首页> 外文期刊>Journal of biomolecular screening: The official journal of the Society for Biomolecular Screening >A high-content analysis toolbox permits dissection of diverse signaling pathways for t lymphocyte polarization
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A high-content analysis toolbox permits dissection of diverse signaling pathways for t lymphocyte polarization

机译:高含量的分析工具箱可剖析t淋巴细胞极化的多种信号通路

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RNA interfering (RNAi) screening strategies offer the potential to elucidate the signaling pathways that regulate integrin and adhesion receptor-mediated changes in T lymphocyte morphology. Of crucial importance, however, is the definition of key sets of parameters that will provide accurate, quantitative, and nonredundant information to flag relevant hits in such assays. In this study, the authors have used an image-based high-content analysis (HCA) technology platform and a panel of 24 pharmacological inhibitors, at a range of concentrations, to define key sets of parameters that enables sensitive and quantitative effects on integrin (LFA-1)-mediated lymphocyte morphology to be evaluated. In particular, multiparametric analysis of lymphocyte morphology that was based on intracellular staining of both the F-actin and α-tubulin cytoskeleton resulted in improved ability to discriminate morphological behavior compared to F-actin staining alone. Morphological and fluorescence intensity/distribution profiling of pharmacologically treated lymphocytes stimulated with integrin (LFA-1) and adhesion receptors (CD44) also revealed notable differences in their sensitivity to inhibitors. The assay described here may be used in HCA strategies such as RNAi screening assays to elucidate the signaling pathways and molecules that regulate integrin/adhesion receptor-mediated T lymphocyte polarization.
机译:RNA干扰(RNAi)筛选策略提供了阐明调节整联蛋白和粘附受体介导的T淋巴细胞形态变化的信号传导途径的潜力。但是,至关重要的是定义关键参数集,这些参数集将提供准确,定量和非冗余的信息以标记此类测定中的相关命中。在这项研究中,作者使用了基于图像的高含量分析(HCA)技术平台和一组24种浓度范围不同的药理抑制剂来定义关键参数集,以实现对整联蛋白的敏感和定量作用( LFA-1)介导的淋巴细胞形态进行评估。特别地,与单独的F-肌动蛋白染色相比,基于F-肌动蛋白和α-微管蛋白细胞骨架的细胞内染色的淋巴细胞形态多参数分析可提高识别形态行为的能力。用整联蛋白(LFA-1)和粘附受体(CD44)刺激的经药理处理的淋巴细胞的形态和荧光强度/分布图也显示出它们对抑制剂的敏感性有显着差异。本文描述的测定法可用于HCA策略(例如RNAi筛选测定法)中,以阐明调节整联蛋白/粘附受体介导的T淋巴细胞极化的信号传导途径和分子。

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