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Integrating Retinoic Acid Signaling With Brain Function

机译:维甲酸信号与脑功能整合

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The vitamin A derivative retinoic acid (RA) regulates the transcription of about a 6th of the human genome. Compelling evidence indicates a role of RA in cognitive activities, but its integration with the molecular mechanisms of higher brain functions is not known. Here we describe the properties of RA signaling in the mouse, which point to unknown means through which RA actions are modified and reinforced at selected brain sites. The locations of RA signaling for the developing dorsal forebrain undergo slow, gradual changes over the life cycle except for two brief periods of accelerated shifts, which coincide with periods of enhanced developmental vulnerability. In the functional cerebral cortex, RA signaling delineates regions with immature, plastic neuronal characteristics, within which the expression of hundreds of genes is differentially regulated. Many of these are involved in neuronal ligand-receptor interactions and signaling cascades for activity dependent gene expression. We propose that RA functions in the brain by contributing topographical information and life cycle changes to combinatorial transcrip_tional mechanisms and that in the postnatal cortex RA signaling designates domains of modifiable neuronal circuitry.
机译:维生素A衍生物视黄酸(RA)调节人类基因组约六分之一的转录。有说服力的证据表明RA在认知活动中的作用,但其与更高脑功能的分子机制的整合尚不清楚。在这里,我们描述了小鼠中RA信号传导的特性,指出了未知的手段,通过该手段,RA行为可以在选定的大脑部位进行修饰和增强。发育中的背侧前脑的RA信号的位置在整个生命周期中会经历缓慢,逐渐的变化,除了两个短暂的加速转变期,这与发育脆弱性增强期相吻合。在功能性大脑皮层中,RA信号描绘了具有不成熟的可塑性神经元特征的区域,其中数百种基因的表达受到差异调节。这些中的许多都参与神经元配体-受体的相互作用和信号转导级联的活动依赖基因表达。我们建议RA通过提供地形信息和生命周期变化来促进组合转录机制,从而在大脑中发挥功能,而在产后皮层中RA信号指示可修饰神经元回路域。

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