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Uncovering the Proteome Response of the Master Circadian Clock to Light Using an AutoProteome System

机译:使用自动蛋白质组系统发现生物钟主生物钟对光的响应

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摘要

In mammals, the suprachiasmatic nucleus (SCN) is the central circadian pacemaker that governs rhythmic fluctuations in behavior and physiology in a 24-hr cycle and synchronizes them to the external environment by daily resetting in response to light. The bilateral SCN is comprised of a mere ∼20,000 neurons serving as cellular oscillators, a fact that has, until now, hindered the systematic study of the SCN on a global proteome level. Here we developed a fully automated and integrated proteomics platform, termed AutoProteome system, for an in-depth analysis of the light-responsive proteome of the murine SCN. All requisite steps for a large-scale proteomic study, including preconcentration, buffer exchanging, reduction, alkylation, digestion and online two-dimensional liquid chromatography-tandem MS analysis, are performed automatically on a standard liquid chromatography-MS system. As low as 2 ng of model protein bovine serum albumin and up to 20 μg and 200 μg of SCN proteins can be readily processed and analyzed by this system. From the SCN tissue of a single mouse, we were able to confidently identify 2131 proteins, of which 387 were light-regulated based on a spectral counts quantification approach. Bioinformatics analysis of the light-inducible proteins reveals their diverse distribution in different canonical pathways and their heavy connection in 19 protein interaction networks. The AutoProteome system identified vasopressin-neurophysin 2-copeptin and casein kinase 1 delta, both of which had been previously implicated in clock timing processes, as light-inducible proteins in the SCN. Ras-specific guanine nucleotide-releasing factor 1, ubiquitin protein ligase E3A, and X-linked ubiquitin specific protease 9, none of which had previously been implicated in SCN clock timing processes, were also identified in this study as light-inducible proteins. The AutoProteome system opens a new avenue to systematically explore the proteome-wide events that occur in the SCN, either in response to light or other stimuli, or as a consequence of its intrinsic pacemaker capacity.
机译:在哺乳动物中,视交叉上核(SCN)是中央昼夜节律起搏器,可控制行为和生理的节律性波动,并在24小时周期内通过每天对光的响应使其与外部环境同步。双边SCN仅由约20,000个神经元组成,充当细胞振荡器,这一事实直到现在仍阻碍了在全球蛋白质组学水平上对SCN的系统研究。在这里,我们开发了一个称为AutoProteome系统的全自动集成蛋白质组学平台,用于对鼠SCN的光响应蛋白质组进行深入分析。大规模蛋白质组学研究的所有必要步骤,包括预浓缩,交换缓冲液,还原,烷基化,消化和在线二维液相色谱-串联质谱分析,均在标准液相色谱-MS系统上自动执行。该系统可轻松处理低至2 ng的模型蛋白牛血清白蛋白以及多达20μg和200μg的SCN蛋白。从一只小鼠的SCN组织中,我们能够自信地鉴定出2131种蛋白质,其中387种是根据光谱计数定量方法进行光调节的。对光诱导蛋白的生物信息学分析表明,它们在不同的经典途径中具有多种分布,在19种蛋白相互作用网络中具有紧密的联系。 AutoProteome系统将血管加压素-神经素2-肽素和酪蛋白激酶1δ识别为SCN中的光诱导性蛋白,而这两种蛋白先前都与时钟计时过程有关。 Ras特异性鸟嘌呤核苷酸释放因子1,泛素蛋白连接酶E3A和X联结的泛素特异性蛋白酶9,以前均未涉及SCN时钟时序过程,在本研究中也被鉴定为光诱导蛋白。 AutoProteome系统打开了一条新途径,可以系统地探索SCN中发生的整个蛋白质组范围的事件,这些事件是对光或其他刺激的响应,或者是其固有的起搏器功能所致。

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