COMPARATIVE ASSESSMENT OF SELECTIVE AND PAN-NMDA RECEPTOR SUBTYPE INHIBITION ON FUNCTIONAL CONNECTIVITY IN THE PREFRONTAL CORTEX BY USING AN NR2B NAM AND S-KETAMINE
Boehringer Ingelheim Pharma GmbH & Co. KG
Presentation
Date TBA
Event Information
Poster Board
PS02-07PM-278
Poster
View posterAbstract
To address these limitations, we investigated the selective negative allosteric modulator (NAM) BI 1569912 of the NR2B receptor aiming to compare its effects with those of S-Ketamine on prefrontal signal processing, focusing on PV and SST interneurons. Further, we evaluated their contributions to network disinhibition and E/I balance restoration. Whole-cell patch-clamp recordings of excitatory projection neurons were performed to measure sEPSC frequency as a proxy for network activity, optimizing the dose-dependent effects of S-Ketamine. Preliminary results demonstrated that S-Ketamine increased sEPSC frequency, indicating heightened network activity and disinhibition, while the NR2B NAM showed selective modulation of NMDA signaling.
Future investigations will include quantifying and comparing the disinhibitory effects of the NR2B NAM versus S-Ketamine, evaluating their direct inhibitory effects on PV and SST interneurons, and using optogenetic circuit mapping to characterize compound-induced network changes across PFC layers. These findings aim to clarify cell-type-specific and compound-specific mechanisms underlying E/I balance restoration, paving the way for the development of safer and more effective treatments for depression.
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