| Literature DB >> 31328313 |
Maria-Eleni Lalioti1, Konstantina Kaplani1, Georgia Lokka1, Theodore Georgomanolis2, Christina Kyrousi1, Weilai Dong3,4,5, Ashley Dunbar3,4,5, Evangelia Parlapani1, Eleni Damianidou1, Nathalie Spassky6, Kristopher T Kahle3,4,5, Argyris Papantonis2,7, Zoi Lygerou8, Stavros Taraviras1.
Abstract
The subventricular zone (SVZ) is one of two main niches where neurogenesis persists during adulthood, as it retains neural stem cells (NSCs) with self-renewal capacity and multi-lineage potency. Another critical cellular component of the niche is the population of postmitotic multiciliated ependymal cells. Both cell types are derived from radial glial cells that become specified to each lineage during embryogenesis. We show here that GemC1, encoding Geminin coiled-coil domain-containing protein 1, is associated with congenital hydrocephalus in humans and mice. Our results show that GemC1 deficiency drives cells toward a NSC phenotype, at the expense of multiciliated ependymal cell generation. The increased number of NSCs is accompanied by increased levels of proliferation and neurogenesis in the postnatal SVZ. Finally, GemC1-knockout cells display altered chromatin organization at multiple loci, further supporting a NSC identity. Together, these findings suggest that GemC1 regulates the balance between NSC generation and ependymal cell differentiation, with implications for the pathogenesis of human congenital hydrocephalus.Entities:
Keywords: GemC1; adult neurogenesis; congenital hydrocephalus; ependymal cells; neural stem cells; neurosurgery; subventricular zone
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Year: 2019 PMID: 31328313 DOI: 10.1002/glia.23690
Source DB: PubMed Journal: Glia ISSN: 0894-1491 Impact factor: 7.452