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Single-cell gene expression profiling reveals functional heterogeneity of undifferentiated human epidermal cells

机译:单细胞基因表达谱揭示未分化的人类表皮细胞的功能异质性

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SUMMARY Human epidermal stem cells express high levels of β1 integrins, delta-like 1 (DLL1) and the EGFR antagonist LRIG1. However, there is cell-to-cell variation in the relative abundance of DLL1 and LRIG1 mRNA transcripts. Single-cell global gene expression profiling showed that undifferentiated cells fell into two clusters delineated by expression of DLL1 and its binding partner syntenin. The DLL1+ cluster had elevated expression of genes associated with endocytosis, integrin-mediated adhesion and receptor tyrosine kinase signaling. Differentially expressed genes were not independently regulated, as overexpression of DLL1 alone or together with LRIG1 led to the upregulation of other genes in the DLL1+ cluster. Overexpression of DLL1 and LRIG1 resulted in enhanced extracellular matrix adhesion and increased caveolin-dependent EGFR endocytosis. Further characterisation of CD46, one of the genes upregulated in the DLL1+ cluster, revealed it to be a novel cell surface marker of human epidermal stem cells. Cells with high endogenous levels of CD46 expressed high levels of β1 integrin and DLL1 and were highly adhesive and clonogenic. Knockdown of CD46 decreased proliferative potential and β1 integrin-mediated adhesion. Thus, the previously unknown heterogeneity revealed by our studies results in differences in the interaction of undifferentiated basal keratinocytes with their environment.
机译:发明内容人表皮干细胞表达高水平的β1整联蛋白,δ样1(DLL1)和EGFR拮抗剂LRIG1。但是,DLL1和LRIG1 mRNA转录本的相对丰度存在细胞间差异。单细胞全局基因表达谱分析表明未分化的细胞分为两个簇,由DLL1及其结合伴侣syntenin的表达描绘。 DLL1 +簇具有与胞吞作用,整联蛋白介导的粘附和受体酪氨酸激酶信号转导相关的基因表达升高。不能单独调节差异表达的基因,因为单独的DLL1或与LRIG1一起过表达会导致DLL1 +簇中其他基因的上调。 DLL1和LRIG1的过表达导致细胞外基质粘附增强和小孔蛋白依赖性EGFR内吞作用增加。 CD46是DLL1 +簇中上调的基因之一,其进一步表征表明它是人表皮干细胞的新型细胞表面标记。具有高内源性CD46的细胞表达高水平的β1整联蛋白和DLL1,并且具有高度粘附性和克隆性。击倒CD46降低了增殖潜能和β1整合素介导的粘附。因此,我们的研究揭示了先前未知的异质性,导致未分化的基底角质形成细胞与其环境相互作用的差异。

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