Epigenetic remodelling licences adult cholangiocytes for organoid formation and 
liver regeneration.

Aloia, Luigi; McKie, Mikel Alexander; Vernaz, Grégoire; Cordero-Espinoza, Lucía; Aleksieva, Niya; Ameele, Jelle van den; Antonica, Francesco; Font-Cunill, Berta; Raven, Alexander; Cigliano, Riccardo Aiese; Belenguer, German; Mort, Richard Lester; Brand, Andrea H; Zernicka-Goetz, Magdalena; Forbes, Stuart J; Miska, Eric A; Huch, Meritxell

doi:10.1038/s41556-019-0402-6

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Epigenetic remodelling licences adult cholangiocytes for organoid formation and liver regeneration.

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Huch, Meritxell
Max Planck Institute for Molecular Cell Biology and Genetics, Max Planck Society;

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Citation

Aloia, L., McKie, M. A., Vernaz, G., Cordero-Espinoza, L., Aleksieva, N., Ameele, J. v. d., et al. (2019). Epigenetic remodelling licences adult cholangiocytes for organoid formation and liver regeneration. Nature cell biology, 21(11), 1321-1333. doi:10.1038/s41556-019-0402-6.

Cite as: https://hdl.handle.net/21.11116/0000-0006-7D9A-1

Abstract

Following severe or chronic liver injury, adult ductal cells (cholangiocytes) contribute to regeneration by restoring both hepatocytes and cholangiocytes. We recently showed that ductal cells clonally expand as self-renewing liver organoids that retain their differentiation capacity into both hepatocytes and ductal cells. However, the molecular mechanisms by which adult ductal-committed cells acquire cellular plasticity, initiate organoids and regenerate the damaged tissue remain largely unknown. Here, we describe that ductal cells undergo a transient, genome-wide, remodelling of their transcriptome and epigenome during organoid initiation and in vivo following tissue damage. TET1-mediated hydroxymethylation licences differentiated ductal cells to initiate organoids and activate the regenerative programme through the transcriptional regulation of stem-cell genes and regenerative pathways including the YAP-Hippo signalling. Our results argue in favour of the remodelling of genomic methylome/hydroxymethylome landscapes as a general mechanism by which differentiated cells exit a committed state in response to tissue damage.