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Identification of Protein Network Alterations upon Retinal Ischemia-Reperfusion Injury by Quantitative Proteomics Using a Rattus norvegicus Model

机译:视网膜缺血再灌注损伤后的蛋白质网络变化的定量蛋白质组学使用褐家鼠模型。

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摘要

Retinal ischemia is a common feature associated with several ocular diseases, including diabetic retinopathy. In this study, we investigated the effect of a retinal ischemia and reperfusion (I/R) injury on protein levels via a quantitative shotgun strategy using stable isotope dimethyl labeling combined with LC-MS/MS analysis. Based on the relative quantitation data of 1088 proteins, 234 proteins showed a greater than 1.5-fold change following I/R injury, 194 of which were up-regulated and 40 were down-regulated. Gene ontology analysis revealed that after I/R injury, there was an increase in the metabolic-process related proteins but a decline in cell communication, system process and transport-related proteins. A ribosome protein network and a secreted protein network consisting of many protease inhibitors were identified among the up-regulated proteins, despite a suppression of the mammalian target of rapamycin (mTOR) pathway following the I/R injury. A synaptic-related protein network was found to be significantly down-regulated, implicating a functional reduction of neurons following a retinal I/R injury. Our results provide new systems-biology clues for the study of retinal ischemia.
机译:视网膜缺血是与包括糖尿病性视网膜病在内的几种眼疾病有关的共同特征。在这项研究中,我们使用稳定的同位素二甲基标记结合LC-MS / MS分析,通过定量shot弹枪策略研究了视网膜缺血和再灌注(I / R)损伤对蛋白质水平的影响。根据1088种蛋白质的相对定量数据,234种蛋白质在I / R损伤后显示出大于1.5倍的变化,其中194种上调而40种下调。基因本体分析显示,I / R损伤后,代谢过程相关蛋白增加,但细胞通讯,系统过程和运​​输相关蛋白下降。尽管在I / R损伤后抑制了雷帕霉素(mTOR)途径的哺乳动物靶标,但在上调的蛋白中鉴定出了由许多蛋白酶抑制剂组成的核糖体蛋白网络和分泌蛋白网络。发现与突触相关的蛋白质网络明显下调,暗示视网膜I / R损伤后神经元的功能减少。我们的结果为视网膜缺血的研究提供了新的系统生物学线索。

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