong Ou; Joseph Thomas Repine; Michael Walters; Andrew David White; Zhijian Zhu
Tetrahedron Letters | 2007
David A. Favor; Douglas S. Johnson; James J. Powers; Tingsheng Li; Rambabu Madabattula
Archive | 2006
David A. Favor; Douglas S. Johnson; Joseph Thomas Repine; Andrew David White
Tetrahedron Letters | 2007
Joseph Thomas Repine; Douglas S. Johnson; Andrew David White; David A. Favor; Michael Andrew Stier; Judy Yip; Trent Rankin; Qizhu Ding; Samarendra N. Maiti
Tetrahedron Letters | 2009
James J. Powers; David A. Favor; Trent Rankin; Rashmi Sharma; Chetan Pandit; Azhwarsamy Jeganathan; Samarendra N. Maiti
Bioorganic & Medicinal Chemistry Letters | 2017
Gregory R. Ott; David A. Favor
