A proteomic screen of neuronal cell-surface molecules reveals IgLONs as structurally conserved interaction modules at the synapse
Date
2019
Authors
Ranaivoson, Fanomezana M.
Turk, Liam S.
Ozgul, Sinem
Kakehi, Sumie
von Daake, Sventja
Lopez, Nicole
Trobiani, Laura
De Jaco, Antonella
Denissova, Natalia
Demeler, Borries
Journal Title
Journal ISSN
Volume Title
Publisher
Cell Press
Abstract
In the developing brain, cell-surface proteins play crucial roles, but their protein-protein interaction network remains largely unknown. A proteomic screen identified 200 interactions, 89 of which were not previously published. Among these interactions, we find that the IgLONs, a family of five cell-surface neuronal proteins implicated in various human disorders, interact as homo- and heterodimers. We reveal their interaction patterns and report the dimeric crystal structures of Neurotrimin (NTRI), IgLON5, and the neuronal growth regulator 1 (NEGR1)/IgLON5 complex. We show that IgLONs maintain an extended conformation and that their dimerization occurs through the first Ig domain of each monomer and is Ca2+ independent. Cell aggregation shows that NTRI and NEGR1 homo- and heterodimerize in trans. Taken together, we report 89 unpublished cell-surface ligand-receptor pairs and describe structural models of trans interactions of IgLONs, showing that their structures are compatible with a model of interaction across the synaptic cleft.
Description
Accepted author manuscript
Keywords
Ligand-receptor pair , ELISA , IgLON , Protein crystallography , SAXS , Cell-surface
Citation
Ranaivoson, F. M., Turk, L. S., Ozgul, S., Kakehi, S., von Daake, S., Lopez, N., Trobiani, L., De Jaco, A., Denissova, N., Demeler, B., Özcan, E., Montelione, G. T., & Comoletti, D. (2019). A proteomic screen of neuronal cell-surface molecules reveals IgLONs as structurally conserved interaction molecules at the synapse. Structure, 27(6), 893-906. https://doi.org/10.1016/j.str.2019.03.004