新型κ阿片受体激动剂甲磺酸盐Sal B的药理学及抗成瘾作用,Sal B是一种强效长效的Salvinorin A类似物。
Pharmacology and anti-addiction effects of the novel κ opioid receptor agonist Mesyl Sal B, a potent and long-acting analogue of salvinorin A.
作者信息
Simonson B, Morani A S, Ewald A W M, Walker L, Kumar N, Simpson D, Miller J H, Prisinzano T E, Kivell B M
机构信息
School of Biological Science, Centre for Biodiscovery, Victoria University of Wellington, Wellington, New Zealand.
出版信息
Br J Pharmacol. 2015 Jan;172(2):515-31. doi: 10.1111/bph.12692. Epub 2014 Jul 1.
BACKGROUND AND PURPOSE
Acute activation of κ opioid (KOP) receptors results in anticocaine-like effects, but adverse effects, such as dysphoria, aversion, sedation and depression, limit their clinical development. Salvinorin A, isolated from the plant Salvia divinorum, and its semi-synthetic analogues have been shown to have potent KOP receptor agonist activity and may induce a unique response with similar anticocaine addiction effects as the classic KOP receptor agonists, but with a different side effect profile.
EXPERIMENTAL APPROACH
We evaluated the duration of effects of Mesyl Sal B in vivo utilizing antinociception assays and screened for cocaine-prime induced cocaine-seeking behaviour in self-administering rats to predict anti-addiction effects. Cellular transporter uptake assays and in vitro voltammetry were used to assess modulation of dopamine transporter (DAT) function and to investigate transporter trafficking and kinase signalling pathways modulated by KOP receptor agonists.
KEY RESULTS
Mesyl Sal B had a longer duration of action than SalA, had anti-addiction properties and increased DAT function in vitro in a KOP receptor-dependent and Pertussis toxin-sensitive manner. These effects on DAT function required ERK1/2 activation. We identified differences between Mesyl Sal B and SalA, with Mesyl Sal B increasing the Vmax of dopamine uptake without altering cell-surface expression of DAT.
CONCLUSIONS AND IMPLICATIONS
SalA analogues, such as Mesyl Sal B, have potential for development as anticocaine agents. Further tests are warranted to elucidate the mechanisms by which the novel salvinorin-based neoclerodane diterpene KOP receptor ligands produce both anti-addiction and adverse side effects.
LINKED ARTICLES
This article is part of a themed section on Opioids: New Pathways to Functional Selectivity. To view the other articles in this section visit http://dx.doi.org/10.1111/bph.2015.172.issue-2.
背景与目的
κ阿片受体(KOP)的急性激活会产生类抗可卡因效应,但诸如烦躁不安、厌恶、镇静和抑郁等不良反应限制了它们的临床开发。从植物鼠尾草中分离出的Salvinorin A及其半合成类似物已被证明具有强大的KOP受体激动剂活性,并且可能诱导出一种独特的反应,具有与经典KOP受体激动剂类似的抗可卡因成瘾作用,但副作用谱不同。
实验方法
我们利用抗伤害感受试验评估了甲磺酸盐Sal B在体内的作用持续时间,并在自我给药的大鼠中筛选可卡因引发的觅药行为,以预测其抗成瘾作用。细胞转运体摄取试验和体外伏安法用于评估多巴胺转运体(DAT)功能的调节,并研究KOP受体激动剂调节的转运体转运和激酶信号通路。
主要结果
甲磺酸盐Sal B的作用持续时间比SalA长,具有抗成瘾特性,并以KOP受体依赖性和百日咳毒素敏感性方式在体外增加DAT功能。这些对DAT功能的影响需要ERK1/2激活。我们确定了甲磺酸盐Sal B和SalA之间的差异,甲磺酸盐Sal B增加了多巴胺摄取的Vmax,而不改变DAT的细胞表面表达。
结论与启示
SalA类似物,如甲磺酸盐Sal B,有开发成为抗可卡因药物的潜力。有必要进行进一步测试,以阐明基于Salvinorin的新型克罗烷二萜KOP受体配体产生抗成瘾和不良副作用的机制。
相关文章
本文是关于阿片类药物:功能选择性新途径主题部分的一部分。要查看本部分的其他文章,请访问http://dx.doi.org/10.1111/bph.2015.172.issue-2。
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