Sox2-mediated differential activation of Six3.2 contributes to forebrain patterning

Author:

Beccari Leonardo123,Conte Ivan1,Cisneros Elsa123,Bovolenta Paola123

Affiliation:

1. Centro de Biología Molecular ‘Severo Ochoa’, CSIC-UAM, c/Nicolas Cabrera 1, Madrid 28049, Spain.

2. CIBER de Enfermedades Raras (CIBERER), c/Nicolas Cabrera 1, Madrid 28049, Spain.

3. Instituto Cajal, CSIC, Avda. Doctor Arce 37, 28002 Madrid, Spain.

Abstract

The vertebrate forebrain is patterned during gastrulation into telencephalic, retinal, hypothalamic and diencephalic primordia. Specification of each of these domains requires the concerted activity of combinations of transcription factors (TFs). Paradoxically, some of these factors are widely expressed in the forebrain, which raises the question of how they can mediate regional differences. To address this issue, we focused on the homeobox TF Six3.2. With genomic and functional approaches we demonstrate that, in medaka fish, Six3.2 regulates, in a concentration-dependent manner, telencephalic and retinal specification under the direct control of Sox2. Six3.2 and Sox2 have antagonistic functions in hypothalamic development. These activities are, in part, executed by Foxg1 and Rx3, which seem to be differentially and directly regulated by Six3.2 and Sox2. Together, these data delineate the mechanisms by which Six3.2 diversifies its activity in the forebrain and highlight a novel function for Sox2 as one of the main regulators of anterior forebrain development. They also demonstrate that graded levels of the same TF, probably operating in partially independent transcriptional networks, pattern the vertebrate forebrain along the anterior-posterior axis.

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

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