The Discovery of Phthalazinone-Based Human H 1 and H 3 Single-Ligand Antagonists Suitable for Intranasal Administration for the Treatment of Allergic Rhinitis

Artigo Revisado por pares

The Discovery of Phthalazinone-Based Human H 1 and H 3 Single-Ligand Antagonists Suitable for Intranasal Administration for the Treatment of Allergic Rhinitis

2011; American Chemical Society; Volume: 54; Issue: 7 Linguagem: Inglês

10.1021/jm1013874

ISSN

1520-4804

Autores

Panayiotis A. Procopiou, Christopher R. Browning, Jennifer M. Buckley, Kenneth L. Clark, Lise C. Fechner, Paul M. Gore, Ashley P. Hancock, Simon T. Hodgson, Duncan S. Holmes, Michael Kranz, Brian E. Looker, Karen M. L. Morriss, Daniel L. Parton, Linda Russell, Robert J. Slack, Steven L. Sollis, Sadie Vile, Clarissa J. Watts,

Tópico(s)

Olfactory and Sensory Function Studies

Resumo

A series of potent phthalazinone-based human H(1) and H(3) bivalent histamine receptor antagonists, suitable for intranasal administration for the potential treatment of allergic rhinitis, were identified. Blockade of H(3) receptors is thought to improve efficacy on nasal congestion, a symptom of allergic rhinitis that is currently not treated by current antihistamines. Two analogues (56a and 56b) had slightly lower H(1) potency (pA(2) 9.1 and 8.9, respectively, vs 9.7 for the clinical gold-standard azelastine, and H(3) potency (pK(i) 9.6 and 9.5, respectively, vs 6.8 for azelastine). Compound 56a had longer duration of action than azelastine, low brain penetration, and low oral bioavailability, which coupled with the predicted low clinical dose, should limit the potential of engaging CNS-related side-effects associated with H(1) or H(3) antagonism.

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The Discovery of Phthalazinone-Based Human H 1 and H 3 Single-Ligand Antagonists Suitable for Intranasal Administration for the Treatment of Allergic Rhinitis