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在慢性肝损伤的小鼠中,反应性胆管细胞可分化为增殖的肝细胞,并具有有效的 DNA 修复能力。

Reactive cholangiocytes differentiate into proliferative hepatocytes with efficient DNA repair in mice with chronic liver injury.

机构信息

Laboratory of Hepato-gastroenterology, Institut de Recherche Expérimentale et Clinique, Université catholique de Louvain, Brussels, Belgium.

Liver Cell Biology Laboratory, Vrije Universiteit Brussels (VUB), Brussels, Belgium.

出版信息

J Hepatol. 2019 Jun;70(6):1180-1191. doi: 10.1016/j.jhep.2019.02.003. Epub 2019 Feb 20.

Abstract

BACKGROUND & AIM: Chronic liver diseases are characterized by expansion of the small immature cholangiocytes - a mechanism named ductular reaction (DR) - which have the capacity to differentiate into hepatocytes. We investigated the kinetics of this differentiation, as well as analyzing several important features of the newly formed hepatocytes, such as functional maturity, clonal expansion and resistance to stress in mice with long-term liver damage.

METHODS

We tracked cholangiocytes using osteopontin-iCreER and hepatocytes with AAV8-TBG-Cre. Mice received carbon tetrachloride (CCl) for >24 weeks to induce chronic liver injury. Livers were collected for the analysis of reporter proteins, cell proliferation and death, DNA damage, and nuclear ploidy; hepatocytes were also isolated for RNA sequencing.

RESULTS

During liver injury we observed a transient DR and the differentiation of DR cells into hepatocytes as clones that expanded to occupy 12% of the liver parenchyma by week 8. By lineage tracing, we confirmed that these new hepatocytes derived from cholangiocytes but not from native hepatocytes. They had all the features of mature functional hepatocytes. In contrast to the exhausted native hepatocytes, these newly formed hepatocytes had higher proliferative capability, less apoptosis, a lower proportion of highly polyploid nuclei and were better at eliminating DNA damage.

CONCLUSIONS

In chronic liver injury, DR cells differentiate into stress-resistant hepatocytes that repopulate the liver. The process might account for the observed parenchymal reconstitution in livers of patients with advanced-stage hepatitis and could be a target for regenerative purposes.

LAY SUMMARY

During chronic liver disease, while native hepatocytes are exhausted and genetically unstable, a subset of cholangiocytes clonally expand to differentiate into young, functional and robust hepatocytes. This cholangiocyte cell population is a promising target for regenerative therapies in patients with chronic liver insufficiency.

摘要

背景与目的

慢性肝病的特征是小不成熟的胆管细胞扩张——一种称为胆管反应(DR)的机制——其具有分化为肝细胞的能力。我们研究了这种分化的动力学,以及分析了新形成的肝细胞的几个重要特征,如功能成熟度、克隆扩张和对长期肝损伤小鼠应激的抗性。

方法

我们使用骨桥蛋白-iCreER 追踪胆管细胞,使用 AAV8-TBG-Cre 追踪肝细胞。小鼠接受四氯化碳(CCl)治疗>24 周以诱导慢性肝损伤。收集肝脏用于分析报告蛋白、细胞增殖和死亡、DNA 损伤和核倍性;还分离了肝细胞进行 RNA 测序。

结果

在肝损伤过程中,我们观察到短暂的 DR,以及 DR 细胞分化为克隆的肝细胞,这些克隆在第 8 周时扩展到占据肝脏实质的 12%。通过谱系追踪,我们证实这些新的肝细胞来自胆管细胞,而不是来自天然的肝细胞。它们具有成熟功能肝细胞的所有特征。与耗尽的天然肝细胞不同,这些新形成的肝细胞具有更高的增殖能力、更少的凋亡、更低比例的高度多倍体核,并且更能清除 DNA 损伤。

结论

在慢性肝损伤中,DR 细胞分化为具有应激抗性的肝细胞,这些肝细胞可以重新填充肝脏。该过程可能解释了在晚期肝炎患者肝脏中观察到的实质重建,并且可能是再生目的的一个目标。

概述

在慢性肝病中,当天然肝细胞衰竭且遗传不稳定时,一小部分胆管细胞克隆扩张分化为年轻、功能和强壮的肝细胞。这种胆管细胞群体是慢性肝功能不全患者再生治疗的有前途的靶点。

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