Olig2 and Ngn2 function in opposition to modulate gene expression in motor neuron progenitor cells

AUTOR(ES)

Lee, Soo-Kyung

FONTE

Cold Spring Harbor Laboratory Press

RESUMO

Spinal motor neurons and oligodendrocytes are generated sequentially from a common pool of progenitors termed pMN cells. Olig2 is a bHLH-class transcription factor in pMN cells, but it has remained unclear how its transcriptional activity is modulated to first produce motor neurons and then oligodendrocytes. Previous studies have shown that Olig2 primes pMN cells to become motor neurons by triggering the expression of Ngn2 and Lhx3. Here we show that Olig2 also antagonizes the premature expression of post-mitotic motor neuron genes in pMN cells. This blockade is counteracted by Ngn2, which accumulates heterogeneously in pMN cells, thereby releasing a subset of the progenitors to differentiate and activate expression of post-mitotic motor neuron genes. The antagonistic relationship between Ngn2 and Olig2 is mediated by protein interactions that squelch activity as well as competition for shared DNA-binding sites. Our data support a model in which the Olig2/Ngn2 ratio in progenitor cells serves as a gate for timing proper gene expression during the development of pMN cells: Olig2high maintains the pMN state, thereby holding cells in reserve for oligodendrocyte generation, whereas Ngn2high favors the conversion of pMN cells into post-mitotic motor neurons.

Documentos Relacionados

• Divergent functions of the proneural genes Mash1 and Ngn2 in the specification of neuronal subtype identity
• Htra2-β1 stimulates an exonic splicing enhancer and can restore full-length SMN expression to survival motor neuron 2 (SMN2)
• The Caenorhabditis elegans gene ham-2 links Hox patterning to migration of the HSN motor neuron
• The pattern of gene expression in human CD15+ myeloid progenitor cells
• The pattern of gene expression in human CD34+ stem/progenitor cells