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Publication : Signaling mechanisms controlling cranial placode neurogenesis and delamination.

First Author  Lassiter RN Year  2014
Journal  Dev Biol Volume  389
Issue  1 Pages  39-49
PubMed ID  24315854 Mgi Jnum  J:208825
Mgi Id  MGI:5565072 Doi  10.1016/j.ydbio.2013.11.025
Citation  Lassiter RN, et al. (2014) Signaling mechanisms controlling cranial placode neurogenesis and delamination. Dev Biol 389(1):39-49
abstractText  The neurogenic cranial placodes are a unique transient epithelial niche of neural progenitor cells that give rise to multiple derivatives of the peripheral nervous system, particularly, the sensory neurons. Placode neurogenesis occurs throughout an extended period of time with epithelial cells continually recruited as neural progenitor cells. Sensory neuron development in the trigeminal, epibranchial, otic, and olfactory placodes coincides with detachment of these neuroblasts from the encompassing epithelial sheet, leading to delamination and ingression into the mesenchyme where they continue to differentiate as neurons. Multiple signaling pathways are known to direct placodal development. This review defines the signaling pathways working at the finite spatiotemporal period when neuronal selection within the placodes occurs, and neuroblasts concomitantly delaminate from the epithelium. Examining neurogenesis and delamination after initial placodal patterning and specification has revealed a common trend throughout the neurogenic placodes, which suggests that both activated FGF and attenuated Notch signaling activities are required for neurogenesis and changes in epithelial cell adhesion leading to delamination. We also address the varying roles of other pathways such as the Wnt and BMP signaling families during sensory neurogenesis and neuroblast delamination in the differing placodes.
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