Skip to main content
Search
Main content
EMBO J
Published

Seizure protein 6 controls glycosylation and trafficking of kainate receptor subunits GluK2 and GluK3.

Authors

Martina Pigoni, Hung-En Hsia, Jana Hartmann, Jasenka Rudan Njavro, Merav D Shmueli, Stephan A Müller, Gökhan Güner, Johanna Tüshaus, Peer-Hendrik Kuhn, Rohit Kumar, Pan Gao, Mai Ly Tran, Bulat Ramazanov, Birgit Blank, Agnes L Hipgrave Ederveen, Julia Von Blume, Christophe Mulle, Jenny M Gunnersen, Manfred Wuhrer, Gerhard Rammes, Marc Aurel Busche, Thomas Koeglsperger, Stefan F Lichtenthaler

Abstract

Seizure protein 6 (SEZ6) is required for the development and maintenance of the nervous system, is a major substrate of the protease BACE1 and is linked to Alzheimer's disease (AD) and psychiatric disorders, but its molecular functions are not well understood. Here, we demonstrate that SEZ6 controls glycosylation and cell surface localization of kainate receptors composed of GluK2/3 subunits. Loss of SEZ6 reduced surface levels of GluK2/3 in primary neurons and reduced kainate-evoked currents in CA1 pyramidal neurons in acute hippocampal slices. Mechanistically, loss of SEZ6 in vitro and in vivo prevented modification of GluK2/3 with the human natural killer-1 (HNK-1) glycan, a modulator of GluK2/3 function. SEZ6 interacted with GluK2 through its ectodomain and promoted post-endoplasmic reticulum transport of GluK2 in the secretory pathway in heterologous cells and primary neurons. Taken together, SEZ6 acts as a new trafficking factor for GluK2/3. This novel function may help to better understand the role of SEZ6 in neurologic and psychiatric diseases.

PMID:32567721 | DOI:10.15252/embj.2019103457

UK DRI Authors

Marc Aurel Busche profile picture

Dr Marc Aurel Busche

Group Leader

Understanding and repairing pathological neural circuits in Alzheimer's disease

Dr Marc Aurel Busche