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青少年大鼠反复给予哌甲酯治疗后皮质纹状体回路中基因诱导的失调:对zif 268和homer 1a的不同影响。

Dysregulation of gene induction in corticostriatal circuits after repeated methylphenidate treatment in adolescent rats: differential effects on zif 268 and homer 1a.

作者信息

Cotterly Lindsay, Beverley Joel A, Yano Motoyo, Steiner Heinz

机构信息

Department of Cellular and Molecular Pharmacology, Rosalind Franklin University of Medicine and Science/The Chicago Medical School, 3333 Green Bay Road, North Chicago, IL 60064, USA.

出版信息

Eur J Neurosci. 2007 Jun;25(12):3617-28. doi: 10.1111/j.1460-9568.2007.05570.x.

Abstract

Psychostimulants and other dopamine agonists produce molecular changes in neurons of cortico-basal ganglia-cortical circuits, and such neuronal changes are implicated in behavioural disorders. Methylphenidate, a psychostimulant that causes dopamine overflow (among other effects), alters gene regulation in neurons of the striatum. The present study compared the effects of acute and repeated methylphenidate treatment on cortical and striatal gene regulation in adolescent rats. Changes in the expression of the immediate-early genes zif 268 and homer 1a were mapped in 23 striatal sectors and 22 cortical areas that provide input to these striatal sectors, in order to determine whether specific corticostriatal circuits were affected by these treatments. Acute administration of methylphenidate (5 mg/kg, i.p.) produced modest zif 268 induction in cortical areas. These cortical zif 268 responses were correlated in magnitude with zif 268 induction in functionally related striatal sectors. In contrast, after repeated methylphenidate treatment (10 mg/kg, 7 days), cortical and striatal gene induction were dissociated. In these animals, the methylphenidate challenge (5 mg/kg) produced significantly greater gene induction (zif 268 and homer 1a) in the cortex. This enhanced response was widespread but regionally selective, as it occurred predominantly in premotor, motor and somatosensory cortical areas. At the same time, striatal gene induction was partly suppressed (zif 268) or unchanged (homer 1a). Thus, repeated methylphenidate treatment disrupted the normally coordinated gene activation patterns in cortical and striatal nodes of corticostriatal circuits. This drug-induced dissociation in cortical and striatal functioning was associated with enhanced levels of behavioural stereotypies, suggesting disrupted motor switching function.

摘要

精神兴奋剂和其他多巴胺激动剂会在皮质-基底神经节-皮质回路的神经元中产生分子变化,而这种神经元变化与行为障碍有关。哌醋甲酯是一种能引起多巴胺溢出(还有其他作用)的精神兴奋剂,它会改变纹状体神经元中的基因调控。本研究比较了急性和重复给予哌醋甲酯对青春期大鼠皮质和纹状体基因调控的影响。即刻早期基因zif 268和homer 1a表达的变化被定位在23个纹状体区域以及为这些纹状体区域提供输入的22个皮质区域,以确定特定的皮质纹状体回路是否受到这些处理的影响。急性给予哌醋甲酯(5毫克/千克,腹腔注射)在皮质区域产生了适度的zif 268诱导。这些皮质zif 268反应在幅度上与功能相关纹状体区域的zif 268诱导相关。相比之下,在重复给予哌醋甲酯处理(10毫克/千克,7天)后,皮质和纹状体基因诱导出现了分离。在这些动物中,哌醋甲酯激发(5毫克/千克)在皮质中产生了显著更强的基因诱导(zif 268和homer 1a)。这种增强的反应很广泛但具有区域选择性,因为它主要发生在前运动、运动和体感皮质区域。与此同时,纹状体基因诱导部分受到抑制(zif 268)或未改变(homer 1a)。因此,重复给予哌醋甲酯处理破坏了皮质纹状体回路皮质和纹状体节点中正常协调的基因激活模式。这种药物诱导的皮质和纹状体功能分离与行为刻板水平的提高有关,提示运动转换功能受到破坏。

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