Modulation on C‐ and N‐Terminal Moieties of a Series of Potent and Selective Linear Tachykinin NK2 Receptor Antagonists |
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Authors: | Martina Gensini Dr. Maria Altamura Dr. Tula Dimoulas Dr. Valentina Fedi Dr. Danilo Giannotti Dr. Sandro Giuliani Dr. Antonio Guidi Dr. Nicholas J. S. Harmat Dr. Stefania Meini Dr. Rossano Nannicini Franco Pasqui Manuela Tramontana Dr. Antonio Triolo Dr. Carlo Alberto Maggi Dr. |
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Affiliation: | 1. Chemistry Department, Menarini Ricerche S.p.A. Via Sette Santi 3, 50131 Florence (Italy), Fax: (+39)?055‐5680419;2. Pharmacology Department, Menarini Ricerche S.p.A. Via Sette Santi 3, 50131 Florence (Italy) |
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Abstract: | Herein we describe the synthesis of a series of new potent tachykinin NK2 receptor antagonists by the modulation of the C‐ and N‐terminal moieties of ibodutant (MEN 15596, 1 ). The N‐terminal benzo[b]thiophene ring was replaced by different substituted naphthalenes and benzofurans, while further modifications were evaluated at the C‐terminal tetrahydropyran moiety. Most compounds demonstrated a high affinity for the human NK2 receptor and high in vitro antagonist potency, indicating that a wide range of substituents at both termini can be incorporated in the molecule without detrimental effects on the interactions with the NK2 receptor. Selected compounds were tested in vivo confirming their activity as NK2 antagonists. In particular, after both iv and id administration to guinea pig, compound 61 b was able to antagonize NK2‐induced colonic contractions with a potency and duration‐of‐action fully comparable to the reference compound 1 (MEN 15596, ibodutant). |
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Keywords: | drug discovery NK2 receptors structure– activity relationships tachykinin |
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