| Literature DB >> 29478916 |
Marina Mikhaylova1, Julia Bär2, Bas van Bommel3, Philipp Schätzle4, PingAn YuanXiang5, Rajeev Raman5, Johannes Hradsky5, Anja Konietzny3, Egor Y Loktionov6, Pasham Parameshwar Reddy5, Jeffrey Lopez-Rojas5, Christina Spilker5, Oliver Kobler7, Syed Ahsan Raza8, Oliver Stork8, Casper C Hoogenraad4, Michael R Kreutz9.
Abstract
Compartmentalization of calcium-dependent plasticity allows for rapid actin remodeling in dendritic spines. However, molecular mechanisms for the spatio-temporal regulation of filamentous actin (F-actin) dynamics by spinous Ca2+-transients are still poorly defined. We show that the postsynaptic Ca2+ sensor caldendrin orchestrates nano-domain actin dynamics that are essential for actin remodeling in the early phase of long-term potentiation (LTP). Steep elevation in spinous [Ca2+]i disrupts an intramolecular interaction of caldendrin and allows cortactin binding. The fast on and slow off rate of this interaction keeps cortactin in an active conformation, and protects F-actin at the spine base against cofilin-induced severing. Caldendrin gene knockout results in higher synaptic actin turnover, altered nanoscale organization of spinous F-actin, defects in structural spine plasticity, LTP, and hippocampus-dependent learning. Collectively, the data indicate that caldendrin-cortactin directly couple [Ca2+]i to preserve a minimal F-actin pool that is required for actin remodeling in the early phase of LTP.Entities:
Keywords: F-actin; STED; calcium; caldendrin; cofilin; cortactin; dendritic spines; synaptic plasticity
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Year: 2018 PMID: 29478916 DOI: 10.1016/j.neuron.2018.01.046
Source DB: PubMed Journal: Neuron ISSN: 0896-6273 Impact factor: 17.173