Discovery of novel, orally active dual NK1/NK2 antagonists |
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| Authors: | Bernstein P R Aharony D Albert J S Andisik D Barthlow H G Bialecki R Davenport T Dedinas R F Dembofsky B T Koether G Kosmider B J Kirkland K Ohnmacht C J Potts W Rumsey W L Shen L Shenvi A Sherwood S Stollman D Russell K |
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| Affiliation: | CNS Discovery Research, AstraZeneca Pharmaceuticals LP, 1800 Concord Pike, PO Box 15437, Wilmington, DE 19850-5437, USA. peter.bernstein@astrazeneca.com |
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| Abstract: | ![]()
Exploration of the SAR around selective NK2 antagonists, SR48968 and ZD7944, led to the discovery that naphth-1-amide analogues provide potent dual NK1 and NK2 antagonists. ZD6021 inhibited binding of [3H]-NKA or [3H]-SP to human NK1 and NK2 receptors, with high-affinity (K(i)=0.12 and 0.62nM, respectively). In functional assays ZD6021 had, at 10(-7)M, in human pulmonary artery pK(B)=8.9 and in human bronchus pK(B)=7.3, for NK1 and NK2, respectively. Oral administration of ZD6021 to guinea pigs dose-dependently attenuated ASMSP induced extravasation of plasma proteins, ED(50)=0.5mg/kg, and NK2 mediated bronchoconstriction, ED(50)=13mg/kg. |
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