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Spatiotemporal expression profiling of proteins in rat sciatic nerve regeneration using reverse phase protein arrays

机译:使用反相蛋白质阵列的大鼠坐骨神经再生中蛋白质的时空表达谱

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Background Protein expression profiles throughout 28 days of peripheral nerve regeneration were characterized using an established rat sciatic nerve transection injury model. Reverse phase protein microarrays were used to identify the spatial and temporal expression profile of multiple proteins implicated in peripheral nerve regeneration including growth factors, extracellular matrix proteins, and proteins involved in adhesion and migration. This high-throughput approach enabled the simultaneous analysis of 3,360 samples on a nitrocellulose-coated slide. Results The extracellular matrix proteins collagen I and III, laminin gamma-1, fibronectin, nidogen and versican displayed an early increase in protein levels in the guide and proximal sections of the regenerating nerve with levels at or above the baseline expression of intact nerve by the end of the 28 day experimental course. The 28 day protein levels were also at or above baseline in the distal segment however an early increase was only noted for laminin, nidogen, and fibronectin. While the level of epidermal growth factor, ciliary neurotrophic factor and fibroblast growth factor-1 and -2 increased throughout the experimental course in the proximal and distal segments, nerve growth factor only increased in the distal segment and fibroblast growth factor-1 and -2 and nerve growth factor were the only proteins in that group to show an early increase in the guide contents. As expected, several proteins involved in cell adhesion and motility; namely focal adhesion kinase, N-cadherin and β-catenin increased earlier in the proximal and distal segments than in the guide contents reflecting the relatively acellular matrix of the early regenerate. Conclusions In this study we identified changes in expression of multiple proteins over time linked to regeneration of the rat sciatic nerve both demonstrating the utility of reverse phase protein arrays in nerve regeneration research and revealing a detailed, composite spatiotemporal expression profile of peripheral nerve regeneration.
机译:使用已建立的大鼠坐骨神经横断损伤模型来表征整个周围神经再生28天的蛋白表达谱。反相蛋白质微阵列用于鉴定与周围神经再生有关的多种蛋白质的时空表达谱,包括生长因子,细胞外基质蛋白质以及参与粘附和迁移的蛋白质。这种高通量方法可以在硝酸纤维素涂层载玻片上同时分析3360个样品。结果胞外基质蛋白I和III胶原,层粘连蛋白gamma-1,纤连蛋白,尼达根和versican在新生神经的引导区和近端区显示出早期蛋白质水平的升高,其水平等于或高于完整神经基线表达的水平。 28天实验课程结束。 28天的蛋白质水平在远端节段也达到或高于基线,但是仅注意到层粘连蛋白,尼古丁和纤连蛋白的早期增加。在整个实验过程中,近端和远端部分的表皮生长因子,睫状神经营养因子和成纤维细胞生长因子-1和-2的水平增加,而神经生长因子仅在远端部分和成纤维细胞生长因子-1和-2的水平增加神经生长因子和神经生长因子是该组中唯一显示早期含量增加的蛋白质。如预期的那样,几种蛋白质参与细胞粘附和运动。即粘着斑激酶,N-钙粘着蛋白和β-连环蛋白在近端和远端节段中的增加比指导内容中的早,反映了早期再生的相对无细胞基质。结论在这项研究中,我们确定了与大鼠坐骨神经再生相关的多种蛋白质表达随时间的变化,既表明了反相蛋白质阵列在神经再生研究中的实用性,又揭示了周围神经再生的详细的复合时空表达谱。

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