Rejection of inappropriate synaptic partners mediated by transcellular FLRT2-UNC5 signaling

Author:

Prigge Cameron L.,Sharma Arsha,Dembla Mayur,El-Quessny Malak,Kozlowski Christopher,Paisley Caitlin E.,Johnson Tyler,Santina Luca Della,Feller Marla B.,Kay Jeremy N.ORCID

Abstract

ABSTRACTDuring nervous system development, neurons choose synaptic partners with remarkable specificity; however, the cell-cell recognition mechanisms governing rejection of inappropriate partners remain enigmatic. Here we show that mouse retinal neurons avoid inappropriate partners using the FLRT2-UNC5 receptor-ligand system. Within the inner plexiform layer (IPL), FLRT2 is expressed by direction-selective (DS) circuit neurons, whereas UNC5C/D are expressed by non-DS neurons projecting to adjacent IPL sublayers. In vivo gain- and loss-of-function experiments demonstrate that FLRT2-UNC5 binding eliminates growing DS dendrites that have strayed from the DS circuit IPL sublayers. Abrogation of FLRT2-UNC5 binding allows mistargeted arbors to persist, elaborate, and acquire synapses from inappropriate partners. Conversely, UNC5C misexpression within DS circuit sublayers inhibits dendrite growth and drives arbors into adjacent sublayers. Mechanistically, UNC5s promote dendrite elimination by interfering with FLRT2-mediated adhesion. Based on their broad expression, FLRT-UNC5 recognition is poised to exert widespread effects upon synaptic partner choices across the nervous system.

Publisher

Cold Spring Harbor Laboratory

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