MK-801对利血平引起的僵硬的抗帕金森作用:肌力图分析。

K Ossowska, E Lorenc-Koci, S Wolfarth
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引用次数: 28

摘要

MK-801是一种NMDA受体的非竞争性拮抗剂,已知在帕金森病的许多动物模型中表现出有益的作用。本研究旨在探讨MK-801对利血平所致肌肉僵硬的影响。刚性通过直接肌力图法估计。这种方法包括在踝关节处连续弯曲和伸直老鼠的后脚,并测量脚对被动运动的阻力。利血平剂量为5-10 mg/kg / ip,单独给药或与α -甲基-对酪氨酸(α MT, 250 mg/kg / ip)联合给药,可诱导僵硬。利血平10 mg/kg给药1 h后肌肉僵直最强。利血平(10 mg/kg ip)后70 min注射MK-801 (0.32 ~ 1.28 mg/kg sc)可降低后者引起的刚性。同样,MK-801 (1.28 mg/kg sc)在利血平(10 mg/kg ip)和α - MT (250 mg/kg ip)联合治疗后27 h 40'给予,强烈抑制利血平诱导的肌肉僵硬。结果表明,谷氨酸能亢进在利血平诱导的强直中起重要作用。由于利血平引起的运动障碍被普遍认为是帕金森症状的动物模型,因此可以假设NMDA受体阻断成分可能在抗帕金森药物的治疗作用中发挥了重要作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Antiparkinsonian action of MK-801 on the reserpine-induced rigidity: a mechanomyographic analysis.

MK-801, a non-competitive antagonist of NMDA receptors, is known to exhibit a beneficial action in many animal models of Parkinson's disease. The aim of this study was to examine the influence of MK-801 on the reserpine-induced muscle rigidity. The rigidity was estimated by a direct mechanomyographic method. This method consists in successive bending and straightening of a rat's hind foot in the ankle joint and measuring the resistance of the foot to passive movements. Reserpine in doses of 5-10 mg/kg ip, given alone or in combination with alpha-methyl-p-tyrosine (alpha MT, 250 mg/kg ip), induced rigidity. The strongest muscle rigidity was induced by 10 mg/kg of reserpine 1 hour after administration. MK-801 (0.32-1.28 mg/kg sc) injected 70 min after reserpine (10 mg/kg ip) decreased the rigidity induced by the latter compound. Similarly, MK-801 (1.28 mg/kg sc), administered 27 h 40' after joint treatment with reserpine (10 mg/kg ip) and alpha MT (250 mg/kg ip), strongly inhibited the reserpine-induced muscle rigidity. The obtained results show that the glutamatergic hyperactivity plays a significant role in the reserpine-induced rigidity. As the reserpine-induced motor disturbances are commonly accepted to be an animal model of parkinsonian symptoms, it may be assumed that the NMDA receptor blocking component may contribute substantially to the therapeutic action of antiparkinsonian drugs.

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