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定量免疫电子显微镜术:评估金标记亚细胞模式的替代方法。

Quantitative immunoelectron microscopy: alternative ways of assessing subcellular patterns of gold labeling.

作者信息

Mayhew Terry M

机构信息

Centre for Integrated System Biology and Medicine, School of Biomedical Sciences and Institute of Clinical Research, University of Nottingham, UK.

出版信息

Methods Mol Biol. 2007;369:309-29. doi: 10.1007/978-1-59745-294-6_15.

Abstract

Using antibodies conjugated with colloidal gold particles, immunoelectron microscopy permits the high-resolution detection, localization, and quantification of one or more defined antigens in cellular compartments. These benefits reflect the properties of gold particles (they are electron dense, punctate, and available in different sizes) and the ability of transmission electron microscopy to resolve both particles and compartments. By relating gold marker to cellular fine structure and by taking into account the study design, three pertinent questions can be addressed. When studying a particular group of cells, we might ask: "What is the spatial distribution of gold particles between compartments within a group of cells?" and/or "Is the spatial distribution of gold particles within a group of cells random or due to preferential labeling of compartments?" When comparing two or more groups, a relevant question is: "Are there shifts in compartment labeling distributions in different groups of cells?" Recently, new ways of testing these basic questions have been developed. The efficiency and validity of all these methods rely on sampling, stereological, and statistical tools. Key processes include random selection of items at each sampling stage (specimen blocks, microscopical fields, etc.), stereological morphometry and/or unbiased counting, and statistical evaluation of a suitable null hypothesis (no difference in labeling between compartments or groups). This chapter reviews these new methods and illustrates their application with a consistent dataset.

摘要

利用与胶体金颗粒偶联的抗体,免疫电子显微镜能够在细胞区室中对一种或多种特定抗原进行高分辨率检测、定位和定量。这些优势反映了金颗粒的特性(电子密度高、呈点状且有不同尺寸)以及透射电子显微镜分辨颗粒和区室的能力。通过将金标记与细胞精细结构相关联并考虑研究设计,可以解决三个相关问题。在研究特定的一组细胞时,我们可能会问:“一组细胞内不同区室之间金颗粒的空间分布是怎样的?”和/或“一组细胞内金颗粒的空间分布是随机的还是由于区室的优先标记?”在比较两组或更多组时,一个相关问题是:“不同组细胞中区室标记分布是否有变化?”最近,已经开发出了测试这些基本问题的新方法。所有这些方法的效率和有效性都依赖于抽样、体视学和统计工具。关键步骤包括在每个抽样阶段(标本块、显微镜视野等)随机选择样本、体视形态测量和/或无偏计数,以及对合适的零假设(区室或组之间标记无差异)进行统计评估。本章回顾了这些新方法,并用一个一致的数据集展示了它们的应用。

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