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Gardiner, J.R.* ; Jackson, A.L.* ; Gordon, J.* ; Lickert, H. ; Manley, N.R.* ; Basson, M.A.*

Localised inhibition of FGF signalling in the third pharyngeal pouch is required for normal thymus and parathyroid organogenesis.

Development 139, 3456-3466 (2012)
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The thymus and parathyroid glands are derived from the third pharyngeal pouch endoderm. The mechanisms that establish distinct molecular domains in the third pouch and control the subsequent separation of these organ primordia from the pharynx are poorly understood. Here, we report that mouse embryos that lack two FGF feedback antagonists, Spry1 and Spry2, display parathyroid and thymus hypoplasia and a failure of these organ primordia to completely separate from the pharynx. We show that FGF ligands and downstream reporter genes are expressed in highly regionalised patterns in the third pouch and that sprouty gene deletion results in upregulated FGF signalling throughout the pouch endoderm. As a consequence, the initiation of markers of parathyroid and thymus fate is altered. In addition, a normal apoptotic programme that is associated with the separation of the primordia from the pharynx is disrupted, resulting in the maintenance of a thymus-pharynx attachment and a subsequent inability of the thymus to migrate to its appropriate position above the heart. We demonstrate that the sprouty genes function in the pharyngeal endoderm itself to control these processes and that the defects in sprouty-deficient mutants are, at least in part, due to hyper-responsiveness to Fgf8. Finally, we provide evidence to suggest that parathyroid hypoplasia in these mutants is due to early gene expression defects in the third pouch, whereas thymus hypoplasia is caused by reduced proliferation of thymic epithelial cells in the thymus primordium.
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Publication type Article: Journal article
Document type Scientific Article
Keywords Fgf ; Sprouty ; Thymus ; Parathyroid ; Pharyngeal Pouch ; Endoderm ; Mouse; Sprouty Genes; Cell-Survival; Sonic-Hedgehog; Nude-Mice; Mouse; Expression; Morphogenesis; Endoderm; Cerebellum; BMP4
Language english
Publication Year 2012
HGF-reported in Year 2012
ISSN (print) / ISBN 0950-1991
e-ISSN 1477-9129
Quellenangaben Volume: 139, Issue: 18, Pages: 3456-3466 Article Number: , Supplement: ,
Publisher Company of Biologists
Reviewing status Peer reviewed
POF-Topic(s) 90000 - German Center for Diabetes Research
30201 - Metabolic Health
30504 - Mechanisms of Genetic and Environmental Influences on Health and Disease
Research field(s) Helmholtz Diabetes Center
Stem Cell and Neuroscience
PSP Element(s) G-501900-231
G-502300-001
G-500890-001
PubMed ID 22912418
Scopus ID 84865216720
Erfassungsdatum 2012-09-27