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Vol. 281, Issue 2, 707-712, 1997
Department of Pharmaceutics and Pharmacodynamics, The University of
Illinois at Chicago Health Sciences Center, Chicago, Illinois
The effects of twice-daily injections of L-arginine or
D-arginine (200 mg/kg i.p.) for 4 days on morphine-induced
antinociception, brain nitric oxide synthase activity and brain and
serum distribution of morphine and brain µ-opioid receptors labeled
with
[3H][D-Ala2,MePhe4,Gly5-ol]enkephalin
were determined in male Swiss-Webster mice. Chronic treatment with
L-arginine, but not D-arginine, decreased the
antinociceptive response to morphine in mice, increased the activity of
nitric oxide synthase in the midbrain and decreased brain levels of
morphine, compared with vehicle-injected controls. Significant
decreases in morphine levels were observed in midbrain, pons and
medulla, hippocampus, striatum and spinal cord of
L-arginine-treated mice, in comparison with
vehicle-injected mice. However, the levels of morphine in cortex,
amygdala and hypothalamus of L-arginine- or
D-arginine-treated mice did not differ from those of
vehicle-injected controls. Acute treatment with L-arginine
(200 mg/kg i.p.) or D-arginine (200 mg/kg i.p.) did not
modify either morphine antinociception or morphine distribution in
brain regions or the spinal cord. Chronic administration of
L-arginine or D-arginine did not alter the
Bmax or Kd values
of
[3H][D-Ala2,MePhe4,Gly5-ol]enkephalin
binding to the mouse brain membranes. These results suggest that
chronic treatment with L-arginine reduces the
antinociceptive effect of morphine by increasing brain nitric oxide
synthase activity and by decreasing the concentration of morphine in
certain brain regions and spinal cord.
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