Abstract

One of the main goals of developmental biology is to elucidate the molecular mechanisms that govern the generation of distinct cell types from unspecified precursors. A detailed knowledge of these mechanisms will not only help us understand fundamental principles of normal ontogeny but also explain, and ultimately correct, instances where development has derailed and disease has resulted. The basic-helix-loop-helix-zipper transcription factor Mitf is encoded by a gene whose mutations in rodents or man may lead to abnormalities in the formation of neural crest-derived and neuroepithelial-derived melanocytes and to the concomitant skin pigmentation defects, deafness, and eye malformations that may lead to retinal degeneration. In mice, Mitf mutations appear to have different effects on neural crest-derived and neuroepithelium-derived melanocytes. Both in vivo and in culture, neural crest-derived mutant cells are blocked in their development at an early, pre-melanoblastic stage and may die. In contrast, mutant neuroepithelial-derived cells which normally become retinal pigment cells survive, display dysregulated expression of melanocyte-specific genes, and may finally develop into neuroretinal cells. Thus, Mitf appears to be a regulator of the developmental fate of at least two distinct cell lineages. To determine whether it has the capacity to respecify the fate of cells not normally destined to become melanocytes, we generated transgenic mice with ubiquitously inducible Mitf expression, are in the process of generating mice in which Mitf expression is specifically targeted to the developing retina, and are able to express Mitf ectopically in retinal and neural crest cell cultures. The analysis of target gene expression in such manipulated cells will help us understand the sequence of events that lead to melanocyte formation. To determine what is the precise fate of mutant neural crest-derived cells, we have initiated the generation of transgenic mice in which early melanoblasts and their derivatives are permanently marked.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Intramural Research (Z01)
Project #
1Z01NS002790-09
Application #
6163042
Study Section
Special Emphasis Panel (LDN)
Project Start
Project End
Budget Start
Budget End
Support Year
9
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
National Institute of Neurological Disorders and Stroke
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Bauer, Georg L; Praetorius, Christian; Bergsteinsdottir, Kristin et al. (2009) The role of MITF phosphorylation sites during coat color and eye development in mice analyzed by bacterial artificial chromosome transgene rescue. Genetics 183:581-94
Bharti, Kapil; Liu, Wenfang; Csermely, Tamas et al. (2008) Alternative promoter use in eye development: the complex role and regulation of the transcription factor MITF. Development 135:1169-78
Lee, Ji-Yeon; Muenzberg, Heike; Gavrilova, Oksana et al. (2008) Loss of cytokine-STAT5 signaling in the CNS and pituitary gland alters energy balance and leads to obesity. PLoS ONE 3:e1639
Bismuth, Keren; Skuntz, Susan; Hallsson, Jon H et al. (2008) An unstable targeted allele of the mouse Mitf gene with a high somatic and germline reversion rate. Genetics 178:259-72
Puligilla, Chandrakala; Feng, Feng; Ishikawa, Kotaro et al. (2007) Disruption of fibroblast growth factor receptor 3 signaling results in defects in cellular differentiation, neuronal patterning, and hearing impairment. Dev Dyn 236:1905-17
Arnheiter, Heinz (2007) Mammalian paramutation: a tail's tale? Pigment Cell Res 20:36-40
Bharti, Kapil; Nguyen, Minh-Thanh T; Skuntz, Susan et al. (2006) The other pigment cell: specification and development of the pigmented epithelium of the vertebrate eye. Pigment Cell Res 19:380-94
Chang, Lan; Blain, Delphine; Bertuzzi, Stefano et al. (2006) Uveal coloboma: clinical and basic science update. Curr Opin Ophthalmol 17:447-70
Murakami, Hideki; Arnheiter, Heinz (2005) Sumoylation modulates transcriptional activity of MITF in a promoter-specific manner. Pigment Cell Res 18:265-77
Horsford, D Jonathan; Nguyen, Minh-Thanh T; Sellar, Grant C et al. (2005) Chx10 repression of Mitf is required for the maintenance of mammalian neuroretinal identity. Development 132:177-87

Showing the most recent 10 out of 24 publications