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Dissecting alterations in human CD8+T cells with aging by high-dimensional single cell mass cytometry

机译:通过高尺寸单细胞质量细胞术抑制人CD8 + T细胞的改变

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摘要

We investigated the effect of aging on the multi-dimensional characteristics and heterogeneity of human peripheral CD8(+) T cells defined by the expression of a set of molecules at the single cell level using the recently developed mass cytometry or Cytometry by Time-Of-Flight (CyTOF) and computational algorithms. CD8(+) T cells of young and older adults had differential expression of molecules, especially those related to cell activation and migration, permitting the clustering of young and older adults through an unbiased approach. The changes in the expression of individual molecules were collectively reflected in the altered high-dimensional profiles of CD8(+) T cells in older adults as visualized by the dimensionality reduction analysis tools principal component analysis (PCA) and t-distributed stochastic neighbor embedding (t-SNE). A combination of PhenoGraph clustering and t-SNE analysis revealed heterogeneous subsets of CD8(+) T cells that altered with aging. Furthermore, intermolecular quantitative relationships in CD8(+) T cells appeared to change with age as determined by the computational algorithm conditional-Density Resampled Estimate of Mutual Information (DREMI). The results of our study showed that heterogeneity, multidimensional characteristics, and intermolecular quantitative relationships in human CD8(+) T cells altered with age, distinctively clustering young and older adults through an unbiased approach.
机译:我们研究了使用最近显影的质量细胞术或通过时间的单细胞水平在单个细胞水平下的一组分子表达定义的人周围CD8(+)T细胞的多维特征和异质性的影响。飞行(Cytof)和计算算法。年轻人和老年人的CD8(+)T细胞具有分子的差异表达,尤其是与细胞激活和迁移有关的差异,允许通过无偏见的方法聚类年轻和老年人。各个分子表达的变化在老年人的CD8(+)T细胞的改变的高分子谱中统称为由维度降低分析工具主成分分析(PCA)和T分布式随机邻居嵌入( t-sne)。现实表聚类和T-SNE分析的组合揭示了随老化改变的CD8(+)T细胞的异质亚基。此外,CD8(+)T细胞中的分子间定量关系似乎随着通过计算算法条件密度重采采样估计的计算算法(DREMI)确定的年龄而变化。我们的研究结果表明,人CD8(+)T细胞中的异质性,多维特征和分子间定量关系随着年龄,独特的青少年成年人通过无偏见的方法而改变。

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