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组织学染色方法与激光捕获显微切割脑样本蛋白质组分析的不兼容性。

Lack of compatibility of histological staining methods with proteomic analysis of laser-capture microdissected brain samples.

作者信息

Mouledous Lionel, Hunt Sybille, Harcourt Rebecca, Harry Jenny L, Williams Keith L, Gutstein Howard B

机构信息

Department of Anesthesiology, M. D. Anderson Cancer Center, Houston, TX 77030, USA.

出版信息

J Biomol Tech. 2002 Dec;13(4):258-64.

Abstract

The anatomical complexity of the brain presents a challenge for the analysis of changes in gene and protein expression. Laser-capture microdissection (LCM) is a technique that is precise enough to dissect single cells within a tissue section. Protein expression in tissues obtained by LCM has been studied by Western blot and two-dimensional (2D) gel electrophoresis. However, it is not known whether histological staining techniques interfere with protein recovery and resolution on 2D gels. The goal of this study was to determine the effects of staining procedures on protein extraction and separation. LCM samples of rat brain striatum obtained after histological staining were compared with unstained, LCM-captured tissue and fresh-frozen, unstained, manually dissected samples. Specimens subsequently underwent protein extraction and 2D gel electrophoresis under identical conditions. Our results indicated that histological staining of the tissue greatly reduced protein recovery from LCM-captured samples. However, fixation and LCM without histological staining did not significantly affect protein recovery from brain tissue. These results indicate that LCM of fixed, unstained brain tissue could be used to dissect discrete brain regions for proteomic analysis. Histological staining of neural tissue should be avoided, because it interferes with protein recovery. LCM appears to be a promising tool for the study of localized protein changes underlying brain plasticity.

摘要

大脑的解剖结构复杂性给基因和蛋白质表达变化的分析带来了挑战。激光捕获显微切割(LCM)是一种精确到足以在组织切片内分离单个细胞的技术。通过蛋白质印迹法和二维(2D)凝胶电泳对LCM获得的组织中的蛋白质表达进行了研究。然而,尚不清楚组织学染色技术是否会干扰蛋白质在二维凝胶上的回收和分辨率。本研究的目的是确定染色程序对蛋白质提取和分离的影响。将组织学染色后获得的大鼠脑纹状体LCM样本与未染色的LCM捕获组织以及新鲜冷冻、未染色的手工解剖样本进行比较。随后,样本在相同条件下进行蛋白质提取和二维凝胶电泳。我们的结果表明,组织的组织学染色大大降低了LCM捕获样本中的蛋白质回收率。然而,未经组织学染色的固定和LCM对脑组织中的蛋白质回收率没有显著影响。这些结果表明,固定的、未染色的脑组织的LCM可用于解剖离散的脑区进行蛋白质组学分析。应避免对神经组织进行组织学染色,因为它会干扰蛋白质回收。LCM似乎是研究大脑可塑性潜在局部蛋白质变化的一个有前途的工具。

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