Synapse-specific trapping of Syntaxin1a into nanoclusters by the general anesthetic isoflurane

Abstract: SummaryGeneral anesthetics disrupt brain network dynamics through multiple pathways, predominately through post-synaptic potentiation of GABAAR and pre-synaptic inhibition of neuroexocytosis. Common clinical general anesthetic drugs, such as propofol and isoflurane, have been shown to interact and interfere with a core component of the exocytic release machinery, Syntaxin1A, to cause impaired neurotransmitter release. Recent in vitro studies however suggest that these drugs to not affect all synapse subtypes e… Show more