4.8 Article

Progenitor potential of lung epithelial organoid cells in a transplantation model

期刊

CELL REPORTS
卷 39, 期 2, 页码 -

出版社

CELL PRESS
DOI: 10.1016/j.celrep.2022.110662

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资金

  1. Hope Funds for Cancer Research Postdoctoral Fellowship
  2. Damon Runyon Cancer Research Foundation [DRG:2368-19]
  3. Burroughs Wellcome Fund [1019903, F31 HL159919, R01 HL090136, R01 HL132266, R01 HL125821, U01 HL100402, RFA-HL-09-004, R35HL150876]
  4. Cystic Fibrosis Foundation Award [KIM19P0]
  5. LONGFONDS | Accelerate, project BREATH
  6. Cystic Fibrosis/Multiple Sclerosis Fund Foundation Inc.
  7. Harvard Stem Cell Institute

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This research demonstrates the progenitor cell functions of lung epithelial organoid cells after reintroduction to the lung, and reveals methods to investigate the potential of lung progenitor cells and model transitional cell states relevant to pathogenic features of lung disease in vivo.
Lung progenitor cells are crucial for regeneration following injury, yet it is unclear whether lung progenitor cells can be functionally engrafted after transplantation. We transplanted organoid cells derived from alveolar type II (AT2) cells enriched by SCA1-negative status (SNO) or multipotent SCA1-positive progenitor cells (SPO) into injured mouse lungs. Transplanted SNO cells are retained in the alveolar regions, whereas SPO cells incorporate into airway and alveolar regions. Single-cell transcriptomics demonstrate that transplanted SNO cells are comparable to native AT2 cells. Transplanted SPO cells exhibit transcriptional hallmarks of alveolar and airway cells, as well as transitional cell states identified in disease. Transplanted cells proliferate after re-injury of recipient mice and retain organoid-forming capacity. Thus, lung epithelial organoid cells exhibit progenitor cell functions after reintroduction to the lung. This study reveals methods to interrogate lung progenitor cell potential and model transitional cell states relevant to pathogenic features of lung disease in vivo.

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