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烟碱型乙酰胆碱受体 α4β2* 正变构调节剂 NS9283 对尼古丁辨别大鼠的辨别性刺激效应。

Discriminative-stimulus effects of NS9283, a nicotinic α4β2* positive allosteric modulator, in nicotine-discriminating rats.

机构信息

Neuroscience Drug Discovery, AbbVie, 1 N. Waukegan Rd., Bldg AP-9A, North Chicago, IL, 60064-6125, USA,

出版信息

Psychopharmacology (Berl). 2014 Jan;231(1):67-74. doi: 10.1007/s00213-013-3207-5. Epub 2013 Aug 8.

Abstract

RATIONALE

Neuronal α4β2* nicotinic acetylcholine receptors mediate cognition, pain, and the discriminative and reinforcing effects of nicotine. In addition to traditional orthosteric agonists, α4β2* positive allosteric modulators (PAMs) have recently been identified. With increased subtype selectivity relative to agonists, PAMs administered alone or in combination with low-dose α4β2* agonists may be used as powerful tools for increasing our understanding of α4β2* pharmacology.

OBJECTIVES

The present experiments tested the nicotine discriminative-stimulus effects of the α4β2* PAM NS9283 (A-969933) in the presence and absence of low-dose nicotine or nicotinic subtype-selective agonist.

METHODS

Rats were trained to discriminate 0.4 mg/kg nicotine from saline in a two-lever drug discrimination paradigm. In subsequent generalization tests, rats were administered nicotine, the α4β2*-preferring agonist ABT-594, and NS9283, alone or in two-drug combinations.

RESULTS

Nicotine and ABT-594 showed dose-dependent nicotine generalization. NS9283 alone resulted in a non-significant increase in nicotine-appropriate lever selection. Combination of non-effective doses of nicotine or ABT-594 with escalating doses of NS9283 resulted in a complete conversion to 100 % nicotine-appropriate choice in the case of nicotine combination and incomplete, though significant, generalization for ABT-594.

CONCLUSIONS

The α4β2* PAM NS9283 alone did not produce nicotine-like discriminative effects, but did demonstrate dose-related increases in nicotine lever choice when combined with a non-effective dose of nicotine or the α4β2* agonist ABT-594. This finding provides confirmation of the positive allosteric modulating effect of NS9283 in a functional in vivo paradigm. NS9283 is a potentially valuable tool for studying the role of α4β2* receptors in various nicotinic acetylcholine receptor-related functions.

摘要

原理

神经元 α4β2* 烟碱型乙酰胆碱受体介导认知、疼痛以及尼古丁的辨别和强化效应。除了传统的正构激动剂之外,最近还发现了 α4β2* 正变构调节剂 (PAM)。与激动剂相比,PAM 具有更高的亚型选择性,单独使用或与低剂量 α4β2* 激动剂联合使用,可能被用作增强我们对 α4β2* 药理学理解的有力工具。

目的

本实验检测了 α4β2* PAM NS9283(A-969933)在低剂量尼古丁或烟碱型选择性激动剂存在或不存在的情况下对尼古丁辨别刺激的影响。

方法

大鼠在双杠药物辨别范式中接受 0.4mg/kg 尼古丁和生理盐水的辨别训练。在随后的概括测试中,大鼠单独给予尼古丁、α4β2*-选择性激动剂 ABT-594 和 NS9283,或联合给予两种药物。

结果

尼古丁和 ABT-594 表现出剂量依赖性的尼古丁概括。NS9283 单独使用会导致尼古丁适当选择的非显著增加。非有效剂量的尼古丁或 ABT-594 与逐渐增加的 NS9283 剂量联合使用,会导致在尼古丁联合的情况下完全转化为 100%尼古丁适当选择,而 ABT-594 的概括不完全,但具有显著意义。

结论

单独使用 α4β2* PAM NS9283 不会产生类似尼古丁的辨别效应,但与非有效剂量的尼古丁或 α4β2* 激动剂 ABT-594 联合使用时,确实会导致尼古丁杠杆选择的剂量相关性增加。这一发现为 NS9283 在功能性体内范式中的正变构调节作用提供了确认。NS9283 是研究各种烟碱型乙酰胆碱受体相关功能中 α4β2* 受体作用的潜在有价值工具。

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