From bradykinin B2 receptor antagonists to orally active and selective bradykinin B1 receptor antagonists |
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| Authors: | Barth Martine Bondoux Michel Luccarini Jean-Michel Peyrou Vincent Dodey Pierre Pruneau Didier Massardier Christine Paquet Jean-Luc |
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| Affiliation: | Department of Chemical Design and Synthesis, Clinical Candidate Selection, Laboratoires Fournier, 50 Rue de Dijon, 21121 Daix, France. martine.barth@abbott.com |
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| Abstract: | The bradykinin (BK) B1 receptor is an attractive target for the treatment of chronic pain and inflammation. Starting from a dual B1 and B2 antagonist, novel antagonists were designed that display low-nanomolar affinity for human B1 receptor and selectivity over B2. Initially, potent imidazoline derivatives were studied, but these compounds suffered from low bioavailability. This issue could be overcome by the use of less basic amino derivatives leading to orally active compounds. |
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