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?-Pix modulates actin-mediated recruitment of synaptic vesicles to synapses.


ABSTRACT: Presynaptic compartments are formed through the recruitment of preassembled clusters of proteins to points of cell-cell contact, however, the molecular mechanism(s) underlying this process remains unclear. We demonstrate that clusters of polymerized actin can recruit and maintain synaptic vesicles to discrete sites along the axon, and that cadherin/?-catenin/scribble/?-pix complexes play an important role in this event. Previous work has demonstrated that ?-catenin and scribble are important for the clustering of vesicles at synapses. We demonstrate that ?-pix, a Rac/Cdc42 guanine nucleotide exchange factor (GEF), forms a complex with cadherin, ?-catenin, and scribble at synapses and enhances localized actin polymerization in rat hippocampal neurons. In cells expressing ?-pix siRNA or dominant-negative ?-pix that lacks its GEF activity, actin polymerization at synapses is dramatically reduced, and synaptic vesicle localization is disrupted. This ?-pix phenotype can be rescued by cortactin overexpression, suggesting that ?-pix-mediated actin polymerization at synapses regulates vesicle localization.

SUBMITTER: Sun Y 

PROVIDER: S-EPMC6623868 | biostudies-literature | 2011 Nov

REPOSITORIES: biostudies-literature

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β-Pix modulates actin-mediated recruitment of synaptic vesicles to synapses.

Sun Yu Y   Bamji Shernaz X SX  

The Journal of neuroscience : the official journal of the Society for Neuroscience 20111101 47


Presynaptic compartments are formed through the recruitment of preassembled clusters of proteins to points of cell-cell contact, however, the molecular mechanism(s) underlying this process remains unclear. We demonstrate that clusters of polymerized actin can recruit and maintain synaptic vesicles to discrete sites along the axon, and that cadherin/β-catenin/scribble/β-pix complexes play an important role in this event. Previous work has demonstrated that β-catenin and scribble are important for  ...[more]

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