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Cerebral oxidative metabolism mapping in four genetic mouse models of anxiety and mood disorders

机译:四种遗传小鼠模型焦虑和情绪障碍的脑氧化代谢映射

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The psychopathology of depression is highly complex and the outcome of studies on animal models is divergent. In order to find brain regions that could be metabolically distinctively active across a variety of mouse depression models and to compare the interconnectivity of brain regions of wild-type and such genetically modified mice, histochemical mapping of oxidative metabolism was performed by the measurement of cytochrome oxidase activity. We included mice with the heterozygous knockout of the vesicular glutamate transporter (VGLUT(1)(-/+)), full knockout of the cannabinoid 1 receptor (CB1(-/-)), an anti-sense knockdown of the gluco- corticoid receptor (GRi) and overexpression of the human 5-hydroxytryptamine transporter (h5-HTT). Altogether 76 mouse brains were studied to measure oxidative metabolism in one hundred brain regions, and the obtained dataset was submitted to a variety of machine learning algorithms and multidimensional scaling. Overall, the top brain regions having the largest contribution to classification into depression model were the lateroanterior hypothalamic nucleus, the anterior part of the basomedial amygdaloid nucleus, claustrum, the suprachiasmatic nucleus, the ventromedial hypothalamic nucleus, and the anterior hypothalamic area. In terms of the patterns of inter-regional relationship between wild-type and genetically modified mice there was little overall difference, while the most deviating brain regions were cortical amygdala and ventrolateral and ventral posteromedial thalamic nuclei. The GRi mice that most clearly differed from their controls exhibited deviation of connectivity for a number of brain regions, such as ventrolateral thalamic nucleus, the intermediate part of the lateral septal nucleus, the anteriodorsal part of the medial amygdaloid nucleus, the medial division of the central amygdaloid nucleus, ventral pallidum, nucleus of the vertical limb of the diagonal band, anteroventral parts of the thalamic nucleus and parts of the bed nucleus of the stria terminalis. Conclusively, the GRi mouse model was characterized by changes in the functional connectivity of the extended amygdala and stress response circuits.
机译:抑郁症的精神病理学非常复杂,动物模型的研究结果发散。为了找到可以在各种小鼠抑制模型中进行代谢上独立活性的脑区域,并比较野生型和这种遗传修饰小鼠的脑区域的互连,通过测量细胞色素氧化酶进行氧化代谢的组织化学映射活动。我们包括具有杂质谷氨酸转运蛋白(Vglut(1)( - / +)),大麻素1受体的全敲除(CB1( - / - )),葡萄糖敲低的小鼠受体(GRI)和人5-羟基特胺转运蛋白(H5-HTT)的过表达。研究了76种鼠标脑中的血液脑在一百个脑区域测量氧化代谢,并且所获得的数据集提交给各种机器学习算法和多维缩放。总的来说,对抑郁模型的分类具有最大贡献的顶部脑区是横钙质丘脑,基础乳腺髓核,猫梗死的前部,短暂的下丘脑核和前丘脑区域的前部。就野生型和遗传修饰小鼠之间的区域间关系的模式而言,总体差异很小,而最偏离的脑区是皮质杏仁菌和腹侧和腹侧后肌瘤核核。从其控制中最清晰地不同的GRI小鼠表现出与许多脑区的连接性偏差,例如腹侧丘脑核,侧面隔膜核的中间部分,内侧杏仁核的翼状胬肉部分,内侧分裂中央杏仁核,腹侧裂隙,垂直肢体的垂直肢体的核,丘脑核的胎肾上腺核和椎间核核的部分。结论,GRI小鼠模型的特征在于扩展Amygdala和应力响应电路的功能性连通性的变化。

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