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Generation of human islet cell type-specific identity genesets

Author

Listed:
  • Léon Gurp

    (University of Geneva)

  • Leon Fodoulian

    (University of Geneva)

  • Daniel Oropeza

    (University of Geneva)

  • Kenichiro Furuyama

    (University of Geneva
    Kyoto University)

  • Eva Bru-Tari

    (University of Geneva)

  • Anh Nguyet Vu

    (Beckman Research Institute)

  • John S. Kaddis

    (Beckman Research Institute)

  • Iván Rodríguez

    (University of Geneva)

  • Fabrizio Thorel

    (University of Geneva)

  • Pedro L. Herrera

    (University of Geneva)

Abstract

Generation of surrogate cells with stable functional identities is crucial for developing cell-based therapies. Efforts to produce insulin-secreting replacement cells to treat diabetes require reliable tools to assess islet cellular identity. Here, we conduct a thorough single-cell transcriptomics meta-analysis to identify robustly expressed markers used to build genesets describing the identity of human α-, β-, γ- and δ-cells. These genesets define islet cellular identities better than previously published genesets. We show their efficacy to outline cell identity changes and unravel some of their underlying genetic mechanisms, whether during embryonic pancreas development or in experimental setups aiming at developing glucose-responsive insulin-secreting cells, such as pluripotent stem-cell differentiation or in adult islet cell reprogramming protocols. These islet cell type-specific genesets represent valuable tools that accurately benchmark gain and loss in islet cell identity traits.

Suggested Citation

  • Léon Gurp & Leon Fodoulian & Daniel Oropeza & Kenichiro Furuyama & Eva Bru-Tari & Anh Nguyet Vu & John S. Kaddis & Iván Rodríguez & Fabrizio Thorel & Pedro L. Herrera, 2022. "Generation of human islet cell type-specific identity genesets," Nature Communications, Nature, vol. 13(1), pages 1-14, December.
  • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-29588-8
    DOI: 10.1038/s41467-022-29588-8
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