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首页> 外文期刊>The journal of immunology >An Integrated Workflow To Assess Technical and Biological Variability of Cell Population Frequencies in Human Peripheral Blood by Flow Cytometry
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An Integrated Workflow To Assess Technical and Biological Variability of Cell Population Frequencies in Human Peripheral Blood by Flow Cytometry

机译:通过流式细胞术评估人外周血中细胞群体频率的技术和生物变异性的集成工作流程

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In the context of large-scale human system immunology studies, controlling for technical and biological variability is crucial to ensure that experimental data support research conclusions. In this study, we report on a universal workflow to evaluate both technical and biological variation in multiparameter flow cytometry, applied to the development of a 10-color panel to identify all major cell populations and T cell subsets in cryopreserved PBMC. Replicate runs from a control donation and comparison of different gating strategies assessed the technical variability associated with each cell population and permitted the calculation of a quality control score. Applying our panel to a large collection of PBMC samples, we found that most cell populations showed low intraindividual variability over time. In contrast, certain subpopulations such as CD56 T cells and Temra CD4 T cells were associated with high interindividual variability. Age but not gender had a significant effect on the frequency of several populations, with a drastic decrease in naive T cells observed in older donors. Ethnicity also influenced a significant proportion of immune cell population frequencies, emphasizing the need to account for these covariates in immune profiling studies. We also exemplify the usefulness of our workflow by identifying a novel cell-subset signature of latent tuberculosis infection. Thus, our study provides a universal workflow to establish and evaluate any flow cytometry panel in systems immunology studies.
机译:在大规模人类系统免疫学研究的背景下,控制技术和生物变异性对于确保实验数据支持研究结论至关重要。在这项研究中,我们报告了一个通用的工作流程,以评估多参数流式细胞术中的技术和生物学差异,该技术应用于开发10色面板以鉴定冷冻保存的PBMC中的所有主要细胞群和T细胞亚群。从对照捐赠中进行重复运行,比较不同的门控策略,评估与每个细胞群体相关的技术变异性,并计算质量控制得分。将我们的小组应用于大量的PBMC样本中,我们发现大多数细胞群体随时间的变化显示出较低的个体差异。相反,某些亚群,例如CD56 T细胞和Temra CD4 T细胞与个体之间的高变异性相关。年龄而非性别对几个人群的频率有重大影响,在较老的供体中观察到的幼稚T细胞急剧下降。种族也影响了很大比例的免疫细胞群频率,强调需要在免疫谱研究中考虑这些协变量。我们还通过鉴定潜伏性结核感染的新型细胞亚基来例证我们工作流程的有用性。因此,我们的研究提供了建立和评估系统免疫学研究中任何流式细胞仪专家组的通用工作流程。

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