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ProSAP1 and membrane nanodomain-associated syndapin I promote postsynapse formation and function.

J Cell Biol.. 2014-04;  205(2):197-215
Schneider K, Seemann E, Liebmann L, Ahuja R, Koch D, Westermann M, HÜbner CA, Kessels MM, Qualmann B. Institute for Biochemistry I.,Jena University Hospital, Friedrich Schiller University Jena, 07743 Jena, Germany.
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摘要

Insights into mechanisms coordinating membrane remodeling, local actin nucleation, and postsynaptic scaffolding during postsynapse formation are important for understanding vertebrate brain function. Gene knockout and RNAi in individual neurons reveal that the F-BAR protein syndapin I is a crucial postsynaptic coordinator in formation of excitatory synapses. Syndapin I deficiency caused significant reductions of synapse and dendritic spine densities. These syndapin I functions reflected direct, SH3 domain-mediated associations and functional interactions with ProSAP1/Shank2. They furthermore required F-BAR domain-mediated membrane binding. Ultra-high-resolution imaging of specifically membrane-associated, endog... More

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