Click here to close
Hello! We notice that you are using Internet Explorer, which is not supported by Xenbase and may cause the site to display incorrectly.
We suggest using a current version of Chrome,
FireFox, or Safari.
???displayArticle.abstract???
Mammalian organs, including the lung and kidney, often adopt a branched structure to achieve high efficiency and capacity of their physiological functions. Formation of a functional lung requires two developmental processes: branching morphogenesis, which builds a tree-like tubular network, and alveolar differentiation, which generates specialized epithelial cells for gas exchange. Much progress has been made to understand each of the two processes individually; however, it is not clear whether the two processes are coordinated and how they are deployed at the correct time and location. Here we show that an epithelial branching morphogenesis program antagonizes alveolar differentiation in the mouse lung. We find a negative correlation between branching morphogenesis and alveolar differentiation temporally, spatially, and evolutionarily. Gain-of-function experiments show that hyperactive small GTPase Kras expands the branching program and also suppresses molecular and cellular differentiation of alveolar cells. Loss-of-function experiments show that SRY-box containing gene 9 (Sox9) functions downstream of Fibroblast growth factor (Fgf)/Kras to promote branching and also suppresses premature initiation of alveolar differentiation. We thus propose that lung epithelial progenitors continuously balance between branching morphogenesis and alveolar differentiation, and such a balance is mediated by dual-function regulators, including Kras and Sox9. The resulting temporal delay of differentiation by the branching program may provide new insights to lung immaturity in preterm neonates and the increase in organ complexity during evolution.
Fig. 1. Temporal (A), spatial (B), and evolutionary (C) negative correlations between branching morphogenesis and alveolar differentiation. (A) Time-course
microarray expression profiling of FACS-purified distallung epithelial cells. Gene expression values (log2) in E14 samples are used as a baseline for comparison.
Horizontal histograms for E15�E19 samples are the frequency distributions of average fold-changes for all genes; the units are shown as the number of genes
(# genes). Alveolar markers are up-regulated (red), and branching (green) and cell cycle (blue) related genes are down-regulated over time. Down-regulated
genes appear to have a smaller fold-change than up-regulated genes, possibly because of perdurance of transcripts. (B) Confocal images of immunostained
E18 lung sections in areas where the airway lumen can be continuously traced from the proximal conducting airways (black/white long dashed lines) to the
distal nonbranch tip (magenta) and branch tip (green) regions, as illustrated in the schematics. Branch tips are outlined with dashed lines. The boxed regions
are enlarged as insets outlined in corresponding colors, showing a spatial negative correlation between branching and alveolar differentiation. AQP1 labels
alveolar type I cells, the vasculature and the mesothelium, which are separated by dashed lines (Insets). There is a very low level of SOX9 expression in
nonbranch tip epithelium, possibly because of protein perdurance. (Scale bars, 20 μm.) (C) Whole-mount in situ hybridization and immunostaining of Xenopus
embryos of indicated stages (St) showing the absence of Sox9 expression and branching in the Xenopus lung. The lungs are indicated with dashed lines if
stained or arrowheads if unstained. Open arrowheads indicate Sox9 expression in the pharyngeal arches. The two Xenopus Sox9 homologs (Sox9a and Sox9b)
are 95% identical on the nucleotide level. OPT images of immunostained embryos (Left, Bottom) are shown as maximal intensity projection (Left) and
sectional view (Right). (Scale bar, 200 μm.)
Fig. S4. Xenopus lungs lack the branching program and Sox9 expression, and initiates alveolar differentiation immediately after lung specification. Whole
mount in situ hybridization of Xenopus embryos at indicated stages (St). The lungs are indicated with dashed lines if stained or arrowheads if unstained. Open
arrowheads indicate Sox9 expression in the pharyngeal arches. The onset of Sftpb expression is slightly later than that of Sftpc expression (Fig. 1C). (Scale bar,
200 μm.)
Agrons,
From the archives of the AFIP: Lung disease in premature neonates: radiologic-pathologic correlation.
2005, Pubmed
Agrons,
From the archives of the AFIP: Lung disease in premature neonates: radiologic-pathologic correlation.
2005,
Pubmed Arnold,
Sox2(+) adult stem and progenitor cells are important for tissue regeneration and survival of mice.
2011,
Pubmed Bi,
Haploinsufficiency of Sox9 results in defective cartilage primordia and premature skeletal mineralization.
2001,
Pubmed Bird,
cAMP response element binding protein is required for differentiation of respiratory epithelium during murine development.
2011,
Pubmed Bridgewater,
Canonical WNT/beta-catenin signaling is required for ureteric branching.
2008,
Pubmed Cardoso,
Regulation of early lung morphogenesis: questions, facts and controversies.
2006,
Pubmed Chen,
Estrogen-related receptor beta/NR3B2 controls epithelial cell fate and endolymph production by the stria vascularis.
2007,
Pubmed Chen,
Integrin Beta 1 suppresses multilayering of a simple epithelium.
2012,
Pubmed De Moerlooze,
An important role for the IIIb isoform of fibroblast growth factor receptor 2 (FGFR2) in mesenchymal-epithelial signalling during mouse organogenesis.
