Literature DB >> 31655025

Novel highly potent OXE receptor antagonists with prolonged plasma lifetimes that are converted to active metabolites in vivo in monkeys.

Qiuji Ye1, Shishir Chourey1, Chintam Nagendra Reddy1, Rui Wang1, Chantal Cossette2, Sylvie Gravel2, Irina Slobodchikova3, Dajana Vuckovic3, Joshua Rokach1, William S Powell2.   

Abstract

BACKGROUND AND
PURPOSE: The 5-lipoxygenase product 5-oxo-6E,8Z,11Z,14Z-eicosatetraenoic acid (5-oxo-ETE), acting through the OXE receptor, is a potent eosinophil chemoattractant that may be an important proinflammatory mediator in eosinophilic diseases such as asthma. We previously identified a series of indole-based OXE receptor antagonists that rapidly appear in the blood following oral administration but have limited lifetimes. The objective of this study was to increase the potency and plasma half-lives of these compounds and thereby identify the optimal candidate for future preclinical studies in monkeys, as rodents do not have an OXE receptor orthologue. EXPERIMENTAL APPROACH: We synthesized a series of substituted phenylalkyl indoles and compared their antagonist potencies, pharmacokinetics, and metabolism to those of our earlier compounds. The potencies of some of their metabolites were also investigated. KEY
RESULTS: Among the compounds tested, the S-enantiomer of the m-chlorophenyl compound (S-Y048) was the most potent, with an pIC50 of about 10.8 for inhibition of 5-oxo-ETE-induced calcium mobilization in human neutrophils. When administered orally to cynomolgus monkeys, S-Y048 rapidly appeared in the blood and had a half-life in plasma of over 7 hr, considerably longer than any of the other OXE analogues tested. A major hydroxylated metabolite, with a potency close to that of its precursor, was identified in plasma. CONCLUSION AND IMPLICATIONS: Because of its highly potent antagonist activity and its long lifetime in vivo, S-Y048 may be a useful anti-inflammatory agent for the treatment of eosinophilic diseases such as asthma, allergic rhinitis, and atopic dermatitis.
© 2019 The British Pharmacological Society.

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Year:  2020        PMID: 31655025      PMCID: PMC6989946          DOI: 10.1111/bph.14874

Source DB:  PubMed          Journal:  Br J Pharmacol        ISSN: 0007-1188            Impact factor:   8.739


  36 in total

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Authors:  Shishir Chourey; Qiuji Ye; Chintam Nagendra Reddy; Rui Wang; Chantal Cossette; Sylvie Gravel; Irina Slobodchikova; Dajana Vuckovic; Joshua Rokach; William S Powell
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  5 in total

1.  Targeting the OXE receptor with a selective antagonist inhibits allergen-induced pulmonary inflammation in non-human primates.

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2.  Inhibition of allergen-induced dermal eosinophilia by an oxoeicosanoid receptor antagonist in non-human primates.

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Journal:  Br J Pharmacol       Date:  2020-01-17       Impact factor: 8.739

3.  Novel highly potent OXE receptor antagonists with prolonged plasma lifetimes that are converted to active metabolites in vivo in monkeys.

Authors:  Qiuji Ye; Shishir Chourey; Chintam Nagendra Reddy; Rui Wang; Chantal Cossette; Sylvie Gravel; Irina Slobodchikova; Dajana Vuckovic; Joshua Rokach; William S Powell
Journal:  Br J Pharmacol       Date:  2020-01-17       Impact factor: 8.739

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