Synthesis and Pharmacological Evaluation in Mice of New Non-classical Antinociceptive Agents, 5-(4-Arylpiperazin-1-yl)-4-benzyl-1,2-oxazin-6-ones
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概要
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Several 5-(4-arylpiperazin-1-yl)-4-benzyl-1,2-oxazin-6-ones have been synthesized and tested for analgesic activity in a visceral pain model (phenylbenzoquinone-induced writhing test=PBQ test). A good correlation has been found between the antinociceptive effects of drugs and both their lipophilic and steric properties. The most active derivatives 5c and 5f, with intraperitoneal ED_<50> values of 10.5 and 10.3 mg kg^<-1> respectively, were more extensively investigated by evaluating their analgesic activity in a somatosensory pain model (hot plate test), as well as their sedative properties. Furthermore, naloxone suppressed the effect of 5c and 5f in the PBQ test, though these derivatives were ineffective to potentiate morphine analgesia. Pretreatment with yohimbine did not significantly attenuate the analgesic effects of 5c and 5f. In addition, pretreatment with 5-hydroxytryptophan associated with carbidopa also failed to potentiate the antinociceptive effects of 5c and 5f. So, a part of the analgesic activity of 5c and 5f seems to be related to an opioidergic mechanism, especially at the μ receptor level. Molecular modeling studies performed on the opiate drug morphine and on the most stable conformer of 5f showed structural similarities between these two molecules.
- 公益社団法人日本薬学会の論文
- 1997-04-15
著者
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Couquelet J
Groupe De Recherche En Pharmacochimie Laboratoire De Chimie Therapeutique Faculte Des Sciences Pharm
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BEBOT Monique
Groupe de Recherche en Pharmacochimie, Laboratoire de Chimie Therapeutique Faculte des Sciences Phar
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COUDERT Pascal
Groupe de Recherche en Pharmacochimie, Laboratoire de Chimie Therapeutique Faculte des Sciences Phar
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RUBAT Catherine
Laboratoire de Pharmacologie Faculte des Sciences Pharmaceutiques, Universite Francois Rabelais
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VALLEE-GOYET Danielle
Laboratoire de Chimie des Substances Naturelles, URA 485 du CNRS Faculte des Sciences Pharmaceutique
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GARDETTE Daniel
Laboratoire de Chimie des Substances Naturelles, URA 485 du CNRS Faculte des Sciences Pharmaceutique
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MAVEL Sylvie
Laboratoire de Chimie Therapeutique Faculte des Sciences Pharmaceutiques, Universite Francois Rabela
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ALBUISSON Eliane
Laboratoire de Biomathematiques et Informatique Medicale
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COUQUELET Jacques
Groupe de Recherche en Pharmacochimie, Laboratoire de Chimie Therapeutique Faculte des Sciences Phar
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Mavel Sylvie
Laboratoire De Chimie Therapeutique Faculte Des Sciences Pharmaceutiques Universite Francois Rabelai
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Bebot Monique
Groupe De Recherche En Pharmacochimie Laboratoire De Chimie Therapeutique Faculte Des Sciences Pharm
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Coudert Pascal
Groupe De Recherche En Pharmacochimie Laboratoire De Chimie Therapeutique Faculte Des Sciences Pharm
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Gardette Daniel
Laboratoire De Chimie Des Substances Naturelles Ura 485 Du Cnrs Faculte Des Sciences Pharmaceutiques
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Rubat C
Laboratoire De Pharmacologie Faculte Des Sciences Pharmaceutiques Universite Francois Rabelais
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Couquelet Jacques
Groupe De Recherche En Pharmacochimie Faculte De Pharmacie
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Vallee-goyet Danielle
Laboratoire De Chimie Des Substances Naturelles Ura 485 Du Cnrs Faculte Des Sciences Pharmaceutiques
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