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Enhanced TARP-γ8-PSD-95 coupling in excitatory neurons contributes to the rapid antidepressant-like action of ketamine in male mice

Shi-Ge Xue, Jin‐Gang He, Lingli Lu, Shi-Jie Song, Meimei Chen, Fang Wang, Jianguo Chen

2023Nature Communications23 citationsDOIOpen Access PDF

Abstract

Ketamine produces rapid antidepressant effects at sub-anesthetic dosage through early and sustained activation of α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptors (AMPARs), however, the exact molecular mechanism still remains unclear. Transmembrane AMPAR regulatory protein-γ8 (TARP-γ8) is identified as one of AMPAR auxiliary subunits, which controls assemblies, surface trafficking and gating of AMPARs. Here, we show that ketamine rescues both depressive-like behaviors and the decreased AMPARs-mediated neurotransmission by recruitment of TARP-γ8 at the postsynaptic sites in the ventral hippocampus of stressed male mice. Furthermore, the rapid antidepressant effects of ketamine are abolished by selective blockade of TARP-γ8-containing AMPAR or uncoupling of TARP-γ8 from PSD-95. Overexpression of TARP-γ8 reverses chronic stress-induced depressive-like behaviors and attenuation of AMPARs-mediated neurotransmission. Conversely, knockdown of TARP-γ8 in excitatory neurons prevents the rapid antidepressant effects of ketamine.

Topics & Concepts

AMPA receptorKetamineNeurotransmissionExcitatory postsynaptic potentialAntidepressantGlutamate receptorNeuroscienceGlutamatergicPharmacologyChemistryHippocampusNMDA receptorPostsynaptic potentialReceptorMedicineBiologyInhibitory postsynaptic potentialBiochemistryTreatment of Major DepressionTryptophan and brain disordersNeuroscience and Neuropharmacology Research
Enhanced TARP-γ8-PSD-95 coupling in excitatory neurons contributes to the rapid antidepressant-like action of ketamine in male mice | Litcius