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强啡肽肽段在炎性疼痛模型中的抗伤害感受作用。

Antinociceptive effects of dynorphin peptides in a model of inflammatory pain.

作者信息

Beyer A, Schäfer M, Stein C

机构信息

Division of Intramural Research, National Institute on Drug Abuse, Baltimore, MD 21224, USA.

出版信息

Pain. 1997 Apr;70(2-3):141-7. doi: 10.1016/s0304-3959(97)03327-7.

DOI:10.1016/s0304-3959(97)03327-7
PMID:9150287
Abstract

Dynorphin A (DYN) peptides, administered into the central nervous system, have produced inconsistent analgesic actions in tests using thermal stimuli. This study examined antinociceptive effects of intravenous and intraplantar DYN-(2-17) against noxious pressure in rats with Freund's adjuvant-induced unilateral hindpaw inflammation. The effects of DYN-(2-17) were compared to those of the opioid agonists morphine. (D-Ala2,N-Methyl-Phe4,Gly-ol5)-enkephalin (DAMGO) and DYN-(1-17). Intravenous DYN-(2-17) (0.188-10 mg/kg) produced dose-dependent elevations of paw pressure thresholds in inflamed and in non-inflamed paws. These effects were similar in magnitude to those of subcutaneous morphine (2 mg/kg), at doses of 0.375-1.5 mg/kg they were significantly greater on the inflamed (right) than on the non-inflamed (left) paw, and they were not reversible by intravenous naloxone (1-10 mg/kg). Intraplantar Dyn-(2-17)(0.001-0.3 mg) was ineffective, whereas both intraplantar DYN-(1-17)(0.15-0.3 mg) and DAMGO (0.008-0.016 mg) produced dose-dependent and naloxone-reversible elevations of paw pressure thresholds. The intraplantar injection of both Dyn peptides produced a transient increase in the volume of non-inflamed paws. These findings suggest that intravenous DYN-(2-17) produces possibly centrally mediated, non-opioid antinociceptive effects against noxious pressure. At certain doses these effects are more potent in inflamed than in non-inflamed paws. In contrast to the opioid peptides DYN-(1-17) and DAMGO, DYN-(2-17) does not appear to have no peripheral antinociceptive actions.

摘要

将强啡肽A(DYN)肽注入中枢神经系统后,在热刺激试验中其镇痛作用并不一致。本研究检测了静脉注射和足底注射DYN-(2-17)对弗氏佐剂诱导的单侧后爪炎症大鼠有害压力的抗伤害感受作用。将DYN-(2-17)的作用与阿片类激动剂吗啡、(D-丙氨酸2,N-甲基苯丙氨酸4,甘醇5)-脑啡肽(DAMGO)和DYN-(1-17)的作用进行了比较。静脉注射DYN-(2-17)(0.188-10mg/kg)可使炎症爪和非炎症爪的爪压力阈值呈剂量依赖性升高。这些作用在程度上与皮下注射吗啡(2mg/kg)相似,在0.375-1.5mg/kg剂量时,对炎症(右侧)爪的作用明显大于对非炎症(左侧)爪的作用,并且静脉注射纳洛酮(1-10mg/kg)不能使其逆转。足底注射Dyn-(2-17)(0.001-0.3mg)无效,而足底注射DYN-(1-17)(0.15-0.3mg)和DAMGO(0.008-0.016mg)均可使爪压力阈值呈剂量依赖性升高且可被纳洛酮逆转。两种Dyn肽足底注射均使非炎症爪的体积短暂增加。这些发现表明,静脉注射DYN-(2-17)可能产生中枢介导的、针对有害压力的非阿片类抗伤害感受作用。在某些剂量下,这些作用在炎症爪中比在非炎症爪中更强。与阿片肽DYN-(1-17)和DAMGO不同,DYN-(2-17)似乎没有外周抗伤害感受作用。

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