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Single cell analysis of human foetal liver captures the transcriptional profile of hepatobiliary hybrid progenitors

机译:人类胎儿肝脏的单细胞分析捕获了肝胆杂种祖细胞的转录谱

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摘要

The liver parenchyma is composed of hepatocytes and bile duct epithelial cells (BECs). Controversy exists regarding the cellular origin of human liver parenchymal tissue generation during embryonic development, homeostasis or repair. Here we report the existence of a hepatobiliary hybrid progenitor (HHyP) population in human foetal liver using single-cell RNA sequencing. HHyPs are anatomically restricted to the ductal plate of foetal liver and maintain a transcriptional profile distinct from foetal hepatocytes, mature hepatocytes and mature BECs. In addition, molecular heterogeneity within the EpCAM+ population of freshly isolated foetal and adult human liver identifies diverse gene expression signatures of hepatic and biliary lineage potential. Finally, we FACS isolate foetal HHyPs and confirm their hybrid progenitor phenotype in vivo. Our study suggests that hepatobiliary progenitor cells previously identified in mice also exist in humans, and can be distinguished from other parenchymal populations, including mature BECs, by distinct gene expression profiles.
机译:肝实质由肝细胞和胆管上皮细胞(BEC)组成。关于胚胎发育,体内平衡或修复过程中人类肝实质组织生成的细胞起源存在争议。在这里,我们报告使用单细胞RNA测序在人类胎儿肝脏中存在肝胆杂种祖细胞(HHyP)。 HHyPs在解剖学上仅限于胎儿肝的导管板,并维持不同于胎儿肝细胞,成熟肝细胞和成熟BEC的转录谱。此外,在新鲜分离的胎儿和成年人类肝脏的EpCAM + 群体中的分子异质性鉴定了肝和胆道谱系潜能的多种基因表达特征。最后,我们通过FACS分离出胎儿HHyPs,并在体内确认其杂交祖细胞表型。我们的研究表明,先前在小鼠中鉴定出的肝胆祖细胞也存在于人类中,并且可以通过独特的基因表达谱与其他实质人群(包括成熟的BEC)区分开。

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