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Publication : Loss of BETA2/NeuroD leads to malformation of the dentate gyrus and epilepsy.

First Author  Liu M Year  2000
Journal  Proc Natl Acad Sci U S A Volume  97
Issue  2 Pages  865-70
PubMed ID  10639171 Mgi Jnum  J:59932
Mgi Id  MGI:1352314 Doi  10.1073/pnas.97.2.865
Citation  Liu M, et al. (2000) Loss of BETA2/NeuroD leads to malformation of the dentate gyrus and epilepsy [published erratum appears in Proc Natl Acad Sci U S A 2000 May 9;97(10):5679]. Proc Natl Acad Sci U S A 97(2):865-70
abstractText  BETA2/NeuroD is a homologue of the Drosophila atonal gene that is widely expressed during development in the mammalian brain and pancreas. Although studies in Xenopus suggest that BETA2/NeuroD is involved in cellular differentiation, its function in the mammalian nervous system is unclear. Here we show that mutant mice homozygous for a deletion at the BETA2/NeuroD locus fail to develop a granule cell layer within the dentate gyrus, one of the principal structures of the hippocampal formation. To understand the basis of this abnormality, we analyzed dentate gyrus development by using immunocytochemical markers in BETA2/NeuroD-deficient mice. The early cell populations in the dentate gyrus, including Cajal-Retzius cells and radial glia, are present and appear normally organized. The migration of dentate precursor cells and newly born granule cells from the neuroepithelium to the dentate gyrus remains intact. However, there is a dramatic defect in the proliferation of precursor cells once they reach the dentate and a significant delay in the differentiation of granule cells. This leads to malformation of the dentate granule cell layer and excess cell death. BETA2/NeuroD null mice also exhibit spontaneous limbic seizures associated with electrophysiological evidence of seizure activity in the hippocampus and cortex. These findings thus establish a critical role of BETA2/NeuroD in the development of a specific class of neurons. Furthermore, failure to express BETA2/NeuroD leads to a stereotyped pattern of pathological excitability of the adult central nervous system.
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