Single-cell omics analysis reveals functional diversification of hepatocytes during liver regeneration

染色质 转录组 肝再生 细胞生物学 生物 再生(生物学) 转录因子 功能(生物学) 细胞 肝细胞 计算生物学 遗传学 基因表达 基因 体外
作者
Tianyi Chen,Seh‐Hoon Oh,Simon G. Gregory,Xiling Shen,Anna Mae Diehl
出处
期刊:JCI insight [American Society for Clinical Investigation]
卷期号:5 (22) 被引量:73
标识
DOI:10.1172/jci.insight.141024
摘要

Adult liver has enormous regenerative capacity; it can regenerate after losing two-thirds of its mass while sustaining essential metabolic functions. How the liver balances dual demands for increased proliferative activity with maintenance of organ function is unknown but essential to prevent liver failure. Using partial hepatectomy (PHx) in mice to model liver regeneration, we integrated single-cell RNA- and ATAC-Seq to map state transitions in approximately 13,000 hepatocytes at single-cell resolution as livers regenerated, and validated key findings with IHC, to uncover how the organ regenerates hepatocytes while simultaneously fulfilling its vital tissue-specific functions. After PHx, hepatocytes rapidly and transiently diversified into multiple distinct populations with distinct functional bifurcation: some retained the chromatin landscapes and transcriptomes of hepatocytes in undamaged adult livers, whereas others transitioned to acquire chromatin landscapes and transcriptomes of fetal hepatocytes. Injury-related signaling pathways known to be critical for regeneration were activated in transitioning hepatocytes, and the most fetal-like hepatocytes exhibited chromatin landscapes that were enriched with transcription factors regulated by those pathways.
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