Agonist-induced PKC phosphorylation regulates GluK2 SUMOylation and kainate receptor endocytosis
Publication date
2011Author
Konopacki, F.A.Jaafari, N.
Rocca, D.L.
Wilkinson, K.A.
Chamberlain, S.E.
Rubin, P.
Kantamneni, Sriharsha
Mellor, J.R.
Henley, J.M.
Keyword
AlanineAmino acid substitution
Animals
Blotting
Western
COS cells
Cercopithecus aethiops
Endocytosis
HEK293 cells
Humans
Kainic acid
Luminescent proteins
Microscopy
Mutation
Neurons
Phosphorylation
Protein kinase C
Rats
Wistar
Receptors
SUMO-1 Protein
Serine
Sumoylation
REF 2014
Peer-Reviewed
YesOpen Access status
closedAccess
Metadata
Show full item recordAbstract
The surface expression and regulated endocytosis of kainate (KA) receptors (KARs) plays a critical role in neuronal function. PKC can modulate KAR trafficking, but the sites of action and molecular consequences have not been fully characterized. Small ubiquitin-like modifier (SUMO) modification of the KAR subunit GluK2 mediates agonist-evoked internalization, but how KAR activation leads to GluK2 SUMOylation is unclear. Here we show that KA stimulation causes rapid phosphorylation of GluK2 by PKC, and that PKC activation increases GluK2 SUMOylation both in vitro and in neurons. The intracellular C-terminal domain of GluK2 contains two predicted PKC phosphorylation sites, S846 and S868, both of which are phosphorylated in response to KA. Phosphomimetic mutagenesis of S868 increased GluK2 SUMOylation, and mutation of S868 to a nonphosphorylatable alanine prevented KA-induced SUMOylation and endocytosis in neurons. Infusion of SUMO-1 dramatically reduced KAR-mediated currents in HEK293 cells expressing WT GluK2 or nonphosphorylatable S846A mutant, but had no effect on currents mediated by the S868A mutant. These data demonstrate that agonist activation of GluK2 promotes PKC-dependent phosphorylation of S846 and S868, but that only S868 phosphorylation is required to enhance GluK2 SUMOylation and promote endocytosis. Thus, direct phosphorylation by PKC and GluK2 SUMOylation are intimately linked in regulating the surface expression and function of GluK2-containing KARs.Version
No full-text in the repositoryCitation
Konopacki FA, Jaafari N, Rocca DL et al (2011) Agonist-induced PKC phosphorylation regulates GluK2 SUMOylation and kainate receptor endocytosis. Proceedings of the National Academy of Sciences of the United States of America. 108(49): 19772-19777.Link to Version of Record
https://doi.org/10.1073/pnas.1111575108Type
Articleae974a485f413a2113503eed53cd6c53
https://doi.org/10.1073/pnas.1111575108