| Literature DB >> 28475893 |
Daniel Del Toro1, Tobias Ruff1, Erik Cederfjäll1, Ana Villalba2, Gönül Seyit-Bremer1, Víctor Borrell2, Rüdiger Klein3.
Abstract
The folding of the mammalian cerebral cortex into sulci and gyri is thought to be favored by the amplification of basal progenitor cells and their tangential migration. Here, we provide a molecular mechanism for the role of migration in this process by showing that changes in intercellular adhesion of migrating cortical neurons result in cortical folding. Mice with deletions of FLRT1 and FLRT3 adhesion molecules develop macroscopic sulci with preserved layered organization and radial glial morphology. Cortex folding in these mutants does not require progenitor cell amplification but is dependent on changes in neuron migration. Analyses and simulations suggest that sulcus formation in the absence of FLRT1/3 results from reduced intercellular adhesion, increased neuron migration, and clustering in the cortical plate. Notably, FLRT1/3 expression is low in the human cortex and in future sulcus areas of ferrets, suggesting that intercellular adhesion is a key regulator of cortical folding across species.Entities:
Keywords: FLRT1; FLRT3; cell adhesion; cortex; folding; neuronal migration
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Year: 2017 PMID: 28475893 DOI: 10.1016/j.cell.2017.04.012
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 66.850