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首页> 外文期刊>Journal of psychiatric research >Expression of dopamine signaling genes in the post-mortem brain of individuals with mental illnesses is moderated by body mass index and mediated by insulin signaling genes
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Expression of dopamine signaling genes in the post-mortem brain of individuals with mental illnesses is moderated by body mass index and mediated by insulin signaling genes

机译:用精神疾病的个体后致癌的多巴胺信号传导基因的表达受到体重指数的调节,并通过胰岛素信号传导基因介导

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Preclinical studies implicate insulin signaling as a modulator of dopamine transmission, but human data is currently limited. We hypothesize that changes in the expression of insulin receptor-related genes in the postmortem brain tissue of patients with mood and psychotic disorders mediate the expression of dopamine regulation-related genes. From a database containing microarray data from the post-mortem dorsolateral prefrontal cortex (dlPFC) (healthy controls [HC]: n = 209; patients: n = 321) and hippocampus (HC: n = 180; patients: n = 196), we conducted a hypothesis-driven analysis through the a priori selection of 12 dopamine- and 3 insulin-related genes. Mediation and moderated mediation models, accounting for the role of body mass index (BMI), were used. In the dlPFC, expressions of insulin receptor- and dopamine regulation-related genes were moderated by BMI, with significantly lower expression in high BMI patients. In the hippocampus, there were significantly lower expressions of these genes, which were not moderated by BMI. Illnesses by BMI effects on expression of dopamine genes were fully mediated by expression of insulin receptor gene (INSR). Analysis of conditional indirect effects showed interactions between INSR and BMI, indicating significantly stronger indirect effects at higher BMI values. In the hippocampus we observed that expression of insulin receptor substrate 1 and 2 fully mediated the effects of illnesses on expression of dopamine genes. In conclusion, differential expression of dopamine-related genes was related to altered expression of insulin signaling genes. BMI had region-specific effects, supporting the hypothesis that metabolic systems are critical mediators of dopaminergic function.
机译:临床前研究将胰岛素信令暗示为多巴胺传输的调节剂,但人类数据目前有限。我们假设情绪和精神病疾病患者患者脑后脑组织表达的变化介绍了多巴胺调节相关基因的表达。从包含来自后验尸背面前额外皮层(DLPFC)的微阵列数据的数据库(健康对照[HC]:n = 209;患者:n = 321)和海马(HC:n = 180;患者:n = 196),通过优先选择12多巴胺和3个胰岛素相关基因进行假设驱动分析。使用调解和适度的中介模型,占体重指数(BMI)的作用。在DLPFC中,BMI调节胰岛素受体和多巴胺调节相关基因的表达,在高BMI患者中具有显着降低的表达。在海马中,这些基因的表达显着下降,这些基因的表达不受BMI调节。通过表达胰岛素受体基因(INSR),完全介导BMI对多巴胺基因表达的疾病。条件间接效应分析显示INSR和BMI之间的相互作用,表明在较高的BMI值下显着强烈的间接效应。在海马中,我们观察到胰岛素受体基质1和2的表达完全介导疾病对多巴胺基因表达的影响。总之,多巴胺相关基因的差异表达与胰岛素信号传导基因的改变表达有关。 BMI具有特定于地区的效果,支持代谢系统是多巴胺能功能的关键介质的假设。

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