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Discovery of Novel and Potent Leukotriene B4 Receptor Antagonists. Part 1

Authors :: Tina Molinaro
Robert Alan Goodnow
Louis M. Renzetti
Alexandra Hicks
Satish Choudhry
Xin Wei
Gesine J. Hermann
Qi Qiao
Anjula Pamidimukkala
A. Robert Catala
Maureen Hargaden
Jian Ping Lou
Nadine Tare
John O’Neil
Ueli Gubler
Karen Pozzani
David J Moore
Jennifer Santiago
Ruben Marcano
Paul Gillespie
Rachid Hamid
Noal Cohen
Hyesun Oh
Lisa C. F. Chao
Laura Singer
Jefferson Wright Tilley
Romyr Dominique
Grazyna Kurylko
Ying L. Li
Radhika Venkat
Achyutharao Sidduri
Matthew Blake Wright
Ann F. Hoffman
Shahid Tannu
Gary Cavallo
Nader Fotouhi
Thomas Egan
Martin Lamb
Jessica D. Ventre
Agnieszka Kowalczyk
D Lavelle
Helena Mancebo
Source :: Journal of Medicinal Chemistry. 53:3502-3516
Publication Year :: 2010
Publisher :: American Chemical Society (ACS), 2010.
Abstract: The inhibition of LTB(4) binding to and activation of G-protein-coupled receptors BLT1 and BLT2 is the premise of a treatment for several inflammatory diseases. In a lead optimization effort starting with the leukotriene B(4) (LTB(4)) receptor antagonist (2), members of a series of 3,5-diarylphenyl ethers were found to be highly potent inhibitors of LTB(4) binding to BLT1 and BLT2 receptors, with varying levels of selectivity depending on the substitution. In addition, compounds 33 and 38 from this series have good in vitro ADME properties, good oral bioavailability, and efficacy after oral delivery in guinea pig LTB(4) and nonhuman primate allergen challenge models. Further profiling in a rat non-GLP toxicity experiment provided the rationale for differentiation and selection of one compound (33) for clinical development.