The gene encoding the T-box factor Tbx2 is a target for the microphthalmia-associated transcription factor in melanocytes

Citation
S. Carreira et al., The gene encoding the T-box factor Tbx2 is a target for the microphthalmia-associated transcription factor in melanocytes, J BIOL CHEM, 275(29), 2000, pp. 21920-21927
Citations number
49
Language
INGLESE
art.tipo
Article
Categorie Soggetti
Biochemistry & Biophysics
Journal title
JOURNAL OF BIOLOGICAL CHEMISTRY
ISSN journal
0021-9258 → ACNP
Volume
275
Issue
29
Year of publication
2000
Pages
21920 - 21927
Database
ISI
SICI code
0021-9258(20000721)275:29<21920:TGETTF>2.0.ZU;2-X
Abstract
Commitment to the melanocyte lineage is characterized by the onset of micro phthalmia-associated transcription factor (Mitf) expression. Mitf plays a f undamental role in melanocyte development, with mice lacking Mitf being ent irely devoid of pigment cells. In the absence of functional Mitf protein, m elanoblasts expressing Mitf mRNA disappear around 2 days after their first appearance either by apoptosis or by losing their identity and adopting an alternative cell fate. The role of Mitf must therefore be to regulate genes required for melanoblast survival, proliferation, or the maintenance of me lanoblast identity. Yet to date, Mitf has been shown to regulate genes such as Tyrosinase, Tyrp-1, and Dct, which are required for pigmentation, a dif ferentiation-specific process. Because expression of these genes cannot acc ount for the complete absence of pigment cells in Mitf-negative mice, Mitf must regulate the expression of other as yet uncharacterized genes. Here we provide several lines of evidence to suggest that Mitf may regulate the ex pression of the Tbx2 transcription factor, a member of the T-box family of proteins implicated in the maintenance of cell identity. First, isolation a nd sequencing of the entire murine Tbx2 gene revealed that the Tbx2 promote r contains a full consensus Mitf recognition element; second, Mitf could bi nd the promoter in vitro and activate Tbx2 expression in vivo in an E box-d ependent fashion; and third, Tbx2 is expressed in melanoma cell lines expre ssing Mitf, but not in a line in which Mitf expression was not detectable. Taken together, with the fact that Tbx2 is expressed in Mitf-positive melan oblasts and melanocytes, but not in Mitf-negative melanoblast precursor cel ls, the evidence suggests that the Tbx2 gene may represent one of the first known targets for Mitf that is not a gene involved directly in the manufac ture of pigment.