| Literature DB >> 24859200 |
Michel Kielar1, Françoise Phan Dinh Tuy2, Sara Bizzotto2, Cécile Lebrand3, Camino de Juan Romero4, Karine Poirier5, Renske Oegema6, Grazia Maria Mancini6, Nadia Bahi-Buisson7, Robert Olaso8, Anne-Gaëlle Le Moing9, Katia Boutourlinsky10, Dominique Boucher11, Wassila Carpentier12, Patrick Berquin9, Jean-François Deleuze8, Richard Belvindrah10, Victor Borrell4, Egbert Welker13, Jamel Chelly5, Alexandre Croquelois1, Fiona Francis2.
Abstract
Neuronal migration disorders such as lissencephaly and subcortical band heterotopia are associated with epilepsy and intellectual disability. DCX, PAFAH1B1 and TUBA1A are mutated in these disorders; however, corresponding mouse mutants do not show heterotopic neurons in the neocortex. In contrast, spontaneously arisen HeCo mice display this phenotype, and our study revealed that misplaced apical progenitors contribute to heterotopia formation. While HeCo neurons migrated at the same speed as wild type, abnormally distributed dividing progenitors were found throughout the cortical wall from embryonic day 13. We identified Eml1, encoding a microtubule-associated protein, as the gene mutated in HeCo mice. Full-length transcripts were lacking as a result of a retrotransposon insertion in an intron. Eml1 knockdown mimicked the HeCo progenitor phenotype and reexpression rescued it. We further found EML1 to be mutated in ribbon-like heterotopia in humans. Our data link abnormal spindle orientations, ectopic progenitors and severe heterotopia in mouse and human.Entities:
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Year: 2014 PMID: 24859200 DOI: 10.1038/nn.3729
Source DB: PubMed Journal: Nat Neurosci ISSN: 1097-6256 Impact factor: 24.884