Persistent expression of Pax3 in the neural crest causes cleft palate and defective osteogenesis in mice
Meilin Wu, … , Joshua B. Plotkin, Jonathan A. Epstein
Meilin Wu, … , Joshua B. Plotkin, Jonathan A. Epstein
Published May 15, 2008
Citation Information: J Clin Invest. 2008;118(6):2076-2087. https://doi.org/10.1172/JCI33715.
View: Text | PDF
Research Article Development

Persistent expression of Pax3 in the neural crest causes cleft palate and defective osteogenesis in mice

Abstract

Transcription factors regulate tissue patterning and cell fate determination during development; however, expression of early regulators frequently abates upon differentiation, suggesting that they may also play a role in maintaining an undifferentiated phenotype. The transcription factor paired box 3 (Pax3) is expressed by multipotent neural crest precursors and is implicated in neural crest disorders in humans such as Waardenburg syndrome. Pax3 is required for development of multiple neural crest lineages and for activation of lineage-specific programs, yet expression is generally extinguished once neural crest cells migrate from the dorsal neural tube and differentiate. Using a murine Cre-inducible system, we asked whether persistent Pax3 expression in neural crest derivatives would affect development or patterning. We found that persistent expression of Pax3 in cranial neural crest cells resulted in cleft palate, ocular defects, malformation of the sphenoid bone, and perinatal lethality. Furthermore, we demonstrated that Pax3 directly regulates expression of Sostdc1, a soluble inhibitor of bone morphogenetic protein (BMP) signaling. Persistent Pax3 expression renders the cranial crest resistant to BMP-induced osteogenesis. Thus, one mechanism by which Pax3 maintains the undifferentiated state of neural crest mesenchyme may be to block responsiveness to differentiation signals from the environment. These studies provide in vivo evidence for the importance of Pax3 downregulation during differentiation of multipotent neural crest precursors and cranial development.

Authors

Meilin Wu, Jun Li, Kurt A. Engleka, Bo Zhou, Min Min Lu, Joshua B. Plotkin, Jonathan A. Epstein

×

Figure 4

Endogenous and persistent Pax3 is expressed in the palate.

Options: View larger image (or click on image) Download as PowerPoint
Endogenous and persistent Pax3 is expressed in the palate. Frontal secti...
Frontal sections through the palatal region of E12.5 (A and D), E13.5 (B and E), and P0 (C and F) embryos are shown. Endogenous Pax3 is expressed in Pax3+/+, R26Pax3/Pax3 embryos in the palatal shelves at E12.5 (A) and E13.5 (B) along the inner surface (arrows) as well as in the tongue (*) and mandible. At birth, Pax3 expression in the palate has abated in control embryos (F). Pax3Cre/+, R26Pax3/Pax3 mice have much higher levels of Pax3 in the palate (arrows) and tongue (*) compared with control at both E12.5 (D) and E13.5 (E), with expression expanded to the entire palate mesenchyme, tongue, and developing mandible but not the epithelium. (F) At P0, Pax3 expression persists in the unfused palatal shelves (arrows) as well as in the tongue. Original magnification, ×6.3.