| Literature DB >> 33974915 |
Ian J Penkala1, Derek C Liberti2, Joshua Pankin3, Aravind Sivakumar3, Madison M Kremp4, Sowmya Jayachandran3, Jeremy Katzen5, John P Leach4, Rebecca Windmueller2, Katharine Stolz3, Michael P Morley4, Apoorva Babu4, Su Zhou6, David B Frank7, Edward E Morrisey8.
Abstract
Regeneration of the architecturally complex alveolar niche of the lung requires precise temporal and spatial control of epithelial cell behavior. Injury can lead to a permanent reduction in gas exchange surface area and respiratory function. Using mouse models, we show that alveolar type 1 (AT1) cell plasticity is a major and unappreciated mechanism that drives regeneration, beginning in the early postnatal period during alveolar maturation. Upon acute neonatal lung injury, AT1 cells reprogram into alveolar type 2 (AT2) cells, promoting alveolar regeneration. In contrast, the ability of AT2 cells to regenerate AT1 cells is restricted to the mature lung. Unbiased genomic assessment reveals that this previously unappreciated level of plasticity is governed by the preferential activity of Hippo signaling in the AT1 cell lineage. Thus, cellular plasticity is a temporally acquired trait of the alveolar epithelium and presents an alternative mode of tissue regeneration in the postnatal lung.Entities:
Keywords: Hippo; alveolus; cellular plasticity; lung; regeneration
Mesh:
Year: 2021 PMID: 33974915 PMCID: PMC8500919 DOI: 10.1016/j.stem.2021.04.026
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 25.269