| First Author | Jalali A | Year | 2012 |
| Journal | Dev Growth Differ | Volume | 54 |
| Issue | 6 | Pages | 633-48 |
| PubMed ID | 22775504 | Mgi Jnum | J:317512 |
| Mgi Id | MGI:6854989 | Doi | 10.1111/j.1440-169X.2012.01364.x |
| Citation | Jalali A, et al. (2012) Induction of palate epithelial mesenchymal transition by transforming growth factor beta3 signaling. Dev Growth Differ 54(6):633-48 |
| abstractText | Transforming growth factor (TGFbeta)3 is essential for palate development, particularly during the late phase of palatogenesis when the disintegration of the palatal medial edge seam (MES) occurs resulting in mesenchymal confluence. The MES is composed of medial-edge epithelium (MEE) of opposite palatal shelves; its complete disintegration is essential for mediating correct craniofacial morphogenesis. This phenomenon is initiated by TGFbeta3 upon adherence of opposing palatal shelves, and subsequently epithelial-mesenchymal transition (EMT) instigates the loss of E-Cadherin, causing the MES to break into small epithelial islands forming confluent palatal mesenchyme; however, apoptosis and cell migration or in combination of all are other established mechanisms of seam disintegration. To investigate the molecular mechanisms that cause this E-Cadherin loss, we isolated and cultured murine embryonic primary MES cells from adhered palates and employed several biological approaches to explore the mechanism by which TGFbeta3 facilitates palatal seam disintegration. Here, we demonstrate that TGFbeta3 signals by activating both Smad-dependent and Smad-independent pathways. However, activation of the two most common EMT related transcription factors, Snail and SIP, was facilitated by Smad-independent pathways, contrary to the commonly accepted Smad-dependent pathway. Finally, we provide the first evidence that TGFbeta3-activated Snail and SIP1, combined with Smad4, bind to the E-Cadherin promoter to repress its transcription in response to TGFbeta3 signaling. These results suggest that TGFbeta3 uses multiple pathways to activate Snail and SIP1 and these transcription factors repress the cell-cell adhesion protein, E-Cadherin, to induce palatal epithelial seam EMT. Manipulation and intervention of the pathways stimulated by TGFbeta3 during palate development may have a significant therapeutic potential. |
