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Semaphorin signaling plays integral roles in multiple developmental processes. Branching morphogenesis is one such role that has not been thoroughly explored. Here, we show in mice that functional blockage of neuropilin 1 (Npn1) inhibits cleft formation in the developing submandibular gland (SMG) cultured ex vivo. This Npn1-dependent morphogenesis is mediated by Sema3A and Sema3C in an additive manner, and can be abolished by decreasing the expression of plexin A2 or plexin D1. VEGF, another known Npn1 ligand, has no apparent effects on SMG development. FGF signaling, which also mediates SMG branching morphogenesis, acts in parallel with semaphorin signaling. Finally, in contrast to the effect of FGF signaling, we find that semaphorins do not stimulate the proliferation of SMG epithelial cells. Instead, the semaphorin signals act locally on the epithelial cells to facilitate SMG cleft formation.
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Development ePress online publication date 11 Jul 2007
doi: 10.1242/dev.005066
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Semaphorin signaling facilitates cleft formation in the developing salivary gland
* Author for correspondence (e-mail: phhuang{at}ntu.edu.tw)
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P. Lu and Z. Werb
Patterning Mechanisms of Branched Organs
Science,
December 5, 2008;
322(5907):
1506 - 1509.
[Abstract]
[Full Text]
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A. Korostylev, T. Worzfeld, S. Deng, R. H. Friedel, J. M. Swiercz, P. Vodrazka, V. Maier, A. Hirschberg, Y. Ohoka, S. Inagaki, et al.
A functional role for semaphorin 4D/plexin B1 interactions in epithelial branching morphogenesis during organogenesis
Development,
October 15, 2008;
135(20):
3333 - 3343.
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© The Company of Biologists Ltd 2007