عنوان مقاله :
ارزيابي اثر تجويز سيستميك مينوسايكلين و رايلوزول بر تحمل به اثرات ضد دردي ناشي از مصرف مزمن مرفين در موش صحرايي
عنوان به زبان ديگر :
Evaluation the Effects of Systemic Administration of Minocycline and Riluzole on
Tolerance to Morphine Analgesic effect in rat
پديد آورندگان :
حبيبي اصل ، بهلول نويسنده دانشكده داروسازي-دانشگاه علوم پزشكي تبريز Habibi Asl, B , علي محمدي، بهرام نويسنده دانشكده داروسازي-دانشگاه علوم پزشكي تبريز Alimohammadi, B , چرخ پور، محمد نويسنده دانشكده داروسازي- دانشگاه علوم پزشكي تبريز Charkh Poor, M , حسن زاده، كامبيز نويسنده دانشكده داروسازي- دانشگاه علوم پزشكي تبريز Hassanzadeh, K
كليدواژه :
Morphine , Minocycline , TOLERANCE , Nitric oxide , مينوسايكلين , نيتريك اكسايد , رايلوزول , تحمل , مرفين , Riluzole
چكيده لاتين :
Objectives: Chronic opiate administration induces tolerance to the analgesic effect. Several studies indicate that
nitric oxide/ N-methyl D-aspartate pathway has important role on morphine induced tolerance. The main goal ofthis
study was to evaluate the effects of systemic administration of Minocycline and Riluzole on Morphine induced
tolerance in rat. Methods: Animals were divided in 8 groups (n=8) and received daily: Saline (I ml/kg-ip) or {Saline
(Irnl/kg- ip) + Morphine (10 mg /kg- ip)} or {Minocycline (10, 20, 40 mg/kg- ip) + Morphine (10 mg/kg- ip)J or
Minocycline (10 mg/kg- ip) or Tween 80 (2%) (I ml/kg- ip) or {Tween 80 (2%) (Irnl/kg- ip) + Morphine (10 mg /kgip)
J or {Riluzole (4, 8, 12 mg/kg- ip) + Morphine (10 mg/kg- ip)J or Riluzole (12 mg/kg- ip), Nociception was
assessed using hot-plate apparatus. The hot-plate latency was recorded when rat licked its hind paw. A baseline
latency was determined daily, then drug was injected. After 30 minutes morphine was administrated and post-drug
latency evaluated 30 minutes after the injection of Morphine. Results: Results showed that Minocycline (20, 40
mglkg) and Minocycline (10 mg/kg), delayed the tolerance appearing time about 3 and 4 days respectively. Riluzole
(8, 12 mglkg) could postpone day of morphine tolerance for 5 days in comparison with control group. Conclu.ioo:
Interaction with nitric oxide system and glutarnatergic pathway are the possible mechanisms of Minocycline and
ability of Riluzole as a glutamate release inhibitor could be the major mechanism in attenuating the development of
Morphine induced tolerance.
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