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PKC? Inhibits Neuronal Dendritic Spine Development through Dual Phosphorylation of Ephexin5.


ABSTRACT: Protein kinase C (PKC)-dependent mechanisms promote synaptic function in the mature brain. However, the roles of PKC signaling during synapse development remain largely unknown. Investigating each brain-enriched PKC isoform in early neuronal development, we show that PKC? acutely and specifically reduces the number of dendritic spines, sites of eventual synapse formation on developing dendrites. This PKC?-mediated spine suppression is temporally restricted to immature neurons and mediated through the phosphorylation and activation of Ephexin5, a RhoA guanine nucleotide exchange factor (GEF) and inhibitor of hippocampal synapse formation. Our data suggest that PKC? acts as an early developmental inhibitor of dendritic spine formation, in contrast to its emerging pro-synaptic roles in mature brain function. Moreover, we identify a substrate of PKC?, Ephexin5, whose early-elevated expression in developing neurons may in part explain the mechanism by which PKC? plays seemingly opposing roles that depend on neuronal maturity.

SUBMITTER: Schaffer TB 

PROVIDER: S-EPMC6371982 | biostudies-literature | 2018 Nov

REPOSITORIES: biostudies-literature

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PKCε Inhibits Neuronal Dendritic Spine Development through Dual Phosphorylation of Ephexin5.

Schaffer Thomas B TB   Smith Jaclyn E JE   Cook Emily K EK   Phan Thao T   Margolis Seth S SS  

Cell reports 20181101 9


Protein kinase C (PKC)-dependent mechanisms promote synaptic function in the mature brain. However, the roles of PKC signaling during synapse development remain largely unknown. Investigating each brain-enriched PKC isoform in early neuronal development, we show that PKCε acutely and specifically reduces the number of dendritic spines, sites of eventual synapse formation on developing dendrites. This PKCε-mediated spine suppression is temporally restricted to immature neurons and mediated throug  ...[more]

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