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Dive into the research topics where Lorraine Kathleen Fay is active.

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Featured researches published by Lorraine Kathleen Fay.


Bioorganic & Medicinal Chemistry Letters | 2009

Benzothiophene piperazine and piperidine urea inhibitors of fatty acid amide hydrolase (FAAH)

Douglas S. Johnson; Kay Ahn; Suzanne Ross Kesten; Scott E. Lazerwith; Yuntao Song; Mark Morris; Lorraine Kathleen Fay; Tracy Fay Gregory; Cory Michael Stiff; James B. Dunbar; Marya Liimatta; David Beidler; Sarah E. Smith; Tyzoon K. Nomanbhoy; Benjamin F. Cravatt

The synthesis and structure-activity relationships (SAR) of a series of benzothiophene piperazine and piperidine urea FAAH inhibitors is described. These compounds inhibit FAAH by covalently modifying the enzymes active site serine nucleophile. Activity-based protein profiling (ABPP) revealed that these urea inhibitors were completely selective for FAAH relative to other mammalian serine hydrolases. Several compounds showed in vivo activity in a rat complete Freunds adjuvant (CFA) model of inflammatory pain.


Bioorganic & Medicinal Chemistry Letters | 2011

Discovery of PF-00217830: Aryl piperazine napthyridinones as D2 partial agonists for schizophrenia and bipolar disorder

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).


ACS Medicinal Chemistry Letters | 2011

Discovery of PF-04457845: A Highly Potent, Orally Bioavailable, and Selective Urea FAAH Inhibitor.

Douglas S. Johnson; Cory Michael Stiff; Scott E. Lazerwith; Suzanne Ross Kesten; Lorraine Kathleen Fay; Mark Morris; David Beidler; Marya Liimatta; Sarah E. Smith; David T. Dudley; Nalini Sadagopan; Shobha N. Bhattachar; Stephen J. Kesten; Tyzoon K. Nomanbhoy; Benjamin F. Cravatt; Kay Ahn


Archive | 2004

[1,8]naphthyridin-2-ones and related compounds for the treatment of schizophrenia

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


Archive | 2007

Biaryl ether urea compounds

Lorraine Kathleen Fay; Douglas S. Johnson; Suzanne Ross Kesten; Scott E. Lazerwith; Mark Anthony Morris; Cory Michael Stiff; Marvin Jay Meyers; Lijuan Jane Wang


Archive | 2009

ETHER BENZYLIDENE PIPERIDINE 5-MEMBERED ARYL CARBOXAMIDE COMPOUNDS USEFUL AS FAAH INHIBITORS

Lorraine Kathleen Fay; Douglas S. Johnson; Marvin Jay Meyers; Barbara Ann Schweitzer; Atli Thorarensen; Lijuan Jane Wang


Archive | 2009

ETHER BENZYLIDENE PIPERIDINE ARYL CARBOXAMIDE COMPOUNDS USEFUL AS FAAH INHIBITORS

Lorraine Kathleen Fay; Douglas S. Johnson; Marvin Jay Meyers; Atli Thorarensen; Lijuan Jane Wang


Archive | 2009

Ether benzylidene piperidine aryl carboxamide compounds

Lorraine Kathleen Fay; Douglas S. Johnson; Marvin Jay Meyers; Atli Thorarensen; Lijuan Jane Wang


Archive | 2009

Composés d'éther-benzylidène-pipéridine-aryl-carboxamide utiles comme inhibiteurs de faah

Lorraine Kathleen Fay; Douglas S. Johnson; Marvin Jay Meyers; Atli Thorarensen; Lijuan Jane Wang


Archive | 2009

Composés d'éther-benzylidène-pipéridine-aryl à 5 chaînons-carboxamide utiles comme inhibiteurs de faah

Lorraine Kathleen Fay; Douglas S. Johnson; Marvin Jay Meyers; Barbara Ann Schweitzer; Atli Thorarensen; Lijuan Jane Wang

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