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吗啡自我给药及消退过程中,Lewis大鼠和Fischer 344大鼠在多巴胺能受体调节方面的品系差异。

Strain differences between Lewis and Fischer 344 rats in the modulation of dopaminergic receptors after morphine self-administration and during extinction.

作者信息

Sánchez-Cardoso Pilar, Higuera-Matas Alejandro, Martín Sonsoles, Miguéns Miguel, Del Olmo Nuria, García-Lecumberri Carmen, Ambrosio Emilio

机构信息

Psychobiology Department, School of Psychology, UNED, C/Juan del Rosal no. 10, 28040 Madrid, Spain.

出版信息

Neuropharmacology. 2009 Jul;57(1):8-17. doi: 10.1016/j.neuropharm.2009.03.014. Epub 2009 Apr 17.

Abstract

The Lewis (LEW) and Fischer 344 (F344) rat strains have been used as a model to study genetic vulnerability to drug addiction and they differ in their dopaminergic systems. We have studied the variation in the D1-like and D2-like receptors in distinct brain regions of LEW and F344 rats that self-administered morphine (1 mg/kg) for 15 days and also after different extinction periods (3, 7 and 15 days). Under basal conditions, binding to D1-like receptors in the olfactory tubercle and substantia nigra, and to D2-like receptors in the Pyriform cortex and hippocampal-CA1 was lower in LEW rats than in F344 rats. Conversely, the LEW rats exhibited stronger D2-like binding in the caudate-putamen. In most brain regions there was a decrease in D1-like binding in LEW rats after self-administration while the F344 animals displayed an increment. Additionally, D2 receptors of LEW rats were down-regulated after self-administration in the caudate-putamen and in the nucleus accumbens (shell and core divisions). Binding to D1-like receptors increased in both strains in the early phases of extinction, while in the later stages a differential regulation was observed between both strains. During the early phases of extinction only F344 rats showed alterations in D2-like receptor binding, however in the latter phases a specific modulation occurred in both strains. These differences in basal D1-like and D2-like receptor binding, and their differential modulation after self-administration and during extinction, may be reflected in the greater vulnerability to opiate addiction shown by LEW strain.

摘要

刘易斯(LEW)大鼠和费希尔344(F344)大鼠品系已被用作研究药物成瘾遗传易感性的模型,它们的多巴胺能系统存在差异。我们研究了自行注射吗啡(1毫克/千克)15天以及在不同戒断期(3天、7天和15天)后,LEW大鼠和F344大鼠不同脑区中D1样和D2样受体的变化。在基础条件下,LEW大鼠嗅结节和黑质中与D1样受体的结合,以及梨状皮质和海马CA1区中与D2样受体的结合低于F344大鼠。相反,LEW大鼠尾状核-壳核中D2样结合更强。在大多数脑区,自行给药后LEW大鼠中D1样结合减少,而F344动物则增加。此外,LEW大鼠尾状核-壳核和伏隔核(壳部和核心部)中自行给药后D2受体下调。在戒断早期,两种品系中与D1样受体的结合均增加,而在后期观察到两种品系之间的差异调节。在戒断早期,只有F344大鼠的D2样受体结合发生改变,然而在后期,两种品系中均发生了特异性调节。基础D1样和D2样受体结合的这些差异,以及自行给药后和戒断期间的差异调节,可能反映在LEW品系对阿片类药物成瘾的更大易感性上。

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