阿片类拮抗剂增强小鼠的伤害性反应。
Enhancement of a nociceptive reaction by opioid antagonists in mice.
作者信息
Jacob J J, Ramabadran K
出版信息
Br J Pharmacol. 1978 Sep;64(1):91-8. doi: 10.1111/j.1476-5381.1978.tb08645.x.
Abstract
- The opioid antagonists, naloxone, GPA 2163, levallorphan and Mr-2266 reduced the latency of the jumping reaction of mice in the hot plate test. The (+)-isomers of levallorphan and Mr-2266 which are devoid of antagonistic activity did not increase this latency. 2. In the same nociceptive reaction test, the enhancing effect of naloxone progressed in a dose-range similar to that required for the antagonism by naloxone of the depressive action of morphine. 3. The facilitatory effect of naloxone was not blocked by the previous administration of morphine or etorphine but it was prevented by pretreatment with a high dose of buprenorphine. 4. The antagonism by naloxone of morphine and of buprenorphine did not follow the same pattern. 5. The factors which are or may be involved in the efficacy of naloxone in enhancing nociceptive reactions are discussed. 6. The enhancing effect of naloxone may be due to an antagonism of endogenous ligands for the opiate receptor. If so, these ligands would be involved in reaction to but not in perception of nociceptive stimuli which need not be harmful ones.
摘要
- 阿片类拮抗剂纳洛酮、GPA 2163、左洛啡烷和Mr-2266在热板试验中缩短了小鼠跳跃反应的潜伏期。左洛啡烷和Mr-2266无拮抗活性的(+)异构体并未延长该潜伏期。2. 在同一项伤害性反应试验中,纳洛酮的增强作用在与纳洛酮拮抗吗啡抑制作用所需剂量范围相似的剂量范围内呈现进展。3. 纳洛酮的促进作用未被预先给予的吗啡或埃托啡阻断,但高剂量丁丙诺啡预处理可阻止该作用。4. 纳洛酮对吗啡和丁丙诺啡的拮抗作用模式不同。5. 讨论了与纳洛酮增强伤害性反应效力相关或可能相关的因素。6. 纳洛酮的增强作用可能是由于对阿片受体内源性配体的拮抗作用。如果是这样,这些配体将参与对伤害性刺激的反应,但不参与对伤害性刺激的感知,而这些刺激不一定是有害刺激。
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本文引用的文献
1
STUDIES ON PAIN. A NEW METHOD FOR MEASURING PAIN THRESHOLD: OBSERVATIONS ON SPATIAL SUMMATION OF PAIN.疼痛研究。一种测量疼痛阈值的新方法:关于疼痛空间总和的观察。
J Clin Invest. 1940 Jul;19(4):649-57. doi: 10.1172/JCI101168.
2
[Action of some analgesics on the behavior of mice exposed to a thermoanalgesic stimulus. II. Immediate nociceptive response. Differential actions of analgesic and psychoactive substances on the leeching and jumping reactions].[某些镇痛药对接受热镇痛刺激的小鼠行为的作用。II. 即时伤害性反应。镇痛药和精神活性物质对水蛭样退缩反应和跳跃反应的不同作用]
Arch Int Pharmacodyn Ther. 1961 Oct 1;133:296-309.
3
The measurement of pain; prototype for the quantitative study of subjective responses.疼痛的测量;主观反应定量研究的原型。
Pharmacol Rev. 1957 Mar;9(1):59-209.
4
Pharmacological effects produced by intracerebral injection of drugs in the conscious mouse.清醒小鼠脑内注射药物所产生的药理效应。
Br J Pharmacol Chemother. 1957 Mar;12(1):12-5. doi: 10.1111/j.1476-5381.1957.tb01354.x.
5
[Enhancement of nociceptive reactions by naloxone in mice and rats (author's transl)].纳洛酮对小鼠和大鼠伤害性反应的增强作用(作者译)
Psychopharmacologia. 1974 Jul 11;37(3):217-23. doi: 10.1007/BF00421535.
6
Levallorphan and related compounds.左洛啡烷及相关化合物。
Adv Biochem Psychopharmacol. 1973;8(0):45-50.
7
Structure-activity relationships in narcotic antagonists with N-furylmethyl substituents.具有N-呋喃甲基取代基的麻醉拮抗剂的构效关系。
Adv Biochem Psychopharmacol. 1973;8(0):91-107.
8
Antagonists in the 5-phenyl-benzomorphan series.5-苯基-苯并吗啡烷系列中的拮抗剂。
Adv Biochem Psychopharmacol. 1973;8(0):81-9.
9
Opioid agonist activity of beta-lipotropin fragments: a possible biological source of morphine-like substances in the pituitary.β-促脂解素片段的阿片样激动剂活性:垂体中吗啡样物质的一种可能生物学来源。
FEBS Lett. 1976 Apr 15;64(1):181-4. doi: 10.1016/0014-5793(76)80278-5.
10
C fragment of lipotropin has a high affinity for brain opiate receptors.促脂解素的C片段对脑阿片受体具有高亲和力。
Nature. 1976 Apr 29;260(5554):793-5. doi: 10.1038/260793a0.
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