| Literature DB >> 30782824 |
David B Frank1,2,3, Ian J Penkala4, Jarod A Zepp2,5, Aravind Sivakumar6,2,3, Ricardo Linares-Saldana3,4,5, William J Zacharias7, Katharine G Stolz6, Josh Pankin6,2, MinQi Lu6, Qiaohong Wang3,4,5, Apoorva Babu3,5, Li Li3, Su Zhou3, Michael P Morley2,3,5, Rajan Jain8,4,5, Edward E Morrisey9,3,4,5.
Abstract
During the stepwise specification and differentiation of tissue-specific multipotent progenitors, lineage-specific transcriptional networks are activated or repressed to orchestrate cell specification. The gas-exchange niche in the lung contains two major epithelial cell types, alveolar type 1 (AT1) and AT2 cells, and the timing of lineage specification of these cells is critical for the correct formation of this niche and postnatal survival. Integrating cell-specific lineage tracing studies, spatially specific mRNA transcript and protein expression, and single-cell RNA-sequencing analysis, we demonstrate that specification of alveolar epithelial cell fate begins concomitantly with the proximal-distal specification of epithelial progenitors and branching morphogenesis earlier than previously appreciated. By using a newly developed dual-lineage tracing system, we show that bipotent alveolar cells that give rise to AT1 and AT2 cells are a minor contributor to the alveolar epithelial population. Furthermore, single-cell assessment of the transcriptome identifies specified AT1 and AT2 progenitors rather than bipotent cells during sacculation. These data reveal a paradigm of organ formation whereby lineage specification occurs during the nascent stages of development coincident with broad tissue-patterning processes, including axial patterning of the endoderm and branching morphogenesis.Entities:
Keywords: alveolar epithelium; lineage fate; lung development; single-cell RNA sequencing
Year: 2019 PMID: 30782824 PMCID: PMC6410851 DOI: 10.1073/pnas.1813952116
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205