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A microfluidic platform enabling single-cell RNA-seq of multigenerational lineages

机译:一种微流体平台,可实现多代谱系的单细胞RNa-seq

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摘要

We introduce a microfluidic platform that enables off-chip single-cell RNA-seq after multi-generational lineage tracking under controlled culture conditions. We use this platform to generate whole-transcriptome profiles of primary, activated murine CD8+ T-cell and lymphocytic leukemia cell line lineages. Here we report that both cell types have greater intra- than inter-lineage transcriptional similarity. For CD8+ T-cells, genes with functional annotation relating to lymphocyte differentiation and function—including Granzyme B—are enriched among the genes that demonstrate greater intra-lineage expression level similarity. Analysis of gene expression covariance with matched measurements of time since division reveals cell type-specific transcriptional signatures that correspond with cell cycle progression. We believe that the ability to directly measure the effects of lineage and cell cycle-dependent transcriptional profiles of single cells will be broadly useful to fields where heterogeneous populations of cells display distinct clonal trajectories, including immunology, cancer, and developmental biology.
机译:我们介绍了一种微流体平台,该平台可在受控培养条件下进行多代谱系跟踪后实现芯片外单细胞RNA-seq。我们使用这个平台来生成原代,激活的鼠CD8 + T细胞和淋巴细胞性白血病细胞系的完整转录组图谱。在这里我们报告这两种细胞类型具有更大的内部比谱系间的转录相似性。对于CD8 + T细胞,在具有更高的谱系内表达水平相似性的基因中富集了具有与淋巴细胞分化和功能相关的功能注释的基因,包括GranzymeB。自分裂以来,对基因表达的协方差进行了时间匹配的分析,揭示了与细胞周期进程相对应的特定细胞类型的转录特征。我们认为,直接测量单个细胞的谱系和细胞周期依赖性转录谱的影响的能力将广泛用于异质细胞群体显示不同克隆轨迹(包括免疫学,癌症和发育生物学)的领域。

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