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Effect of styrene maleic acid WIN55,212-2 micelles on neuropathic pain in a rat model

机译:苯乙烯马来酸WIN55,212-2胶束对大鼠神经性疼痛的影响

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摘要

Cannabinoid receptor agonists are moderately effective at reducing neuropathic pain but are limited by psychoactivity. We developed a styrene maleic acid (SMA) based on the cannabinoid WIN 55,212-2 (WIN) and tested in a rat model of neuropathic pain and in the rotarod test. We hypothesized that miceller preparation can ensure prolonged plasma half-life being above the renal threshold of excretion. Furthermore, SMA-WIN could potentially reduce the central nervous system effects of encapsulated WIN by limiting its transport across the blood-brain barrier. Using the chronic constriction injury model of sciatic neuropathy, the SMA-WIN micelles were efficacious in the treatment of neuropathic pain for a prolonged period compared to control (base WIN). Attenuation of chronic constriction injury-induced mechanical allodynia occurred for up to 8 h at a dose of 11.5 mg/kg of SMA-WIN micelles. To evaluate central effects on motor function, the rotarod assessment was utilized. Results showed initial impairment caused by SMA-WIN micelles to be identical to WIN control for up to 1.5 h. Despite this, the SMA-WIN micelle formulation was able to produce prolonged analgesia over a time when there was decreased impairment in the rotarod test compared with base WIN.
机译:大麻素受体激动剂在减轻神经性疼痛方面有中度有效,但受精神活动的限制。我们开发了基于大麻类WIN 55,212-2(WIN)的苯乙烯马来酸(SMA),并在神经性疼痛大鼠模型和旋转脚架测试中进行了测试。我们假设胶束制备可以确保延长的血浆半衰期高于肾脏排泄阈值。此外,SMA-WIN可能会通过限制其跨血脑屏障的运输来降低封装的WIN对中枢神经系统的影响。与坐骨神经痛(基础WIN)相比,使用坐骨神经病的慢性收缩损伤模型,SMA-WIN胶束可长时间有效治疗神经性疼痛。 SMA-WIN胶束剂量为11.5 mg / kg时,慢性压迫性损伤引起的机械性异常性疼痛可长达8小时。为了评估对运动功能的中枢效应,使用了旋转脚踏车评估。结果表明,由SMA-WIN胶束引起的初始损伤与WIN对照长达1.5小时相同。尽管如此,当与基础WIN相比,旋转棒试验的损伤减少时,SMA-WIN胶束制剂仍能产生长时间的镇痛作用。

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