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DNA chip technology in brain banks: confronting a degrading world.

机译:脑库中的DNA芯片技术:面对一个日益恶化的世界。

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DNA microarray technology is based on the principle of hybridization between 2 complementary strands of nucleic acids, one being fixed into a solid membrane, the other being the sample to analyze. This has resulted in a very powerful method to examine differential gene expression between samples, and has been widely used in the study of tumors. The application of DNA microarray technology to the study of the nervous system has to consider several properties of the nervous tissue: composition of various neuronal types, as well as astrocytes, oligodendrocytes, and microglia; regional and area differences; developmental and age-dependent variations; and functional and pathological status. Moreover, human samples are usually obtained postmortem following variable agonal periods and postmortem delays between death and tissue preservation, which are accompanied by variable RNA degradation. Yet human postmortem nervous tissue stored in brain banks offers a unique opportunity to facilitate material for the study of diseases of the nervous system and to gain direct understanding on the mechanisms of disease. This review analyzes the application of DNA microarray technology to current practice using brain-banked tissues in order to recognize and minimize sub-optimal processing of brain samples and to correct pitfalls due to inadequate procedures. Also discussed are RNA preservation and RNA degradation effects on expression pattern assessments, analysis of individual versus pooled samples, array normalization, types of DNA chip platforms, whole genomic analysis versus specialized chips, and microgenomics. Minimizing RNA degradation and improving detection of resistant RNA in postmortem brain has been considered in detail in order to improve the efficiency and reliability of DNA microarray technology employed in the study of human postmortem nervous tissue.
机译:DNA微阵列技术基于两条核酸互补链之间的杂交原理,一条固定在固体膜上,另一条固定在待分析的样品上。这导致了一种非常有效的方法来检查样品之间的差异基因表达,并已被广泛用于肿瘤研究中。 DNA微阵列技术在神经系统研究中的应用必须考虑神经组织的几种特性:各种神经元类型的组成,以及星形胶质细胞,少突胶质细胞和小胶质细胞;地区和地区差异;发育和年龄相关的变异;以及功能和病理状态。而且,人类样品通常在不同的痛楚期和死亡与组织保存之间的死后延迟之后进行死后采集,这伴随有可变的RNA降解。然而,储存在脑库中的人体尸体神经组织提供了一个独特的机会,可以促进研究神经系统疾病的材料并获得对疾病机制的直接了解。这篇综述分析了DNA微阵列技术在当前使用脑库组织的实践中的应用,以便识别和最小化对脑样本的次优处理,并纠正由于程序不足而导致的陷阱。还讨论了RNA保留和RNA降解对表达模式评估,单个样品与合并样品的分析,阵列归一化,DNA芯片平台的类型,完整基因组分析与专用芯片的比较以及微基因组学。为了提高在人类死后神经组织研究中使用的DNA微阵列技术的效率和可靠性,已经详细考虑了最小化RNA降解并改善死后大脑中抗性RNA的检测。

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