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首页> 外文期刊>Biochemical and Biophysical Research Communications >Developmental genetic profiles of glutamate receptor system, neuromodulator system, protector of normal tissue and mitochondria, and reelin in marmoset cortex: Potential molecular mechanisms of pruning phase of spines in primate synaptic formation process during the end of infancy and prepuberty (II)
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Developmental genetic profiles of glutamate receptor system, neuromodulator system, protector of normal tissue and mitochondria, and reelin in marmoset cortex: Potential molecular mechanisms of pruning phase of spines in primate synaptic formation process during the end of infancy and prepuberty (II)

机译:mar猴皮层中谷氨酸受体系统,神经调节剂系统,正常组织和线粒体保护剂以及reelin的发育遗传概况:婴儿期和青春期结束时灵长类动物突触形成过程中棘的修剪阶段的潜在分子机制(II)

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This is the second report of a series paper, which reports molecular mechanisms underlying the occurrence of pruning spine phase after rapid spinogenesis phase in neonates and young infant in the primate brain. We performed microarray analysis between the peak of spine numbers [postnatal 3 months (M)] and spine pruning (postnatal 6 M) in prefrontal, inferior temporal, and primary visual cortices of the common marmoset (Callithrix jacchus). The pruning phase is not clearly defined in rodents but is in primates including the marmoset. The differentially expressed genes between 3 M and 6 M in all three cortical areas were selected by two-way analysis of variance. The list of selected genes was analyzed by canonical pathway analysis using "Ingenuity Pathway Analysis of complex omics data" (IPA; Ingenuity Systems, Qiagen, Hilden, Germany). In this report, we discuss these lists of genes for the glutamate receptor system, G-protein-coupled neuromodulator system, protector of normal tissue and mitochondria, and reelin. (1) Glutamate is a common neurotransmitter. Its receptors AMPA1, GRIK1, and their scaffold protein DLG4 decreased as spine numbers decreased. Instead, GRIN3 (NMDA receptor) increased, suggesting that strong NMDA excitatory currents may be required for a single neuron to receive sufficient net synaptic activity in order to compensate for the decrease in synapse. (2) Most of the G protein-coupled receptor genes (e.g., ADRA1D, HTR2A, HTR4, and DRD1) in the selected list were upregulated at 6 M. The downstream gene ROCK2 in these receptor systems plays a role of decreasing synapses, and ROCK2 decreased at 6 M. (3) Synaptic phagosytosis by microglia with complement and other cytokines could cause damage to normal tissue and mitochondria. SOD1, XIAP, CD46, and CD55, which play protective roles in normal tissue and mitochondria, showed higher expression at 6 M than at 3 M, suggesting that normal brain tissue is more protected at 6 M. (4) Reelin has an important role in cortical layer formation. In addition, RELN and three different pathways of reelin were expressed at 6 M, suggesting that new synapse formation decreased at that age. Moreover, if new synapses were formed, their positions were free and probably dependent on activity.
机译:这是该系列论文的第二份报告,该论文报告了在灵长类动物大脑中的新生婴儿和快速婴儿发生快速自旋形成阶段之后,修剪脊柱阶段发生的分子机制。我们在普通mar猴(Callithrix jacchus)的额叶,颞下叶和初级视皮层中的脊柱数目[产后3个月(M)]和脊柱修剪(产后6 M)之间进行了微阵列分析。修剪阶段在啮齿动物中没有明确定义,但在灵长类动物(包括mar猴)中定义。通过方差的双向分析,选择了所有三个皮质区域中3 M和6 M之间的差异表达基因。使用“复杂组学数据的Ingenuity Pathway Analysis”(IPA; Ingenuity Systems,Qiagen,Hilden,德国),通过规范途径分析来分析所选基因的列表。在这份报告中,我们讨论了谷氨酸受体系统,G蛋白偶联神经调节剂系统,正常组织和线粒体保护物以及reelin的这些基因清单。 (1)谷氨酸是一种常见的神经递质。随着脊柱数量的减少,其受体AMPA1,GRIK1及其支架蛋白DLG4也会减少。取而代之的是,GRIN3(NMDA受体)增加,表明单个神经元可能需要强大的NMDA兴奋性电流才能获得足够的净突触活性,以补偿突触的减少。 (2)所选清单中的大多数G蛋白偶联受体基因(例如ADRA1D,HTR2A,HTR4和DRD1)均在6 M上调。这些受体系统中的下游基因ROCK2起到减少突触的作用,并且ROCK2在6 M时下降。(3)小胶质细胞与补体和其他细胞因子的突触吞噬可能对正常组织和线粒体造成损害。在正常组织和线粒体中起保护作用的SOD1,XIAP,CD46和CD55在6M处的表达高于在3M处的表达,这表明正常脑组织在6M处受到更多的保护。(4)Reelin具有重要作用在皮层形成。此外,RELN和reelin的三种不同途径在6 M时表达,表明该年龄的新突触形成减少。而且,如果形成了新的突触,它们的位置是自由的,并且可能取决于活性。

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