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Single-cell transcriptomics reveals the landscape of intra-tumoral heterogeneity and sternness-related subpopulations in liver cancer

机译:单细胞转录组学揭示了肝癌中肿瘤内异质性和沉默群的景观

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摘要

Hepatocellular carcinoma (HCC) is heterogeneous, rendering its current curative treatments ineffective. The emergence of single-cell genomics represents a powerful strategy in delineating the complex molecular landscapes of cancers. In this study, we demonstrated the feasibility and merit of using single-cell RNA sequencing to dissect the intra-tumoral heterogeneity and analyze the single-cell transcriptomic landscape to detect rare cell subpopulations of significance. Exploration of the inter-relationship among liver cancer stem cell markers showed two distinct major cell populations according to EPCAM expression, and the EPCAM+ cells had upre-gulated expression of multiple oncogenes. We also identified a CD24+/CD44+-enriched cell subpopulation within the EPCAM+ cells which had specific signature genes and might indicate a novel sternness-related cell subclone in HCC. Notably, knockdown of signature gene CTSE for CD24+/CD44+ cells significantly reduced self-renewal ability on HCC cells in vitro and the sternness-related role of CTSE was further confirmed by in vivo tumorigenicity assays in nude mice. In summary, single-cell genomics is a useful tool to delineate HCC in-tratumoral heterogeneity at better resolution. It can identify rare but important cell subpopulations, and may guide better precision medicine in the long run.
机译:肝细胞癌(HCC)是异质的,使其目前的治疗方法无效。单细胞基因组学的出现是划清划清复杂的癌症的复杂分子景观的强大策略。在这项研究中,我们证明了使用单细胞RNA测序的可行性和优点来描述肿瘤内异质性并分析单细胞转录组景观以检测稀有细胞群的重要性。肝癌干细胞标志物之间的关系探索显示了根据EPCAM表达的两个不同的主要细胞群,EPCAM +细胞具有多种癌基因的umbord-gulated表达。我们还鉴定了具有特异性签名基因的EPCAM +细胞内的CD24 + / CD44 + - 细胞群,并且可以表明HCC中的新型胸部相关细胞亚克隆。值得注意的是,用于CD24 + / CD44 +细胞的签名基因CTSE的敲低显着降低了在体外HCC细胞上的自我更新能力,并且通过在裸鼠的体内致瘤性测定中进一步证实了CTSE的损伤相关作用。总之,单细胞基因组学是一种以更好的分辨率描绘HCC In-TraTumoral异质性的有用工具。它可以识别罕见但重要的细胞群,并可从长远来看引导更好的精确药。

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