| Literature DB >> 33328171 |
Talia Nasr1,2, Andrea M Holderbaum1,2, Praneet Chaturvedi1, Kunal Agarwal1, Jessica L Kinney1, Keziah Daniels1, Stephen L Trisno1,2, Vladimir Ustiyan3,4, John M Shannon3, James M Wells1,2, Debora Sinner2,3, Vladimir V Kalinichenko2,3,4, Aaron M Zorn5,2.
Abstract
Congenital tracheomalacia, resulting from incomplete tracheal cartilage development, is a relatively common birth defect that severely impairs breathing in neonates. Mutations in the Hedgehog (HH) pathway and downstream Gli transcription factors are associated with tracheomalacia in patients and mouse models; however, the underlying molecular mechanisms are unclear. Using multiple HH/Gli mouse mutants including one that mimics Pallister-Hall Syndrome, we show that excessive Gli repressor activity prevents specification of tracheal chondrocytes. Lineage tracing experiments show that Sox9+ chondrocytes arise from HH-responsive splanchnic mesoderm in the fetal foregut that expresses the transcription factor Foxf1. Disrupted HH/Gli signaling results in 1) loss of Foxf1 which in turn is required to support Sox9+ chondrocyte progenitors and 2) a dramatic reduction in Rspo2, a secreted ligand that potentiates Wnt signaling known to be required for chondrogenesis. These results reveal a HH-Foxf1-Rspo2 signaling axis that governs tracheal cartilage development and informs the etiology of tracheomalacia.Entities:
Keywords: Cartilage; Hedgehog; Trachea; Tracheomalacia
Year: 2020 PMID: 33328171 PMCID: PMC7875488 DOI: 10.1242/dmm.046573
Source DB: PubMed Journal: Dis Model Mech ISSN: 1754-8403 Impact factor: 5.758