| Literature DB >> 29847800 |
Kira V Gromova1, Mary Muhia1, Nicola Rothammer1, Christine E Gee2, Edda Thies1, Irina Schaefer1, Sabrina Kress1, Manfred W Kilimann3, Olga Shevchuk4, Thomas G Oertner2, Matthias Kneussel5.
Abstract
Autism spectrum disorders (ASDs) are associated with mutations affecting synaptic components, including GluN2B-NMDA receptors (NMDARs) and neurobeachin (NBEA). NBEA participates in biosynthetic pathways to regulate synapse receptor targeting, synaptic function, cognition, and social behavior. However, the role of NBEA-mediated transport in specific trafficking routes is unclear. Here, we highlight an additional function for NBEA in the local delivery and surface re-insertion of synaptic receptors in mouse neurons. NBEA dynamically interacts with Rab4-positive recycling endosomes, transiently enters spines in an activity-dependent manner, and regulates GluN2B-NMDAR recycling. Furthermore, we show that the microtubule growth inhibitor kinesin KIF21B constrains NBEA dynamics and is present in the NBEA-recycling endosome-NMDAR complex. Notably, Kif21b knockout decreases NMDAR surface expression and alters social behavior in mice, consistent with reported social deficits in Nbea mutants. The influence of NBEA-KIF21B interactions on GluN2B-NMDAR local recycling may be relevant to mechanisms underlying ASD etiology.Entities:
Keywords: KIF21B; NMDA receptor; Rab GTPase; autism spectrum disorder; dynein; endosomal recycling; neurobeachin; retromer; social behavior; synapse
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Year: 2018 PMID: 29847800 DOI: 10.1016/j.celrep.2018.04.112
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423