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Cocaine-induced metabolic activation in cortico-limbic circuitry is increased after exposure to the histone deacetylase inhibitor, sodium butyrate

机译:暴露于组蛋白去乙酰化酶抑制剂丁酸钠后,可卡因诱导的皮质 - 边缘电路中的代谢活化增加

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摘要

Drug-induced inhibition of histone deacetylase (HDAC) results in the modification of many behavioral changes resulting from exposure to cocaine and other stimulant drugs-of-abuse, but a comprehensive map of the neuronal circuitries involved is lacking. The present study used blood-oxygen-level-dependent functional magnetic resonance imaging (BOLD fMRI) in awake rats to determine the effects of the HDAC inhibitor, sodium butyrate (SBt) on brain metabolic activation patterns during the initial stage of repeated cocaine administration. Three groups of rats received cocaine during BOLD fMRI, (i) acutely for the first time, or pretreated for 2 days with either (ii) saline or (iii) SBt 30 min prior to cocaine. Acute but not repeated exposure to cocaine resulted in widespread BOLD activation in fore- and mid-brain. Pretreatment with SBt restored BOLD signals in the forebrain after repeated cocaine exposure, including a pronounced activation in the anterior thalamus, the hippocampus/amygdala and various portions of limbic and sensory cortex. Mesocorticolimbic areas showed a similar trend, but did not reach statistical significance. These findings suggest that HDACi modulation after repeated stimulant exposure involves cortico-limbic circuitry regulating emotion, motivation and memory.
机译:药物诱导的组蛋白脱乙酰基酶(HDAC)抑制作用导致许多行为变化的改变,这些行为变化是由于接触可卡因和其他刺激性滥用药物而引起的,但是缺乏所涉及的神经元回路的全面图谱。本研究在清醒大鼠中使用了血氧水平依赖性功能磁共振成像(BOLD fMRI),以确定可卡因重复给药初始阶段中HDAC抑制剂丁酸钠(SBt)对脑代谢活化模式的影响。三组大鼠在BOLD fMRI期间接受可卡因,(i)首次急性接受,或在可卡因之前30分钟用(ii)盐水或(iii)SBt预处理2天。急性但不反复暴露于可卡因导致前脑和中脑广泛的BOLD活化。反复暴露于可卡因后,SBt预处理可恢复前脑的BOLD信号,包括前丘脑,海马/杏仁核以及边缘和感觉皮层各部分的明显激活。中皮质皮质区显示出类似的趋势,但未达到统计学意义。这些发现表明,反复刺激暴露后的HDACi调节涉及调节情绪,动机和记忆的皮质-边缘电路。

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