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Quantitative profiling of regional protein expression in rat retina after partial optic nerve transection using fluorescence difference two-dimensional gel electrophoresis

机译:荧光差异二维凝胶电泳定量分析部分视神经横断后大鼠视网膜区域蛋白表达的定量分析

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摘要

To examine the difference between primary and secondary retinal ganglion cell (RGC) degeneration, the protein expression at four regions of retina including superior, temporal, inferior and nasal quadrant in a rat model of partial optic nerve transection (pONT) using 2-D Fluorescence Difference Gel Electrophoresis (DIGE) were investigated. Unilateral pONT was performed on the temporal side of optic nerves of adult Wistar rats to separate primary and secondary RGC loss. Topographical quantification of RGCs labeled by Rbpms antibody and analysis of axonal injury by grading of optic nerve damage at 1 week (n=8) and 8 weeks (n=15) after pONT demonstrated early RGC loss at temporal region, which is considered as primary RGC degeneration and progressing RGC loss at nasal region, which is considered as secondary RGC degeneration. Early protein expression in each retinal quadrant (n=4) at 2 weeks after pONT was compared with the corresponding quadrant in the contralateral control eye by DIGE. For all comparisons, 24 differentially expressed proteins (>1.2-fold; P<0.05; ≥3 non-duplicated peptide matches) were identified by mass spectrometry (MS). Interestingly, in the nasal retina, serum albumin and members of crystallin family, including αA, αB, βA2, βA3, βB2 and γS indicating stress response were upregulated. By contrast, only αB and βA2 crystallin proteins were altered in temporal quadrant. In the superior and inferior quadrants, βB2 crystallin, keratin type I, S-arrestin and lamin-B1 were upregulated, while heat shock cognate 71 kDa protein and heterogeneous nuclear ribonucleoproteins A2/B1 were downregulated. In summary, the use of DIGE followed by MS is useful to detect early regional protein regulation in the retina after localized optic nerve injury.
机译:为了研究视网膜神经节细胞退化与继发性视网膜神经节细胞退化之间的差异,使用二维荧光在大鼠部分视神经横断(pONT)模型中在视网膜的四个区域(包括上,颞,下和鼻象限)表达蛋白质研究了差异凝胶电泳(DIGE)。在成年Wistar大鼠视神经的颞侧进行单侧pONT,以分离原发性和继发性RGC损失。 pONT后第1周(n = 8)和第8周(n = 15)时,用Rbpms抗体标记的RGC的地形定量和通过视神经损伤的分级对轴突损伤进行分析,表明颞区早期RGC丢失,这被认为是主要的RGC变性和鼻腔区域不断进行的RGC丧失,被认为是继发性RGC变性。通过DIGE将pONT后2周时每个视网膜象限(n = 4)中的早期蛋白质表达与对侧对照眼中的相应象限进行比较。对于所有比较,通过质谱(MS)鉴定了24种差异表达的蛋白质(> 1.2倍; P <0.05;≥3个非重复的肽段匹配)。有趣的是,在鼻视网膜中,血清白蛋白和结晶蛋白家族成员,包括指示应激反应的αA,αB,βA2,βA3,βB2和γS上调。相比之下,颞象限中只有αB和βA2晶体蛋白被改变。在上,下象限中,βB2晶状蛋白,I型角蛋白,S-arrestin和lamin-B1上调,而热休克同源的71 kDa蛋白和异核核糖核蛋白A2 / B1下调。总之,在局部视神经损伤后,使用DIGE继之MS可用于检测视网膜的早期区域蛋白调节。

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