Precise levels of nectin-3 are required for proper synapse formation in postnatal visual cortex

Developing cortical neurons express a tightly choreographed sequence of cytoskeletal and transmembrane proteins to form and strengthen specific synaptic connections during circuit formation. Nectin-3 is a cell-adhesion molecule with previously described roles in synapse formation and maintenance. Th...

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Bibliographic Details
Published in:Neural development 2020-11, Vol.15 (1), p.13-13, Article 13
Main Authors: Tomorsky, Johanna, Parker, Philip R L, Doe, Chris Q, Niell, Cristopher M
Format: Article
Language:English
Subjects:
Amino acids
Animals
Brain
Critical period
Cyclin-dependent kinase inhibitor p21
Cytoskeleton
Dendritic spine density
Dendritic spines
Dendritic Spines - physiology
Deoxyribonucleic acid
Design
DNA
DNA polymerase
E coli
Electroporation
Eye
Eye opening
Female
HEK293 Cells
Humans
Hybridization
Male
Membrane proteins
Mice, Inbred C57BL
Mice, Transgenic
Nectin
Nectin-3
Nectins - metabolism
Neurons
Ocular dominance
Phosphatase
Plasmids
Postnatal development
Protein binding
RNA polymerase
Synapse formation
Synapses
Synapses - physiology
Synaptogenesis
Visual cortex
Visual Cortex - growth & development
Visual Cortex - metabolism
Visual pathways
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Summary:Developing cortical neurons express a tightly choreographed sequence of cytoskeletal and transmembrane proteins to form and strengthen specific synaptic connections during circuit formation. Nectin-3 is a cell-adhesion molecule with previously described roles in synapse formation and maintenance. This protein and its binding partner, nectin-1, are selectively expressed in upper-layer neurons of mouse visual cortex, but their role in the development of cortical circuits is unknown. Here we block nectin-3 expression (via shRNA) or overexpress nectin-3 in developing layer 2/3 visual cortical neurons using in utero electroporation. We then assay dendritic spine densities at three developmental time points: eye opening (postnatal day (P)14), one week following eye opening after a period of heightened synaptogenesis (P21), and at the close of the critical period for ocular dominance plasticity (P35). Knockdown of nectin-3 beginning at E15.5 or ~ P19 increased dendritic spine densities at P21 or P35, respectively. Conversely, overexpressing full length nectin-3 at E15.5 decreased dendritic spine densities when all ages were considered together. The effects of nectin-3 knockdown and overexpression on dendritic spine densities were most significant on proximal secondary apical dendrites. Interestingly, an even greater decrease in dendritic spine densities, particularly on basal dendrites at P21, was observed when we overexpressed nectin-3 lacking its afadin binding domain. These data collectively suggest that the proper levels and functioning of nectin-3 facilitate normal synapse formation after eye opening on apical and basal dendrites in layer 2/3 of visual cortex.
ISSN:1749-8104
1749-8104
DOI:10.1186/s13064-020-00150-w