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Quantitative lineage analysis identifies a hepato-pancreato-biliary progenitor niche

Author

Listed:
  • David Willnow

    (King’s College London
    Berlin Institute of Health)

  • Uwe Benary

    (Max-Delbrueck-Center for Molecular Medicine)

  • Anca Margineanu

    (Max-Delbrueck-Center for Molecular Medicine)

  • Maria Lillina Vignola

    (King’s College London)

  • Fabian Konrath

    (Max-Delbrueck-Center for Molecular Medicine)

  • Igor M. Pongrac

    (Max-Delbrueck-Center for Molecular Medicine)

  • Zahra Karimaddini

    (ETH Zurich
    Swiss Institute of Bioinformatics)

  • Alessandra Vigilante

    (King’s College London)

  • Jana Wolf

    (Max-Delbrueck-Center for Molecular Medicine
    Free University)

  • Francesca M. Spagnoli

    (King’s College London)

Abstract

Studies based on single cells have revealed vast cellular heterogeneity in stem cell and progenitor compartments, suggesting continuous differentiation trajectories with intermixing of cells at various states of lineage commitment and notable degrees of plasticity during organogenesis1–5. The hepato-pancreato-biliary organ system relies on a small endoderm progenitor compartment that gives rise to a variety of different adult tissues, including the liver, pancreas, gall bladder and extra-hepatic bile ducts6,7. Experimental manipulation of various developmental signals in the mouse embryo has underscored important cellular plasticity in this embryonic territory6. This is reflected in the existence of human genetic syndromes as well as congenital malformations featuring multi-organ phenotypes in liver, pancreas and gall bladder6. Nevertheless, the precise lineage hierarchy and succession of events leading to the segregation of an endoderm progenitor compartment into hepatic, biliary and pancreatic structures have not yet been established. Here we combine computational modelling approaches with genetic lineage tracing to accurately reconstruct the hepato-pancreato-biliary lineage tree. We show that a multipotent progenitor subpopulation persists in the pancreato-biliary organ rudiment, contributing cells not only to the pancreas and gall bladder but also to the liver. Moreover, using single-cell RNA sequencing and functional experiments we define a specialized niche that supports this subpopulation in a multipotent state for an extended time during development. Together these findings indicate sustained plasticity underlying hepato-pancreato-biliary development that might also explain the rapid expansion of the liver while attenuating pancreato-biliary growth.

Suggested Citation

  • David Willnow & Uwe Benary & Anca Margineanu & Maria Lillina Vignola & Fabian Konrath & Igor M. Pongrac & Zahra Karimaddini & Alessandra Vigilante & Jana Wolf & Francesca M. Spagnoli, 2021. "Quantitative lineage analysis identifies a hepato-pancreato-biliary progenitor niche," Nature, Nature, vol. 597(7874), pages 87-91, September.
  • Handle: RePEc:nat:nature:v:597:y:2021:i:7874:d:10.1038_s41586-021-03844-1
    DOI: 10.1038/s41586-021-03844-1
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    Cited by:

    1. Xiaochan Xu & Philip Allan Seymour & Kim Sneppen & Ala Trusina & Anuska la Rosa Egeskov-Madsen & Mette Christine Jørgensen & Mogens Høgh Jensen & Palle Serup, 2023. "Jag1-Notch cis-interaction determines cell fate segregation in pancreatic development," Nature Communications, Nature, vol. 14(1), pages 1-17, December.
    2. Zhuo Ma & Xiaofei Zhang & Wen Zhong & Hongyan Yi & Xiaowei Chen & Yinsuo Zhao & Yanlin Ma & Eli Song & Tao Xu, 2023. "Deciphering early human pancreas development at the single-cell level," Nature Communications, Nature, vol. 14(1), pages 1-17, December.

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