Regulation of DLG localization at synapses by CaMKII-dependent phosphorylation

Young Ho Koh; Evgenya Popova; Ulrich Thomas; Leslie C. Griffith; Vivian Budnik

doi:10.1016/S0092-8674(00)81964-9

Regulation of DLG localization at synapses by CaMKII-dependent phosphorylation

Young Ho Koh, Evgenya Popova, Ulrich Thomas, Leslie C. Griffith, Vivian Budnik

Research output: Contribution to journal › Article › peer-review

214 Scopus citations

Abstract

Discs large (DLG) mediates the clustering of synaptic molecules. Here we demonstrate that synaptic localization of DLG itself is regulated by CaMKII. We show that DLG and CaMKII colocalize at synapses and exist in the same protein complex. Constitutively activated CaMKII phenocopied structural abnormalities of dig mutant synapses and dramatically increased extrajunctional DLG. Decreased CaMKII activity caused opposite alterations. In vitro, CaMKII phosphorylated a DLG fragment with a stoichiometry close to one. Moreover, expression of site-directed dig mutants that blocked or mimicked phosphorylation had effects similar to those observed upon inhibiting or constitutively activating CaMKII. We propose that CaMKII- dependent DLG phosphorylation regulates the association of DLG with the synaptic complex during development and plasticity, thus providing a link between synaptic activity and structure.

Original language	English (US)
Pages (from-to)	353-363
Number of pages	11
Journal	Cell
Volume	98
Issue number	3
DOIs	https://doi.org/10.1016/S0092-8674(00)81964-9
State	Published - Aug 6 1999

All Science Journal Classification (ASJC) codes

General Biochemistry, Genetics and Molecular Biology

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10.1016/S0092-8674(00)81964-9

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title = "Regulation of DLG localization at synapses by CaMKII-dependent phosphorylation",

abstract = "Discs large (DLG) mediates the clustering of synaptic molecules. Here we demonstrate that synaptic localization of DLG itself is regulated by CaMKII. We show that DLG and CaMKII colocalize at synapses and exist in the same protein complex. Constitutively activated CaMKII phenocopied structural abnormalities of dig mutant synapses and dramatically increased extrajunctional DLG. Decreased CaMKII activity caused opposite alterations. In vitro, CaMKII phosphorylated a DLG fragment with a stoichiometry close to one. Moreover, expression of site-directed dig mutants that blocked or mimicked phosphorylation had effects similar to those observed upon inhibiting or constitutively activating CaMKII. We propose that CaMKII- dependent DLG phosphorylation regulates the association of DLG with the synaptic complex during development and plasticity, thus providing a link between synaptic activity and structure.",

author = "Koh, {Young Ho} and Evgenya Popova and Ulrich Thomas and Griffith, {Leslie C.} and Vivian Budnik",

note = "Funding Information: We thank Xiaomeng Long for generating the CaMKII antibody; Michael Gorczyca and Mary Packard for critical reading of the manuscript and helpful discussions; and Mary Packard for help with EM. We also thank the EM Facility and the Biology Computer Resource Center (BCRC) at the University of Massachusetts. This paper was supported by NIH grants RO1 NS30072 and KO4 NS01786 and R01 GM54408 and K02 NS01897 (to V. B. and L. C. G., respectively). U. T. was supported by the Max Kade Foundation.",

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doi = "10.1016/S0092-8674(00)81964-9",

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T1 - Regulation of DLG localization at synapses by CaMKII-dependent phosphorylation

AU - Koh, Young Ho

AU - Popova, Evgenya

AU - Thomas, Ulrich

AU - Griffith, Leslie C.

AU - Budnik, Vivian

N1 - Funding Information: We thank Xiaomeng Long for generating the CaMKII antibody; Michael Gorczyca and Mary Packard for critical reading of the manuscript and helpful discussions; and Mary Packard for help with EM. We also thank the EM Facility and the Biology Computer Resource Center (BCRC) at the University of Massachusetts. This paper was supported by NIH grants RO1 NS30072 and KO4 NS01786 and R01 GM54408 and K02 NS01897 (to V. B. and L. C. G., respectively). U. T. was supported by the Max Kade Foundation.

PY - 1999/8/6

Y1 - 1999/8/6

N2 - Discs large (DLG) mediates the clustering of synaptic molecules. Here we demonstrate that synaptic localization of DLG itself is regulated by CaMKII. We show that DLG and CaMKII colocalize at synapses and exist in the same protein complex. Constitutively activated CaMKII phenocopied structural abnormalities of dig mutant synapses and dramatically increased extrajunctional DLG. Decreased CaMKII activity caused opposite alterations. In vitro, CaMKII phosphorylated a DLG fragment with a stoichiometry close to one. Moreover, expression of site-directed dig mutants that blocked or mimicked phosphorylation had effects similar to those observed upon inhibiting or constitutively activating CaMKII. We propose that CaMKII- dependent DLG phosphorylation regulates the association of DLG with the synaptic complex during development and plasticity, thus providing a link between synaptic activity and structure.

AB - Discs large (DLG) mediates the clustering of synaptic molecules. Here we demonstrate that synaptic localization of DLG itself is regulated by CaMKII. We show that DLG and CaMKII colocalize at synapses and exist in the same protein complex. Constitutively activated CaMKII phenocopied structural abnormalities of dig mutant synapses and dramatically increased extrajunctional DLG. Decreased CaMKII activity caused opposite alterations. In vitro, CaMKII phosphorylated a DLG fragment with a stoichiometry close to one. Moreover, expression of site-directed dig mutants that blocked or mimicked phosphorylation had effects similar to those observed upon inhibiting or constitutively activating CaMKII. We propose that CaMKII- dependent DLG phosphorylation regulates the association of DLG with the synaptic complex during development and plasticity, thus providing a link between synaptic activity and structure.

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Regulation of DLG localization at synapses by CaMKII-dependent phosphorylation

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