Oligodendrocyte precursor cells modulate the neuronal network by activity-dependent ectodomain cleavage of glial NG2.

6533b7d4fe1ef96bd1262a8e

RESEARCH PRODUCT

Oligodendrocyte precursor cells modulate the neuronal network by activity-dependent ectodomain cleavage of glial NG2.

Dominik Sakry Jeet Singh Daniele Marongiu Beat Lutz Kristina Endres Sumudhu S. Perera Thomas Mittmann Fabien Binamé Angela Neitz Konstantin Radyushkin Renato Frischknecht Jacqueline Trotter

subject

Male QH301-705.5 ADAM10 Long-Term Potentiation AMPA receptor Receptors N-Methyl-D-Aspartate General Biochemistry Genetics and Molecular Biology Cell Line ADAM10 Protein Mice Biological neural network Animals Biology (General)Antigens Mice Knockout Neurons Neuronal Plasticity General Immunology and Microbiology biology General Neuroscience Pyramidal Cells Glutamate receptor Membrane Proteins Biology and Life Sciences Long-term potentiation Sensory Gating Cell biology Extracellular Matrix Protein Structure Tertiary stomatognathic diseases ADAM Proteins Oligodendroglia Biochemistry Ectodomain nervous system Receptors Glutamate Synapses biology.protein Synopsis NMDA receptor Proteoglycans Amyloid Precursor Protein Secretases General Agricultural and Biological Sciences Amyloid precursor protein secretase Neuroscience

description

The role of glia in modulating neuronal network activity is an important question. Oligodendrocyte precursor cells (OPC) characteristically express the transmembrane proteoglycan nerve-glia antigen 2 (NG2) and are unique glial cells receiving synaptic input from neurons. The development of NG2+ OPC into myelinating oligodendrocytes has been well studied, yet the retention of a large population of synapse-bearing OPC in the adult brain poses the question as to additional functional roles of OPC in the neuronal network. Here we report that activity-dependent processing of NG2 by OPC-expressed secretases functionally regulates the neuronal network. NG2 cleavage by the α-secretase ADAM10 yields an ectodomain present in the extracellular matrix and a C-terminal fragment that is subsequently further processed by the γ-secretase to release an intracellular domain. ADAM10-dependent NG2 ectodomain cleavage and release (shedding) in acute brain slices or isolated OPC is increased by distinct activity-increasing stimuli. Lack of NG2 expression in OPC (NG2-knockout mice), or pharmacological inhibition of NG2 ectodomain shedding in wild-type OPC, results in a striking reduction of N-methyl-D-aspartate (NMDA) receptor-dependent long-term potentiation (LTP) in pyramidal neurons of the somatosensory cortex and alterations in the subunit composition of their α-amino-3-hydroxy-5-methyl-4-isoxazolepr opionicacid (AMPA) receptors. In NG2-knockout mice these neurons exhibit diminished AMPA and NMDA receptor-dependent current amplitudes; strikingly AMPA receptor currents can be rescued by application of conserved LNS protein domains of the NG2 ectodomain. Furthermore, NG2-knockout mice exhibit altered behavior in tests measuring sensorimotor function. These results demonstrate for the first time a bidirectional cross-talk between OPC and the surrounding neuronal network and demonstrate a novel physiological role for OPC in regulating information processing at neuronal synapses.

year	journal	country	edition	language
2014-11-01	PLoS biology

10.1371/journal.pbio.1001993 https://pubmed.ncbi.nlm.nih.gov/25386988