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可卡因对心理遗传选择的罗马高回避和低回避大鼠的终纹床核和前额叶皮质细胞核中细胞外信号调节激酶磷酸化的不同影响。

Differential effects of cocaine on extracellular signal-regulated kinase phosphorylation in nuclei of the extended amygdala and prefrontal cortex of psychogenetically selected Roman high- and low-avoidance rats.

作者信息

Giorgi Osvaldo, Corda Maria G, Sabariego Marta, Giugliano Valentina, Piludu Maria A, Rosas Michela, Acquas Elio

机构信息

Department of Life and Environmental Sciences, University of Cagliari, Cagliari, Italy.

出版信息

J Neurosci Res. 2015 May;93(5):714-21. doi: 10.1002/jnr.23526. Epub 2014 Dec 11.

DOI:10.1002/jnr.23526
PMID:25502299
Abstract

Roman high (RHA)- and low (RLA)-avoidance rats are selectively bred for rapid vs. poor acquisition of active avoidance, respectively, and differ markedly in emotional reactivity, coping style, and behavioral and neurochemical responses to morphine and psychostimulants. Accordingly, acute cocaine induces more robust increments in locomotion and dopamine output in the nucleus accumbens shell (AcbSh) of RHA than of RLA rats. Cocaine induces short- and long-term neuronal plasticity via activation of the extracellular signal-regulated kinase (ERK) pathway. This study compares the effects of acute cocaine on ERK phosphorylation (pERK) in limbic brain areas of Roman rats. In RHA but not RLA rats, cocaine (5 mg/kg) increased pERK in the infralimbic prefrontal cortex and AcbSh, two areas involved in its acute effects, but did not modify pERK in the prelimbic prefrontal cortex and Acb core, which mediate the chronic effects of cocaine. Moreover, cocaine failed to affect pERK immunolabeling in the bed nucleus of stria terminalis pars lateralis and central amygdala of either line but increased it in the basolateral amygdala of RLA rats. These results extend to pERK expression previous findings on the greater sensitivity to acute cocaine of RHA vs. RLA rats and confirm the notion that genetic factors influence the differential responses of the Roman lines to addictive drugs. Moreover, they support the view that the Roman lines are a useful tool to investigate the molecular underpinnings of individual vulnerability to drug addiction.

摘要

罗马高回避(RHA)和低回避(RLA)大鼠分别被选择性培育,以实现主动回避的快速获得与较差获得,它们在情绪反应性、应对方式以及对吗啡和精神兴奋剂的行为和神经化学反应方面存在显著差异。相应地,急性给予可卡因会使RHA大鼠伏隔核壳(AcbSh)中的运动和多巴胺输出增加幅度比RLA大鼠更大。可卡因通过激活细胞外信号调节激酶(ERK)途径诱导短期和长期的神经元可塑性。本研究比较了急性给予可卡因对罗马大鼠边缘脑区ERK磷酸化(pERK)的影响。在RHA大鼠而非RLA大鼠中,可卡因(5毫克/千克)增加了参与其急性效应的两个区域——眶下前额叶皮质和AcbSh中的pERK,但未改变介导可卡因慢性效应的前额叶皮质前边缘区和Acb核心中的pERK。此外,可卡因对两品系大鼠的终纹床核外侧部和中央杏仁核中的pERK免疫标记均无影响,但增加了RLA大鼠基底外侧杏仁核中的pERK。这些结果将之前关于RHA大鼠比RLA大鼠对急性可卡因更敏感的研究结果扩展到了pERK表达,并证实了遗传因素影响罗马品系对成瘾药物的不同反应这一观点。此外,它们支持了罗马品系是研究个体对药物成瘾易感性分子基础的有用工具这一观点。

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