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Developmentally-Dynamic Murine Brain Proteomes and Phosphoproteomes Revealed by Quantitative Proteomics

机译:定量蛋白质组学揭示发育动态的鼠脑蛋白质组和磷酸化蛋白质组。

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摘要

Developmental processes are governed by a diverse suite of signaling pathways employing reversible phosphorylation. Recent advances in large-scale phosphoproteomic methodologies have made possible the identification and quantification of hundreds to thousands of phosphorylation sites from primary tissues. Towards a global characterization of proteomic changes across brain development, we present the results of a large-scale quantitative mass spectrometry study comparing embryonic, newborn and adult murine brain. Using anti-phosphotyrosine immuno-affinity chromatography and strong cation exchange (SCX) chromatography, coupled to immobilized metal affinity chromatography (IMAC), we identified and quantified over 1,750 phosphorylation sites and over 1,300 proteins between three developmental states. Bioinformatic analyses highlight functions associated with the identified proteins and phosphoproteins and their enrichment at distinct developmental stages. These results serve as a primary reference resource and reveal dynamic developmental profiles of proteins and phosphoproteins from the developing murine brain.
机译:发育过程受采用可逆磷酸化作用的多种信号通路的支配。大规模磷酸化蛋白质组学方法学的最新进展使得鉴定和定量来自原始组织的数百至数千个磷酸化位点成为可能。为了对整个大脑发育中的蛋白质组学变化进行全球表征,我们提出了一项大规模定量质谱研究的结果,该研究比较了胚胎,新生和成年鼠脑。使用抗磷酸酪氨酸免疫亲和色谱和强阳离子交换(SCX)色谱,再结合固定金属亲和色谱(IMAC),我们鉴定并定量了三种发育状态之间的1,750多个磷酸化位点和1,300多种蛋白质。生物信息学分析突出了与鉴定出的蛋白质和磷蛋白相关的功能,以及它们在不同发育阶段的富集。这些结果作为主要参考资源,揭示了来自发育中的鼠脑的蛋白质和磷蛋白的动态发育概况。

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