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Dive into the research topics where Wendy Eccles is active.

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Featured researches published by Wendy Eccles.


Bioorganic & Medicinal Chemistry Letters | 2013

Identification of benzofuran central cores for the inhibition of leukotriene A 4 hydrolase

Wendy Eccles; Jonathan M. Blevitt; Jamila N. Booker; Christa C. Chrovian; Shelby Crawford; Aimee Rose de Leon; Xiaohu Deng; Anne Fourie; Cheryl A. Grice; Krystal Herman; Lars Karlsson; Aaron M. Kearney; Alice Lee-Dutra; Jimmy T. Liang; Rosa Luna; Dan Pippel; Navin Rao; Jason P. Riley; Alejandro Santillan; Virginia M. Tanis; Xiaohua Xue; Arlene L. Young

Leukotrienes (LTs) are known to play a physiological role in inflammatory immune response. Leukotriene A(4) hydrolase (LTA(4)H) is a cystolic enzyme that stereospecifically catalyzes the transformation of LTA(4) to LTB(4). LTB(4) is a known pro-inflammatory mediator. This paper describes the identification and synthesis of substituted benzofurans as LTH(4)H inhibitors. The benzofuran series demonstrated reduced mouse and human whole blood LTB(4) levels in vitro and led to the identification one analog for advanced profiling. Benzofuran 28 showed dose responsive target engagement and provides a useful tool to explore a LTA(4)H inhibitor for the treatment of inflammatory diseases, such as asthma and inflammatory bowel disease (IBD).


Journal of Biomolecular Screening | 2016

Polypharmacology of Small-Molecule Modulators of the 5-Lipoxygenase Activating Protein (FLAP) Observed via a High-throughput Lipidomics Platform

Jiao Song; Xuejun Liu; Jian Zhu; Mandana Tootoonchi; John M. Keith; Steven P. Meduna; Curt A. Dvorak; Wendy Eccles; Paul J. Krawczuk; Jonathan M. Blevitt; Jiejun Wu; Navin Rao; Alec D. Lebsack; Marcos E. Milla

Leukotrienes (LTs) and related species are proinflammatory lipid mediators derived from arachidonic acid (AA) that have pathological roles in autoimmune and inflammatory conditions, cardiovascular diseases, and cancer. 5-Lipoxygenase activating protein (FLAP) plays a critical accessory role in the conversion of AA to LTA4, and its subsequent conversion to LTC4 by LTC4 synthase. Pharmacological inhibition of FLAP results in a loss of LT production by preventing the biosynthesis of both LTB4 and LTC4, making it an attractive target for the treatment of inflammatory diseases in which LTs likely play a role. Small-molecule (SM) drugs often exhibit polypharmacology through various pathways, which may explain the differential therapeutic efficacies of compounds sharing structural similarity. We have profiled a series of SM FLAP modulators for their selectivity across enzymes of AA cascade in human whole blood (HWB), using a recently developed LC/MS (liquid chromatography–mass spectrometry)-based high-throughput lipidomics platform that monitors 122 eicosanoids in multiplex. Highly efficient data acquisition coupled with fast and accurate data analysis allowed facile compound profiling from ex vivo study samples. This platform allowed us to quantitatively map the effects of those SMs on the entire AA cascade, demonstrating its potential to discriminate structurally related compounds.


Archive | 2008

Aryl-substituted bridged or fused diamines as modulators of leukotriene A4 hydrolase

Genesis M. Bacani; Scott D. Bembenek; Wendy Eccles; James P. Edwards; Matthew T. Epperson; Laurent Gomez; Cheryl A. Grice; Aaron M. Kearney; Adrienne M. Landry-Bayle; Alice Lee-Dutra; Kelly J. Mcclure; Taraneh Mirzadegan; Alejandro Santillan


Archive | 2014

1,2,6-SUBSTITUTED BENZIMIDAZOLES AS FLAP MODULATORS

Wenying Chai; Curt A. Dvorak; Wendy Eccles; James P. Edwards; Steven Goldberg; Paul J. Krawczuk; Alec D. Lebsack; Jing Liu; Daniel J. Pippel; Zachary S. Sales; Virginia M. Tanis; Mark S. Tichenor; John J.M. Wiener


Archive | 2017

COMPUESTOS DERIVADOS DE HETEROARILO Y HETEROCICLO CONDENSADOS

Russell C. Smith; William M. Jones; Alec D. Lebsack; Wendy Eccles; John M. Keith; Steven P. Meduna; Wenying Chai; Scott D. Bembenek; Jennifer D. Venable; Jianyang Weng; Zhulin Zhang; Hong Jia; Guangxiu Dai; Weiguo Su


Archive | 2017

FLAP MODULATORS FLAP

Genesis M. Bacani; Wendy Eccles; Anne E. Fitzgerald; Steven Goldberg; Michael D. Hack; Natalie A. Hawryluk; William M. Jones; John M. Keith; Paul J. Krawczuk; Alec D. Lebsack; Alice Lee-Dutra; Jing Liu; Kelly J. Mcclure; Steven P. Meduna; Daniel J. Pippel; Mark D. Rosen; Zachary S. Sales


Archive | 2014

COMPUESTOS SUSTITUIDOS COMO MODULADORES DE LA PRO TEÍNA DE ACTIVACIÓN DE LA 5-LIPOXIGENASA (FLAP)

Wendy Eccles; Fitzgerald Anne E; Hack Michael D; Hawyrluk Natalie A; Jones William M; Keith John M; Paul J. Krawczuk; Lebsack Alec D; Jing Liu; Mani Neelakandha S; Mcclure Kelly J; Meduna Steven P; Rosen Mark D


Archive | 2010

COMPUESTOS CON DOS PORCIONES HETEROARILO BICÍCLICAS FUSIONADAS COMO MODULADORES DE LA HIDROLASA DE LEUCOTRIENO A4

Wendy Eccles; Grice Cheryl A; Kearney Aaron M; Landry-Bayle Adrienne M; Lee-Dutra Alice; Genesis M. Bacani; Chrovian Crhista C; Fourie Anne M; Gomez Laurent; Jr Alejandro Santillan; Tanis Virginia M; Wiener John J M


Archive | 2010

Verbindungen mit zwei bicyclischen heteroarylderivaten als modulatoren von leukotrien-a4-hydrolase

Genesis M. Bacani; Christa C. Chrovian; Wendy Eccles; Anne M. Fourie; Laurent Gomez; Cheryl A. Grice; Aaron M. Kearney; Adrienne M. Landry-Bayle; Alice Lee-Dutra; Alejandro Santillan; Virginia M. Tanis; John J. M. Wiener


Archive | 2010

Verbindungen mit zwei kondensierten bicyclischen heteroarylteilen als modulatoren der leukotrien-a4-hydrolase

Genesis M. Bacani; Christa C. Chrovian; Wendy Eccles; Anne M. Fourie; Laurent Gomez; Cheryl A. Grice; Aaron M. Kearney; Adrienne M. Landry-Bayle; Alice Lee-Dutra; Alejandro Santillan; Virginia M. Tanis; John J. M. Wiener

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