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Three-dimensional regulation of radial glial functions by lis1-nde1 and dystrophin glycoprotein complexes
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نویسنده
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pawlisz a.s. ,feng y.
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منبع
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plos biology - 2011 - دوره : 9 - شماره : 10
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چکیده
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Radial glial cells (rgcs) are distinctive neural stem cells with an extraordinary slender bipolar morphology and dual functions as precursors and migration scaffolds for cortical neurons. here we show a novel mechanism by which the lis1-nde1 complex maintains rgc functions through stabilizing the dystrophin/dystroglycan glycoprotein complex (dgc). a direct interaction between nde1 and utrophin/dystrophin allows for the assembly of a multi-protein complex that links the cytoskeleton to the extracellular matrix of rgcs to stabilize their lateral membrane,cell-cell adhesion,and radial morphology. lis1-nde1 mutations destabilized the dgc and resulted in deformed,disjointed rgcs and disrupted basal lamina. besides impaired rgc self-renewal and neuronal migration arrests,lis1-nde1 deficiencies also led to neuronal over-migration. additional to phenotypic resemblances of lis1-nde1 with dgc,strong synergistic interactions were found between nde1 and dystroglycan in rgcs. as functional insufficiencies of lis1,nde1,and dystroglycan all cause lissencephaly syndromes,our data demonstrated that a three-dimensional regulation of rgc's cytoarchitecture by the lis1-nde1-dgc complex determines the number and spatial organization of cortical neurons as well as the size and shape of the cerebral cortex. © 2011 pawlisz,feng.
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آدرس
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department of neurology and center for genetic medicine,northwestern university feinberg school of medicine,chicago,il, United States, department of neurology and center for genetic medicine,northwestern university feinberg school of medicine,chicago,il, United States
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Authors
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