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Quantitative Proteomics in Laser Capture Microdissected Sleep Nuclei From Rat Brain

机译:激光捕获从大鼠脑中显微解剖的睡眠核中的定量蛋白质组学。

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摘要

The combination of stable isotope labeling of amino acids in mammals (SILAM) and laser capture microdissection (LCM) for selective proteomic analysis of the targeted tissues holds tremendous potential for refined characterization of proteome changes within complex tissues such as the brain. The authors have applied this approach to measure changes in relative protein abundance in ventral tegmental area (VTA) of the rat brain that correlate to pharmacological perturbations. Enriched 13C6 15N2-lysine was introduced in vivo via diet. These animals were sacrificed during the middle of the 12-hour light period to extract isotopically “heavy” proteins, which were then used as a reference for extracts from dosed, unlabeled rats. Animals were administered an orexin peptide (Ox-B), an orexin receptor antagonist (ORA), or a mixture of both (Ox-B + ORA). All samples were obtained at same phase of the sleep cycle. Labeled-pair identification and differential quantitation provided protein identification and expression ratio data. Five proteins were found to exhibit decreased relative abundance after administration of an ORA, including α-synuclein and rat myelin basic protein. Conversely, six proteins showed increased relative abundance upon antagonist treatment, including 2’,3’-cyclic nucleotide 3’-phosphodiesterase.
机译:哺乳动物中氨基酸的稳定同位素标记(SILAM)和激光捕获显微切割(LCM)的结合,用于对目标组织进行选择性蛋白质组学分析,具有对复杂组织(例如大脑)中的蛋白质组变化进行精确表征的巨大潜力。作者已经应用这种方法来测量大鼠脑腹侧被盖区(VTA)中相对蛋白丰度的变化,该变化与药理学扰动有关。通过饮食将富集的 13 C6 15 N2-赖氨酸引入体内。在12小时光照中途将这些动物处死,以提取同位素“重”蛋白,然后将其用作未剂量大鼠的提取物的参考。给动物施用了orexin肽(Ox-B),orexin受体拮抗剂(ORA)或两者的混合物(Ox-B + ORA)。所有样品均在睡眠周期的相同阶段获得。标记对鉴定和差异定量提供了蛋白质鉴定和表达比数据。发现施用ORA后有5种蛋白质的相对丰度降低,其中包括α-突触核蛋白和大鼠髓鞘碱性蛋白。相反,在拮抗药处理后,六种蛋白质显示出相对丰度增加,包括2',3'-环核苷酸3'-磷酸二酯酶。

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