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Region-specific alterations of A-to-I RNA editing of serotonin 2c receptor in the cortex of suicides with major depression

机译:在具有重大抑郁症的自杀皮层中血清素2C受体的A-in-I RNA编辑的区域特异性改变

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Brain region-specific abnormalities in serotonergic transmission appear to underlie suicidal behavior. Alterations of RNA editing on the serotonin receptor 2C (HTR2C) pre-mRNA in the brain of suicides produce transcripts that attenuate 5-HT 2C R signaling by impairing intracellular G-protein coupling and subsequent intracellular signal transduction. In brain, the distribution of RNA-editing enzymes catalyzing deamination (A-to-I modification) shows regional variation, including within the cerebral cortex. We tested the hypothesis that altered pre-mRNA 5-HT 2C R receptor editing in suicide is region-specific. To this end, we investigated the complete 5-HT 2C R mRNA-editing profile in two architectonically distinct cortical areas involved in mood regulation and decision-making in a clinically well-characterized cohort of age- and sex-matched non-psychiatric drug-free controls and depressed suicides. By using an original biochemical detection method, that is, capillary electrophoresis single-stranded conformational polymorphism (CE-SSCP), we corroborated the 5-HT 2C R mRNA-editing profile previously described in the dorsolateral prefrontal cortex (Brodmann area 9 (BA9)). Editing of 5-HT 2C R mRNA displayed clear regional difference when comparing dorsolateral prefrontal cortex (BA9) and anterior cingulate cortex (BA24). Compared with non-psychiatric control individuals, alterations of editing levels of 5-HT2CR mRNA were detected in both cortical areas of depressed suicides. A marked increase in editing on 5-HT 2C R was especially observed in the anterior cingulate cortex in suicides, implicating this cortical area in suicide risk. The results suggest that region-specific changes in RNA editing of 5-HT 2C R mRNA and deficient receptor function likely contribute to the etiology of major depressive disorder or suicide.
机译:血清onerogic传播中的脑区特异性异常似乎是自杀行为的基础。在自杀脑中血清素受体2C(HTR2C)前mRNA对血清素受体2C(HTR2C)前mRNA的改变产生通过损害细胞内G-蛋白偶联和随后的细胞内信号转导进行5-HT 2C R信号传导的转录物。在大脑中,RNA编辑酶催化脱胺(A-TO-I改性)的分布显示区域变异,包括在脑皮层内。我们测试了在自杀中改变改变的预体5-HT 2C R受体的假设是特异性的。为此,我们调查了在临床和性匹配的非精神病毒群体中涉及情绪调节和决策中涉及情绪调节和决策的完整5-HT 2C R mRNA编辑配置文件。自由控制和抑郁的自杀。通过使用原始生化检测方法,即毛细管电泳单链构象多态性(CE-SSCP),我们在背侧前额叶皮质(Brodmann Area 9(Ba9)中先前描述了5-HT 2C R mRNA编辑型材)。在比较背侧前额叶皮质(BA9)和前铰接皮质(BA24)时,编辑5-HT 2C R mRNA显示出明确的区域差异。与非精神病毒对照个体相比,在抑制自杀的两种皮质区域中检测到5-HT2CR mRNA的编辑水平的改变。在自杀中的前铰接皮质中特别观察到5-HT 2C R的编辑的显着增加,暗示了这种皮质区域的自杀风险。结果表明,5-HT 2C R mRNA的RNA编辑的区域特异性变化和缺陷的受体功能可能有助于主要抑郁症或自杀的病因。

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