Synthetic and Structure/Activity Studies on Acid-Substituted 2-Arylphenols: Discovery of 2-[2-Propyl-3-[3-[2-ethyl-4-(4-fluorophenyl)-5-hydroxyphenoxy]- propoxy]phenoxy]benzoic Acid, a High-Affinity Leukotriene B4 Receptor Antagonist

Structural derivatives of LY255283 have been studied as receptor antagonists of leukotriene B4. Substitution of the 2-hydroxyacetophenone subunit of 1 (LY255283) with a 2-arylphenol group provided entry into several new series that feature various mono- and diacidic core functionality. These new ana...

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Published in	Journal of medicinal chemistry Vol. 38; no. 22; pp. 4411 - 4432
Main Authors	Sawyer, J. Scott, Bach, Nicholas J, Baker, S. Richard, Baldwin, Ronald F, Borromeo, Peter S, Cockerham, Sandra L, Fleisch, Jerome H, Floreancig, Paul, Froelich, Larry L
Format	Journal Article
Language	English
Published	United States American Chemical Society 01.10.1995
Subjects	Airway Obstruction - metabolism Animals Benzoates - chemical synthesis Benzoates - chemistry Benzoates - pharmacology Guinea Pigs Humans Leukotriene B4 - antagonists & inhibitors Leukotriene B4 - pharmacology Lung - drug effects Lung - metabolism Neutrophils - drug effects Neutrophils - metabolism Phenols - chemical synthesis Phenols - chemistry Phenols - pharmacology Receptors, Leukotriene B4 - antagonists & inhibitors Structure-Activity Relationship Tetrazoles - chemistry Tetrazoles - pharmacology
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Abstract	Structural derivatives of LY255283 have been studied as receptor antagonists of leukotriene B4. Substitution of the 2-hydroxyacetophenone subunit of 1 (LY255283) with a 2-arylphenol group provided entry into several new series that feature various mono- and diacidic core functionality. These new analogues, the subject of a broad structure-activity investigation, displayed significantly increased in vitro and in vivo activity as receptor antagonists of LTB4. A series of diaryl ether carboxylic acids demonstrated especially interesting activity and led to the discovery of compound 43b, 2-[2-propyl-3-[3-[2-ethyl-4-(4- fluorophenyl)-5-hydroxyphenoxy]-propoxy]phenoxy]benzoic acid (LY293111), a 2-arylphenol-substituted diaryl ether carboxylic acid which displayed potent binding to human neutrophils (IC50 = 17 +/- 4.6 nM) and guinea pig lung membranes (IC50 = 6.6 +/- 0.71 nM), inhibition of LTB4-induced expression of the CD11b/CD18 receptor on human neutrophils (IC50 = 3.3 +/- 0.81 nM), and inhibition of LTB4-induced contraction of guinea pig lung parenchyma (pKB = 8.7 +/- 0.16). In vivo, 43b demonstrated potent activity in inhibiting LTB4-induced airway obstruction in the guinea pig when dosed by the oral (ED50 = 0.40 mg/kg) or intravenous (ED50 = 0.014 mg/kg) routes. A specific LTB4 receptor antagonist, 43b had little effect on inhibiting contractions of guinea pig lung parenchyma induced by leukotriene D4 (LTD4), histamine, carbachol, or U46619. Compound 43b has been chosen as a clinical candidate and is currently in phase I studies for a variety of inflammatory diseases.
AbstractList	Structural derivatives of LY255283 have been studied as receptor antagonists of leukotriene B4. Substitution of the 2-hydroxyacetophenone subunit of 1 (LY255283) with a 2-arylphenol group provided entry into several new series that feature various mono- and diacidic core functionality. These new analogues, the subject of a broad structure-activity investigation, displayed significantly increased in vitro and in vivo activity as receptor antagonists of LTB4. A series of diaryl ether carboxylic acids demonstrated especially interesting activity and led to the discovery of compound 43b, 2-[2-propyl-3-[3-[2-ethyl-4-(4- fluorophenyl)-5-hydroxyphenoxy]-propoxy]phenoxy]benzoic acid (LY293111), a 2-arylphenol-substituted diaryl ether carboxylic acid which displayed potent binding to human neutrophils (IC50 = 17 +/- 4.6 nM) and guinea pig lung membranes (IC50 = 6.6 +/- 0.71 nM), inhibition of LTB4-induced expression of the CD11b/CD18 receptor on human neutrophils (IC50 = 3.3 +/- 0.81 nM), and inhibition of LTB4-induced contraction of guinea pig lung parenchyma (pKB = 8.7 +/- 0.16). In vivo, 43b demonstrated potent activity in inhibiting LTB4-induced airway obstruction in the guinea pig when dosed by the oral (ED50 = 0.40 mg/kg) or intravenous (ED50 = 0.014 mg/kg) routes. A specific LTB4 receptor antagonist, 43b had little effect on inhibiting contractions of guinea pig lung parenchyma induced by leukotriene D4 (LTD4), histamine, carbachol, or U46619. Compound 43b has been chosen as a clinical candidate and is currently in phase I studies for a variety of inflammatory diseases.
Author	Baker, S. Richard Cockerham, Sandra L Floreancig, Paul Froelich, Larry L Sawyer, J. Scott Bach, Nicholas J Borromeo, Peter S Fleisch, Jerome H Baldwin, Ronald F
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SubjectTerms	Airway Obstruction - metabolism Animals Benzoates - chemical synthesis Benzoates - chemistry Benzoates - pharmacology Guinea Pigs Humans Leukotriene B4 - antagonists & inhibitors Leukotriene B4 - pharmacology Lung - drug effects Lung - metabolism Neutrophils - drug effects Neutrophils - metabolism Phenols - chemical synthesis Phenols - chemistry Phenols - pharmacology Receptors, Leukotriene B4 - antagonists & inhibitors Structure-Activity Relationship Tetrazoles - chemistry Tetrazoles - pharmacology
Title	Synthetic and Structure/Activity Studies on Acid-Substituted 2-Arylphenols: Discovery of 2-[2-Propyl-3-[3-[2-ethyl-4-(4-fluorophenyl)-5-hydroxyphenoxy]- propoxy]phenoxy]benzoic Acid, a High-Affinity Leukotriene B4 Receptor Antagonist
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