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Vol. 284, Issue 1, 196-201, 1998
Department of Pharmacology and Physiology, The University of
Rochester, School of Medicine and Dentistry, Rochester, New York
The role of the supraspinal nitric oxide (NO)/cyclic GMP system in the
development of acute morphine antinociceptive tolerance was
investigated by use of the mouse 55°C warm-water tail-flick test. A
single intracerebroventricular (i.c.v.) pretreatment of mice with
morphine (3 nmol, 140 min before testing) produced an acute
antinociceptive tolerance to subsequent i.c.v. doses of morphine, as
demonstrated by a 120-fold rightward shift of the morphine
dose-response curve. When co-administered with morphine (140 min before
testing), the NO synthase inhibitors: N-nitro-L-arginine methyl ester (L-NAME), 3-bromo-7-nitroindazole,
7-nitroindazole and NG-monomethyl-L-arginine,
attenuated the development of morphine tolerance. All four NO synthase
inhibitors completely blocked the rightward shift of the morphine
dose-response curve caused by i.c.v. morphine pretreatment (3 nmol, 140 min before testing). This effect was partially antagonized by
L-arginine, but not D-arginine, in a
dose-dependent manner. Also, D-NAME did not block the
development of tolerance. Like the NO synthase inhibitors, LY-83,583, a
guanylyl cyclase inhibitor, blocked the development of tolerance, which suggests that NO acting through the cyclic GMP pathway is involved in
the development of acute antinociceptive tolerance. The effects of
increased NO production on acute morphine antinociceptive tolerance were also studied. When co-administered with morphine (140 min before
testing), neither L-arginine (100 nmol) nor the NO donors, sodium nitroprusside (5 nmol) and isosorbide dinitrate (10 nmol), had
any effect on the magnitude of morphine antinociceptive tolerance. These results suggest that NO, acting through the cyclic GMP pathway, mediates the development of acute antinociceptive tolerance, but that
NO production does not alter the magnitude of antinociceptive tolerance.
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