Endothelin 3 promotes neural crest cell proliferation and mediates a vast increase in melanocyte number in culture.
AUTOR(ES)
Lahav, R
RESUMO
Mutations in the endothelin 3 (EDN3) gene severely affect the development of neural crest-derived melanocytes. In this paper, we report the action of EDN3 on neural crest cells in vitro. The presence of EDN3 leads to a large increase in the number of cells, the majority of which eventually differentiate into melanocytes that aggregate to form a reproducible pigmentation pattern. Quantitative analysis of the effect of different culture conditions revealed that EDN3 initially promotes neural crest cell proliferation. This phase of expansion, which can be prolonged for a few weeks if the cells are replaced regularly, is followed by both a decrease in cell proliferation and the onset of melanocytic differentiation. Therefore, EDN3 is a potent mitogen for early neural crest cell precursors that can give rise to melanocytes.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=39455Documentos Relacionados
- Endothelin 3 selectively promotes survival and proliferation of neural crest-derived glial and melanocytic precursors in vitro
- The neural crest stem cells: control of neural crest cell fate and plasticity by endothelin-3
- Informatic selection of a neural crest-melanocyte cDNA set for microarray analysis
- Endothelin 3 induces the reversion of melanocytes to glia through a neural crest-derived glial-melanocytic progenitor
- Xenopus Zic3, a primary regulator both in neural and neural crest development
