胆管上皮产生肝祖细胞。
The biliary epithelium gives rise to liver progenitor cells.
作者信息
Rodrigo-Torres Daniel, Affò Silvia, Coll Mar, Morales-Ibanez Oriol, Millán Cristina, Blaya Delia, Alvarez-Guaita Anna, Rentero Carles, Lozano Juan José, Maestro Miguel Angel, Solar Myriam, Arroyo Vicente, Caballería Joan, van Grunsven Leo A, Enrich Carlos, Ginès Pere, Bataller Ramon, Sancho-Bru Pau
机构信息
Liver Unit, Hospital Clínic, Institut d'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), University of Barcelona, Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBERehd), Barcelona, Spain.
出版信息
Hepatology. 2014 Oct;60(4):1367-77. doi: 10.1002/hep.27078. Epub 2014 Aug 21.
UNLABELLED
Severe liver diseases are characterized by expansion of liver progenitor cells (LPC), which correlates with disease severity. However, the origin and role of LPC in liver physiology and in hepatic injury remains a contentious topic. We found that ductular reaction cells in human cirrhotic livers express hepatocyte nuclear factor 1 homeobox B (HNF1β). However, HNF1β expression was not present in newly generated epithelial cell adhesion molecule (EpCAM)-positive hepatocytes. In order to investigate the role of HNF1β-expressing cells we used a tamoxifen-inducible Hnf1βCreER/R26R(Yfp/LacZ) mouse to lineage-trace Hnf1β(+) biliary duct cells and to assess their contribution to LPC expansion and hepatocyte generation. Lineage tracing demonstrated no contribution of HNF1β(+) cells to hepatocytes during liver homeostasis in healthy mice or after loss of liver mass. After acute acetaminophen or carbon tetrachloride injury no contribution of HNF1β(+) cells to hepatocyte was detected. We next assessed the contribution of Hnf1β(+) -derived cells following two liver injury models with LPC expansion, a diethoxycarbonyl-1,4-dihydro-collidin (DDC)-diet and a choline-deficient ethionine-supplemented (CDE)-diet. The contribution of Hnf1β(+) cells to liver regeneration was dependent on the liver injury model. While no contribution was observed after DDC-diet treatment, mice fed with a CDE-diet showed a small population of hepatocytes derived from Hnf1β(+) cells that were expanded to 1.86% of total hepatocytes after injury recovery. Genome-wide expression profile of Hnf1β(+) -derived cells from the DDC and CDE models indicated that no contribution of LPC to hepatocytes was associated with LPC expression of genes related to telomere maintenance, inflammation, and chemokine signaling pathways.
CONCLUSION
HNF1β(+) biliary duct cells are the origin of LPC. HNF1β(+) cells do not contribute to hepatocyte turnover in the healthy liver, but after certain liver injury, they can differentiate to hepatocytes contributing to liver regeneration.
未标记
严重肝脏疾病的特征是肝祖细胞(LPC)扩增,这与疾病严重程度相关。然而,LPC在肝脏生理学和肝损伤中的起源及作用仍是一个有争议的话题。我们发现,人类肝硬化肝脏中的小胆管反应细胞表达肝细胞核因子1同源框B(HNF1β)。然而,新生成的上皮细胞黏附分子(EpCAM)阳性肝细胞中不存在HNF1β表达。为了研究表达HNF1β的细胞的作用,我们使用了他莫昔芬诱导型Hnf1βCreER/R26R(Yfp/LacZ)小鼠来对Hnf1β(+)胆管细胞进行谱系追踪,并评估它们对LPC扩增和肝细胞生成的贡献。谱系追踪表明,在健康小鼠的肝脏稳态期间或肝实质损失后,HNF1β(+)细胞对肝细胞没有贡献。在急性对乙酰氨基酚或四氯化碳损伤后,未检测到HNF1β(+)细胞对肝细胞有贡献。接下来,我们在两种伴有LPC扩增的肝损伤模型,即二乙氧基羰基-1,4-二氢可力丁(DDC)饮食和胆碱缺乏乙硫氨酸补充(CDE)饮食后,评估了Hnf1β(+)衍生细胞的贡献。Hnf1β(+)细胞对肝脏再生的贡献取决于肝损伤模型。在DDC饮食处理后未观察到贡献,而喂食CDE饮食的小鼠显示有一小部分肝细胞来源于Hnf1β(+)细胞,在损伤恢复后这些细胞扩增至占总肝细胞的1.86%。来自DDC和CDE模型的Hnf1β(+)衍生细胞的全基因组表达谱表明,LPC对肝细胞无贡献与LPC中与端粒维持、炎症和趋化因子信号通路相关基因的表达有关。
结论
HNF1β(+)胆管细胞是LPC的起源。HNF1β(+)细胞在健康肝脏中对肝细胞更新无贡献,但在某些肝损伤后,它们可分化为肝细胞,有助于肝脏再生。
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