L-NG-硝基精氨酸甲酯在小鼠中表现出抗伤害感受活性。
L-NG-nitro arginine methyl ester exhibits antinociceptive activity in the mouse.
作者信息
Moore P K, Oluyomi A O, Babbedge R C, Wallace P, Hart S L
机构信息
Smooth Muscle Pharmacology Group, King's College, University of London.
出版信息
Br J Pharmacol. 1991 Jan;102(1):198-202. doi: 10.1111/j.1476-5381.1991.tb12153.x.
Abstract
- L-NG-nitro arginine methyl ester (L-NAME, 1-75 mg kg-1) administered intraperitoneally (i.p.) elicits dose-related antinociception in the mouse assessed by the formalin-induced paw licking procedure. Antinociceptive activity is still present 24 h after injection. L-NAME (75 mg kg-1, i.p.) is also antinociceptive in the acetic acid-induced abdominal constriction and hot plate procedures. 2. L-NAME additionally produces a dose-related inhibition of formalin-induced paw licking following intracerebroventricular (i.c.v., 0.1-100 microgram per mouse) and oral (p.o., 75-150 mg kg-1) administration. 3. L-Arginine (600 mg kg-1, i.p.) but not D-arginine (600 mg kg-1) or naloxone (5 mg kg-1) reverses the antinociceptive effect of L-NAME in the formalin test. 4. High doses of L-NAME (37.5-600 mg kg-1) but not D-NAME (75 mg kg-1) administered i.p. produce dose-related increases in blood pressure of the urethane-anaesthetized mouse whilst i.c.v. injected L-NAME (0.1 and 100 microgram per mouse) in inactive. 5. L-NAME (75 mg kg-1, i.p.) did not inhibit oedema formation in the formalin-injected mouse hindpaw. 6. L-NAME (75 mg kg-1) did not produce any overt behavioural changes in treated mice and failed to influence locomotor activity or the incidence of dipping, crossing, rearing or circling behaviour assessed by a modified 'head-dipping' board procedure. A high dose of L-NAME (600 mg kg-1) reduced dipping behaviour and locomotor activity suggesting a possible sedative effect. D-NAME (600mgkg 1) was inactive. 7. These results suggest that L-NAME produces an opioid-independent and long-lasting antinociception in the mouse most probably by a direct effect within the central nervous system.
摘要
- 通过福尔马林诱导的舔足实验评估,腹腔注射L-硝基精氨酸甲酯(L-NAME,1 - 75毫克/千克)可使小鼠产生剂量相关的抗伤害感受作用。注射后24小时仍存在抗伤害感受活性。L-NAME(75毫克/千克,腹腔注射)在醋酸诱导的腹部收缩和热板实验中也具有抗伤害感受作用。2. L-NAME经脑室内注射(每只小鼠0.1 - 100微克)和口服(75 - 150毫克/千克)后,对福尔马林诱导的舔足行为也产生剂量相关的抑制作用。3. L-精氨酸(600毫克/千克,腹腔注射)可逆转L-NAME在福尔马林实验中的抗伤害感受作用,而D-精氨酸(600毫克/千克)或纳洛酮(5毫克/千克)则不能。4. 腹腔注射高剂量的L-NAME(37.5 - 600毫克/千克)可使乌拉坦麻醉的小鼠血压产生剂量相关的升高,而脑室内注射L-NAME(每只小鼠0.1和100微克)则无此作用。5. L-NAME(75毫克/千克,腹腔注射)对福尔马林注射所致小鼠后爪水肿形成无抑制作用。6. L-NAME(75毫克/千克)对处理后的小鼠未产生任何明显的行为变化,且未影响运动活性或通过改良的“头部浸入”板实验评估的浸入、交叉、直立或转圈行为的发生率。高剂量的L-NAME(600毫克/千克)可减少浸入行为和运动活性,提示可能具有镇静作用。D-NAME(600毫克/千克)无活性。7. 这些结果表明,L-NAME在小鼠中产生一种不依赖阿片类物质的持久抗伤害感受作用,最可能是通过对中枢神经系统的直接作用实现的。
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