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Embryonic mesothelial-derived hepatic lineage of quiescent and heterogenous scar-orchestrating cells defined but suppressed by WT1

Author

Listed:
  • Timothy James Kendall

    (The University of Edinburgh
    University of Edinburgh Centre for Inflammation Research, The University of Edinburgh)

  • Catherine Mary Duff

    (The University of Edinburgh
    University of Edinburgh Centre for Inflammation Research, The University of Edinburgh)

  • Luke Boulter

    (The University of Edinburgh)

  • David H. Wilson

    (The University of Edinburgh)

  • Elisabeth Freyer

    (The University of Edinburgh)

  • Stuart Aitken

    (The University of Edinburgh)

  • Stuart John Forbes

    (The University of Edinburgh)

  • John Peter Iredale

    (University of Edinburgh Centre for Inflammation Research, The University of Edinburgh
    Senate House, University of Bristol)

  • Nicholas Dixon Hastie

    (The University of Edinburgh)

Abstract

Activated hepatic stellate cells (aHSCs) orchestrate scarring during liver injury, with putative quiescent precursor mesodermal derivation. Here we use lineage-tracing from development, through adult homoeostasis, to fibrosis, to define morphologically and transcriptionally discreet subpopulations of aHSCs by expression of WT1, a transcription factor controlling morphological transitions in organogenesis and adult homoeostasis. Two distinct populations of aHSCs express WT1 after injury, and both re-engage a transcriptional signature reflecting embryonic mesothelial origin of their discreet quiescent adult precursor. WT1-deletion enhances fibrogenesis after injury, through upregulated Wnt-signalling and modulation of genes central to matrix persistence in aHSCs, and augmentation of myofibroblastic transition. The mesothelial-derived lineage demonstrates punctuated phenotypic plasticity through bidirectional mesothelial-mesenchymal transitions. Our findings demonstrate functional heterogeneity of adult scar-orchestrating cells that can be whole-life traced back through specific quiescent adult precursors to differential origin in development, and define WT1 as a paradoxical regulator of aHSCs induced by injury but suppressing scarring.

Suggested Citation

  • Timothy James Kendall & Catherine Mary Duff & Luke Boulter & David H. Wilson & Elisabeth Freyer & Stuart Aitken & Stuart John Forbes & John Peter Iredale & Nicholas Dixon Hastie, 2019. "Embryonic mesothelial-derived hepatic lineage of quiescent and heterogenous scar-orchestrating cells defined but suppressed by WT1," Nature Communications, Nature, vol. 10(1), pages 1-18, December.
  • Handle: RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-12701-9
    DOI: 10.1038/s41467-019-12701-9
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