The antinociceptive effect of SM 32 was examined in mice by using the hot-plate (10–40 mg kg-1 i.p; 3–30 mg per mouse i.c.v.) and abdominal constriction (10–30 mg kg-1 i.p) tests. In the antinociceptive dose-range, SM 32 did not impair mouse spontaneous motility and motor coordination evaluated respectively by the Animex and rota-rod tests. The increase in the pain threshold produced by SM 32 was prevented by dicyclomine, pirenzepine and hemicholinium-3 but not by naloxone and CGP 35348. In vitro experiments showed that the SM 32 amplified electrically- and nicotine-evoked guinea-pig ileum contractions. On the basis of the above data, it can be postulated that SM 32 exerts its antinociceptive effect through a potentiation of central cholinergic transmission.
ANTINOCICEPTION INDUCED BY SM32 DEPENDS ON CENTRAL CHOLINERGIC MECHANISM / C. GHELARDINI; N. GALEOTTI; F. GUALTIERI; M. ROMANELLI; A. BARTOLINI. - In: PHARMACOLOGICAL RESEARCH. - ISSN 1043-6618. - STAMPA. - 35:(1997), pp. 141-147. [10.1006/phrs.1996.0110]
ANTINOCICEPTION INDUCED BY SM32 DEPENDS ON CENTRAL CHOLINERGIC MECHANISM
GHELARDINI, CARLA;GALEOTTI, NICOLETTA;GUALTIERI, FULVIO;ROMANELLI, MARIA NOVELLA;BARTOLINI, ALESSANDRO
1997
Abstract
The antinociceptive effect of SM 32 was examined in mice by using the hot-plate (10–40 mg kg-1 i.p; 3–30 mg per mouse i.c.v.) and abdominal constriction (10–30 mg kg-1 i.p) tests. In the antinociceptive dose-range, SM 32 did not impair mouse spontaneous motility and motor coordination evaluated respectively by the Animex and rota-rod tests. The increase in the pain threshold produced by SM 32 was prevented by dicyclomine, pirenzepine and hemicholinium-3 but not by naloxone and CGP 35348. In vitro experiments showed that the SM 32 amplified electrically- and nicotine-evoked guinea-pig ileum contractions. On the basis of the above data, it can be postulated that SM 32 exerts its antinociceptive effect through a potentiation of central cholinergic transmission.
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