The chromatin-remodeling protein ATRX is critical for neuronal survival during corticogenesis
The chromatin-remodeling protein ATRX is critical for neuronal survival during corticogenesis
Mutations in genes encoding chromatin-remodeling proteins, such as the ATRX gene, underlie a number of genetic disorders including several X-linked mental retardation syndromes; however, the role of these proteins in normal CNS development is unknown. Here, we used a conditional gene-targeting approach to inactivate Atrx, specifically in the forebrain of mice. Loss of ATRX protein caused widespread hypocellularity in the neocortex and hippocampus and a pronounced reduction in forebrain size. Neuronal "birthdating" confirmed that fewer neurons reached the superficial cortical layers, despite normal progenitor cell proliferation. The loss of cortical mass resulted from a 12-fold increase in neuronal apoptosis during early stages of corticogenesis in the mutant animals. Moreover, cortical progenitors isolated from Atrx-null mice undergo enhanced apoptosis upon differentiation. Taken together, our results indicate that ATRX is a critical mediator of cell survival during early neuronal differentiation. Thus, increased neuronal loss may contribute to the severe mental retardation observed in human patients.
- Northamptonshire Healthcare NHS Foundation Trust United Kingdom
- University of Ottawa Canada
- University of Oxford United Kingdom
- John Radcliffe Hospital United Kingdom
- University of Queensland Australia
Mice, Knockout, Neurons, X-linked Nuclear Protein, Organogenesis, Stem Cells, DNA Helicases, Nuclear Proteins, Apoptosis, Cell Differentiation, Neocortex, Hippocampus, Chromatin, Mice, ATRX, Animals, Newborn, X-Linked Intellectual Disability, Gene Targeting, Animals, 060410 Neurogenetics, Cell Proliferation
Mice, Knockout, Neurons, X-linked Nuclear Protein, Organogenesis, Stem Cells, DNA Helicases, Nuclear Proteins, Apoptosis, Cell Differentiation, Neocortex, Hippocampus, Chromatin, Mice, ATRX, Animals, Newborn, X-Linked Intellectual Disability, Gene Targeting, Animals, 060410 Neurogenetics, Cell Proliferation
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