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氯氮平增加了社交隔离大鼠几个脑区的 c-Fos 蛋白表达。

Clozapine increased c-Fos protein expression in several brain subregions of socially isolated rats.

机构信息

Laboratory of Molecular Biology and Endocrinology, Institute of Nuclear Sciences "Vinča", University of Belgrade, 11001 Belgrade, Serbia.

Institute of Psychopharmacology, Central Institute of Mental Health, Medical Faculty Mannheim, Heidelberg University, Mannheim 68159, Germany.

出版信息

Brain Res Bull. 2019 Oct;152:35-44. doi: 10.1016/j.brainresbull.2019.07.005. Epub 2019 Jul 9.

Abstract

Chronic social stress and/or pharmacological treatments differentially modulate the expression of c-Fos, a marker of neuronal activity, in subregions of the rat brain. Here, we examined the effect of the atypical antipsychotic Clozapine (Clz) (20 mg/kg/day for 3 weeks) on the neuronal activation pattern of c-Fos protein expression in stress-relevant brain subregions of adult male Wistar rats exposed to chronic social isolation (CSIS: 3 weeks), an animal model of depression and schizophrenia, and controls. The protein expression of c-Fos was also used to map neuronal populations in brain subregions activated by CSIS alone. Subregions which showed significantly increased c-Fos protein expression following CSIS included the retrosplenial cortex (RSC), (subregions:RSC granular cortex, c region (RSGc) and dysgranular (RSD)), dentate gyrus, dorsal (DGd), paraventricular thalamic nucleus, posterior part (PVP), lateral (LA)/basolateral (BL) complex of amygdala, caudate putamen (CPu) and accumbens nucleus, shell (AcbSh). Increases in c-Fos protein expression in the RSGc, RSD, DGd, PVP, LA/BL complex of amygdala and striatum (CPu, Acb Core (AcbC) and AcbSh) following Clz treatment in controls were found. Clz applied simultaneously with CSIS modulated neuronal activity in CPu, AcbC and AcbSh subregions compared to CSIS alone, increasing c-Fos protein expression. Furthermore, Clz revealed synergistic effects with CSIS in the CA1d and PVP. These identified neural circuits reflect brain subregions activated following CSIS and/or Clz administration. These data further contribute to the understanding of the effectiveness of Clz in the modulation of brain subregion activation in response to CSIS.

摘要

慢性社会压力和/或药物治疗可差异调节神经元活性标志物 c-Fos 在大鼠脑区中的表达。在这里,我们研究了非典型抗精神病药氯氮平(Clz)(20mg/kg/天,持续 3 周)对慢性社会隔离(CSIS:3 周)暴露的成年雄性 Wistar 大鼠应激相关脑区中 c-Fos 蛋白表达的神经元激活模式的影响,CSIS 是一种抑郁和精神分裂症的动物模型,以及对照组。c-Fos 蛋白的表达也用于绘制 CSIS 单独激活的脑区中的神经元群体图谱。CSIS 后 c-Fos 蛋白表达显著增加的脑区包括后穹窿皮质(RSC)(亚区:RSC 颗粒皮质、c 区(RSGc)和颗粒减少(RSD))、齿状回、背侧(DGd)、室旁丘脑核、后部分(PVP)、杏仁核外侧/基底外侧(LA/BL)复合体、尾状核壳部(CPu)和伏隔核壳部(AcbSh)。在对照组中,Clz 治疗后 RSGc、RSD、DGd、PVP、LA/BL 复合体和纹状体(CPu、Acb 核心(AcbC)和 AcbSh)中的 c-Fos 蛋白表达增加。CSIS 同时应用 Clz 可调节 CPu、AcbC 和 AcbSh 亚区的神经元活性,增加 c-Fos 蛋白表达。此外,Clz 与 CSIS 一起在 CA1d 和 PVP 中显示出协同作用。这些鉴定的神经回路反映了 CSIS 后和/或 Clz 给药后激活的脑区。这些数据进一步有助于理解 Clz 调节 CSIS 后脑区激活的有效性。

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