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Publication : Pax3 functions at a nodal point in melanocyte stem cell differentiation.

First Author  Lang D Year  2005
Journal  Nature Volume  433
Issue  7028 Pages  884-7
PubMed ID  15729346 Mgi Jnum  J:96431
Mgi Id  MGI:3530428 Doi  10.1038/nature03292
Citation  Lang D, et al. (2005) Pax3 functions at a nodal point in melanocyte stem cell differentiation. Nature 433(7028):884-7
abstractText  Most stem cells are not totipotent. Instead, they are partially committed but remain undifferentiated. Upon appropriate stimulation they are capable of regenerating mature cell types. Little is known about the genetic programmes that maintain the undifferentiated phenotype of lineage-restricted stem cells. Here we describe the molecular details of a nodal point in adult melanocyte stem cell differentiation in which Pax3 simultaneously functions to initiate a melanogenic cascade while acting downstream to prevent terminal differentiation. Pax3 activates expression of Mitf, a transcription factor critical for melanogenesis, while at the same time it competes with Mitf for occupancy of an enhancer required for expression of dopachrome tautomerase, an enzyme that functions in melanin synthesis. Pax3-expressing melanoblasts are thus committed but undifferentiated until Pax3-mediated repression is relieved by activated beta-catenin. Thus, a stem cell transcription factor can both determine cell fate and simultaneously maintain an undifferentiated state, leaving a cell poised to differentiate in response to external stimuli.
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