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对α4β2具有选择性但对α3β4或α7烟碱型受体无选择性的配体可推广至大鼠体内的尼古丁辨别刺激。

Ligands selective for alpha4beta2 but not alpha3beta4 or alpha7 nicotinic receptors generalise to the nicotine discriminative stimulus in the rat.

作者信息

Smith Janice W, Mogg Adrian, Tafi Elisiana, Peacey Eleanor, Pullar Ian A, Szekeres Philip, Tricklebank Mark

机构信息

Eli Lilly & Co Ltd, Lilly Research Centre, Sunninghill Road, Windlesham, Surrey, UK.

出版信息

Psychopharmacology (Berl). 2007 Feb;190(2):157-70. doi: 10.1007/s00213-006-0596-8. Epub 2006 Nov 18.

Abstract

RATIONALE

Nicotine produces behavioural effects that are potentially related to its interaction with diverse nicotinic acetylcholine receptor populations. Evidence from gene deletion studies suggests that the interoceptive stimulus properties of nicotine are mediated by heteromeric high-affinity receptors containing alpha4beta2 subunits. Mice lacking beta2 subunits do not discriminate nicotine (Shoaib et al., Neuropharmacology, 42:530-539, 2002), and nicotine does not elicit dopamine release in these animals (Grady et al., J Neurochem, 76:258-268, 2001). The stimulus properties of nicotine can be detected in rats using a two-lever operant drug discrimination paradigm, allowing them to be classified pharmacologically using ligands with selectivity for receptors containing alpha4beta2, alpha3beta4 or alpha7 subunits.

MATERIALS AND METHODS

Rats trained to discriminate 0.4 mg/kg nicotine from vehicle were given the nicotinic receptor agonists, cytisine, varenicline, TC2559, ABT-594, A-85380 (all having high affinity but varying selectivity for alpha4beta2-containing receptors), and WO 03/062224 and WO 01/60821A1 (selective for beta4- and alpha7-containing receptors, respectively). In separate studies, WO 03/062224 was used as the training stimulus.

RESULTS

Nicotine, TC-2559, A-85380 and ABT-594 showed dose-dependent and complete stimulus substitution, whilst WO 03/062224 and WO 01/60821A1 were completely without effect. Cytisine and varenicline showed partial generalisation, consistent with their partial agonist activity at nicotinic receptors eliciting dopamine release in rat striatal slices. After almost 50 training sessions with WO 03/062224, there was no clear evidence that an alpha3beta4 receptor agonist could sustain a discriminable stimulus.

CONCLUSION

Substitution to the nicotine discriminative stimulus required high-affinity and high intrinsic activity at beta2 but not at beta4- or at alpha7-containing nicotinic receptors.

摘要

原理

尼古丁产生的行为效应可能与其与多种烟碱型乙酰胆碱受体群体的相互作用有关。基因缺失研究的证据表明,尼古丁的内感受刺激特性由含有α4β2亚基的异源高亲和力受体介导。缺乏β2亚基的小鼠无法区分尼古丁(Shoaib等人,《神经药理学》,42:530 - 539,2002年),并且尼古丁在这些动物中不会引发多巴胺释放(Grady等人,《神经化学杂志》,76:258 - 268,2001年)。尼古丁的刺激特性可以在大鼠中使用双杠杆操作性药物辨别范式检测到,这使得它们能够使用对含有α4β2、α3β4或α7亚基的受体具有选择性的配体进行药理学分类。

材料与方法

对经过训练以区分0.4mg/kg尼古丁和溶剂的大鼠给予烟碱型受体激动剂,包括金雀花碱、伐尼克兰、TC2559、ABT - 594、A - 85380(所有这些对含有α4β2的受体具有高亲和力但选择性不同),以及WO 03/062224和WO 01/60821A1(分别对含有β4和α7的受体具有选择性)。在单独的研究中,WO 03/062224被用作训练刺激物。

结果

尼古丁、TC - 2559、A - 85380和ABT - 594表现出剂量依赖性和完全的刺激替代,而WO 03/062224和WO 01/60821A1则完全没有效果。金雀花碱和伐尼克兰表现出部分泛化,这与其在大鼠纹状体切片中引发多巴胺释放的烟碱型受体上的部分激动剂活性一致。在用WO 03/062224进行了近50次训练后,没有明确证据表明α3β4受体激动剂能够维持可辨别的刺激。

结论

替代尼古丁辨别刺激需要对含有β2但不是含有β4或α7的烟碱型受体具有高亲和力和高内在活性。

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