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Published August 24, 2016 | Published
Journal Article Open

Phosphorylation of Synaptojanin Differentially Regulates Endocytosis of Functionally Distinct Synaptic Vesicle Pools

Abstract

The rapid replenishment of synaptic vesicles through endocytosis is crucial for sustaining synaptic transmission during intense neuronal activity. Synaptojanin (Synj), a phosphoinositide phosphatase, is known to play an important role in vesicle recycling by promoting the uncoating of clathrin following synaptic vesicle uptake. Synj has been shown to be a substrate of the minibrain (Mnb) kinase, a fly homolog of the dual-specificity tyrosine phosphorylation-regulated kinase 1A (DYRK1A); however, the functional impacts of Synj phosphorylation by Mnb are not well understood. Here we identify that Mnb phosphorylates Synj at S1029 in Drosophila. We find that phosphorylation of Synj at S1029 enhances Synj phosphatase activity, alters interaction between Synj and endophilin, and promotes efficient endocytosis of the active cycling vesicle pool (also referred to as exo-endo cycling pool) at the expense of reserve pool vesicle endocytosis. Dephosphorylated Synj, on the other hand, is deficient in the endocytosis of the active recycling pool vesicles but maintains reserve pool vesicle endocytosis to restore total vesicle pool size and sustain synaptic transmission. Together, our findings reveal a novel role for Synj in modulating reserve pool vesicle endocytosis and further indicate that dynamic phosphorylation and dephosphorylation of Synj differentially maintain endocytosis of distinct functional synaptic vesicle pools. SIGNIFICANCE STATEMENT Synaptic vesicle endocytosis sustains communication between neurons during a wide range of neuronal activities by recycling used vesicle membrane and protein components. Here we identify that Synaptojanin, a protein with a known role in synaptic vesicle endocytosis, is phosphorylated at S1029 in vivo by the Minibrain kinase. We further demonstrate that the phosphorylation status of Synaptojanin at S1029 differentially regulates its participation in the recycling of distinct synaptic vesicle pools. Our results reveal a new role for Synaptojanin in maintaining synaptic vesicle pool size and in reserve vesicle endocytosis. As Synaptojanin and Minibrain perturbations are associated with various neurological disorders, such as Parkinson's, autism, and Down syndrome, understanding mechanisms modulating Synaptojanin function provides valuable insights into processes affecting neuronal communication.

Additional Information

© 2016 the authors. The authors grant the Society for Neuroscience an exclusive license to publish their work for the first 6 months. After 6 months the work becomes available to the public to copy, distribute, or display under a Creative Commons Attribution 4.0 International (CC BY 4.0) license. Received May 4, 2016; revised July 11, 2016; accepted July 14, 2016. This work was supported by National Institutes of Health Grant NS080946 and Alzheimer's Association and Global Down Syndrome Foundation to K.T.C. We thank Martin Heisenberg (University of Wuzburg, Wuzburg, Germany) for the mnb^1 stock; Hugo Bellen (Baylor University, Waco, Texas) for generous sharing of synj^1 and synj^2 flies, endophilin antibody, and synaptojanin antibody, which we renamed here to p-Synj for clarification; Syed Qadri for performing preliminary experiments; and the Developmental Studies Hybridoma Bank (Iowa City, Iowa) for antibodies. Author contributions: K.T.C. designed research; J.G., L.W., J.Y.L., and C.-K.C. performed research; J.G., L.W., J.Y.L., C.-K.C., and K.T.C. analyzed data; J.G., L.W., and K.T.C. wrote the paper. G.G. and L.W. contributed equally to this study. The authors declare no competing financial interests.

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August 22, 2023
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