Synaptic vesicle proteins and ATG9A self-organize in distinct vesicle phases within synapsin condensates

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作者
Daehun Park
Yumei Wu
Xinbo Wang
Swetha Gowrishankar
Aaron Baublis
Pietro De Camilli
机构
[1] Yale University School of Medicine,Department of Neuroscience
[2] Yale University School of Medicine,Department of Cell Biology
[3] Yale University School of Medicine,Howard Hughes Medical Institute
[4] Yale University School of Medicine,Program in Cellular Neuroscience, Neurodegeneration, and Repair
[5] University of Illinois at Chicago,Department of Anatomy and Cell Biology, College of Medicine
[6] Harvard T.H. Chan School of Public Health,Harvard Chan Advanced Multi
[7] Yale University School of Medicine,omics Platform
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Ectopic expression in fibroblasts of synapsin 1 and synaptophysin is sufficient to generate condensates of vesicles highly reminiscent of synaptic vesicle (SV) clusters and with liquid-like properties. Here we show that unlike synaptophysin, other major integral SV membrane proteins fail to form condensates with synapsin, but co-assemble into the clusters formed by synaptophysin and synapsin in this ectopic expression system. Another vesicle membrane protein, ATG9A, undergoes activity-dependent exo-endocytosis at synapses, raising questions about the relation of ATG9A traffic to the traffic of SVs. We find that both in fibroblasts and in nerve terminals ATG9A does not co-assemble into synaptophysin-positive vesicle condensates but localizes on a distinct class of vesicles that also assembles with synapsin but into a distinct phase. Our findings suggest that ATG9A undergoes differential sorting relative to SV proteins and also point to a dual role of synapsin in controlling clustering at synapses of SVs and ATG9A vesicles.
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