Signaling across the synapse: a role for Wnt and Dishevelled in presynaptic assembly and neurotransmitter release

Author:

Ahmad-Annuar Azlina1,Ciani Lorenza1,Simeonidis Iordanis1,Herreros Judit1,Fredj Naila Ben1,Rosso Silvana B.1,Hall Anita1,Brickley Stephen2,Salinas Patricia C.1

Affiliation:

1. Department of Anatomy and Developmental Biology, University College London, London WC1E 6BT, England, UK

2. Department of Biological Sciences, Imperial College London, London SW8 2AY, England, UK

Abstract

Proper dialogue between presynaptic neurons and their targets is essential for correct synaptic assembly and function. At central synapses, Wnt proteins function as retrograde signals to regulate axon remodeling and the accumulation of presynaptic proteins. Loss of Wnt7a function leads to defects in the localization of presynaptic markers and in the morphology of the presynaptic axons. We show that loss of function of Dishevelled-1 (Dvl1) mimics and enhances the Wnt7a phenotype in the cerebellum. Although active zones appear normal, electrophysiological recordings in cerebellar slices from Wnt7a/Dvl1 double mutant mice reveal a defect in neurotransmitter release at mossy fiber–granule cell synapses. Deficiency in Dvl1 decreases, whereas exposure to Wnt increases, synaptic vesicle recycling in mossy fibers. Dvl increases the number of Bassoon clusters, and like other components of the Wnt pathway, it localizes to synaptic sites. These findings demonstrate that Wnts signal across the synapse on Dvl-expressing presynaptic terminals to regulate synaptic assembly and suggest a potential novel function for Wnts in neurotransmitter release.

Publisher

Rockefeller University Press

Subject

Cell Biology

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