2000,
Pubmed El-Hashash,
Eyes absent 1 (Eya1) is a critical coordinator of epithelial, mesenchymal and vascular morphogenesis in the mammalian lung.
2011,
Pubmed French,
Murine clusterin: molecular cloning and mRNA localization of a gene associated with epithelial differentiation processes during embryogenesis.
1993,
Pubmed Habermehl,
Glucocorticoid activity during lung maturation is essential in mesenchymal and less in alveolar epithelial cells.
2011,
Pubmed Harfe,
Evidence for an expansion-based temporal Shh gradient in specifying vertebrate digit identities.
2004,
Pubmed Harris,
Dicer function is essential for lung epithelium morphogenesis.
2006,
Pubmed Hyatt,
Lung specific developmental expression of the Xenopus laevis surfactant protein C and B genes.
2007,
Pubmed
,
Xenbase Jackson,
Analysis of lung tumor initiation and progression using conditional expression of oncogenic K-ras.
2001,
Pubmed Johnson,
K-ras is an essential gene in the mouse with partial functional overlap with N-ras.
1997,
Pubmed Kranenburg,
The KRAS oncogene: past, present, and future.
2005,
Pubmed Lin,
Misexpression of MIA disrupts lung morphogenesis and causes neonatal death.
2008,
Pubmed Liu,
Differential gene expression in the distal tip endoderm of the embryonic mouse lung.
2002,
Pubmed Lyons,
Requirement of Wnt/beta-catenin signaling in pronephric kidney development.
2009,
Pubmed
,
Xenbase Madisen,
A robust and high-throughput Cre reporting and characterization system for the whole mouse brain.
2010,
Pubmed Manwani,
Reduced viability of mice with lung epithelial-specific knockout of glucocorticoid receptor.
2010,
Pubmed Marose,
Beta-catenin is necessary to keep cells of ureteric bud/Wolffian duct epithelium in a precursor state.
2008,
Pubmed
,
Xenbase Martis,
C/EBPalpha is required for lung maturation at birth.
2006,
Pubmed Metzger,
The branching programme of mouse lung development.
2008,
Pubmed Morrisey,
Preparing for the first breath: genetic and cellular mechanisms in lung development.
2010,
Pubmed Morrisey,
Balancing the developmental niches within the lung.
2013,
Pubmed Muzumdar,
A global double-fluorescent Cre reporter mouse.
2007,
Pubmed Nechiporuk,
Dlg5 maintains apical aPKC and regulates progenitor differentiation during lung morphogenesis.
2013,
Pubmed O'Brien,
CARM1 is required for proper control of proliferation and differentiation of pulmonary epithelial cells.
2010,
Pubmed Panico,
Clusterin (CLU) and lung cancer.
2009,
Pubmed Perl,
Normal lung development and function after Sox9 inactivation in the respiratory epithelium.
2005,
Pubmed Que,
Multiple roles for Sox2 in the developing and adult mouse trachea.
2009,
Pubmed Rajagopal,
Wnt7b stimulates embryonic lung growth by coordinately increasing the replication of epithelium and mesenchyme.
2008,
Pubmed Reginensi,
SOX9 controls epithelial branching by activating RET effector genes during kidney development.
2011,
Pubmed Salaun,
CD208/dendritic cell-lysosomal associated membrane protein is a marker of normal and transformed type II pneumocytes.
2004,
Pubmed Sekine,
Fgf10 is essential for limb and lung formation.
1999,
Pubmed Seymour,
A Sox9/Fgf feed-forward loop maintains pancreatic organ identity.
2012,
Pubmed Shannon,
Induction of alveolar type II cell differentiation in fetal tracheal epithelium by grafted distal lung mesenchyme.
1994,
Pubmed Sharpe,
Optical projection tomography as a tool for 3D microscopy and gene expression studies.
2002,
Pubmed Sherr,
CDK inhibitors: positive and negative regulators of G1-phase progression.
1999,
Pubmed Shu,
Wnt/beta-catenin signaling acts upstream of N-myc, BMP4, and FGF signaling to regulate proximal-distal patterning in the lung.
2005,
Pubmed Small,
Developmental expression of the Xenopus Nkx2-1 and Nkx2-4 genes.
2000,
Pubmed
,
Xenbase Soeda,
Sox9-expressing precursors are the cellular origin of the cruciate ligament of the knee joint and the limb tendons.
2010,
Pubmed Tang,
Control of mitotic spindle angle by the RAS-regulated ERK1/2 pathway determines lung tube shape.
2011,
Pubmed Taniguchi,
A resource of Cre driver lines for genetic targeting of GABAergic neurons in cerebral cortex.
2011,
Pubmed Tompkins,
Sox2 is required for maintenance and differentiation of bronchiolar Clara, ciliated, and goblet cells.
2009,
Pubmed Ueno,
Processing of pulmonary surfactant protein B by napsin and cathepsin H.
2004,
Pubmed Warburton,
Lung organogenesis.
2010,
Pubmed Ward,
Alveolar type I and type II cells.
1984,
Pubmed Whitsett,
Alveolar surfactant homeostasis and the pathogenesis of pulmonary disease.
2010,
Pubmed Yu,
Conditional inactivation of FGF receptor 2 reveals an essential role for FGF signaling in the regulation of osteoblast function and bone growth.
2003,
Pubmed
