LAUSR

HighlightsActivation of BLA (glutamate, idazoxan or isoprenaline) impaired H‐PFC LTP.Inhibition of BLA (muscimol, NA, clonidine or propranolol) enhanced H‐PFC LTP.The BLA negatively regulates H‐PFC plasticity.NA in BLA affects H‐PFC plasticity via alpha‐2 and beta adrenoceptors. ABSTRACT Noradrenaline (NA), released by the locus coeruleus (LC), plays a key role in mediating the effects of stress on memory functions. The LC provides diffuse projections to many forebrain nuclei including the hippocampus, the prefrontal cortex (PFC), and the basolateral amygdala (BLA). These three structures are intricately interlinked. The hippocampal‐prefrontal (H‐PFC) pathway is involved in various cognitive functions. The first aim of this study was to examine the role of BLA in H‐PFC plasticity by infusion of drugs to activate and inactivate the BLA and studying the effects on H‐PFC long‐term potentiation (LTP) in the rat in vivo. Activation of the BLA with glutamate impaired, while inactivation with muscimol augmented, H‐PFC LTP. This study also aimed to demonstrate how directly applying noradrenaline and other noradrenergic agents in the BLA can affect H‐PFC LTP. Noradrenaline at 1 &mgr;g/0.2 &mgr;l enhanced H‐PFC LTP. Stimulating alpha‐2‐adrenoceptors in the BLA with clonidine enhanced LTP while blocking alpha‐2 adrenoceptors with idazoxan impaired it. Propranolol, a non‐selective beta antagonist, enhanced H‐PFC LTP while isoprenaline, a non‐selective beta agonist, decreased H‐PFC LTP. These results suggest that the BLA regulates H‐PFC plasticity negatively and also provide a mechanism by which noradrenaline in the BLA can affect H‐PFC plasticity via alpha‐2 and beta adrenoceptors.