Abstract
Noradrenaline, acting via β2- and β3- adrenoceptors (AR), enhances memory formation in single trial-discriminated avoidance learning in day-old chicks by mechanisms involving changes in metabolism of glucose and/or glycogen. Earlier studies of memory consolidation in chicks implicated β3- rather than β2-ARs in enhancement of memory consolidation by glucose, but did not elucidate whether stimulation of glucose uptake or of glycolysis was responsible. This study examines the role of glucose transport in memory formation using central injection of the nonselective facilitative glucose transporter (GLUT) inhibitor cytochalasin B, the endothelial/astrocytic GLUT-1 inhibitor phloretin and the Na+/energy-dependent endothelial glucose transporter (SGLT) inhibitor phlorizin. Cytochalasin B inhibited memory when injected into the mesopallium (avian cortex) either close to or between 25 and 45 min after training, whereas phloretin and phlorizin only inhibited memory at 30 min. This suggested that astrocytic/endothelial (GLUT-1) transport is critical at the time of consolidation, whereas a different transporter, probably the neuronal glucose transporter (GLUT-3), is important at the time of training. Inhibition of glucose transport by cytochalasin B, phloretin, or phlorizin also interfered with β3-AR-mediated memory enhancement 20 min posttraining, whereas inhibition of glycogenolysis interfered with β2-AR agonist enhancement of memory. We conclude that in astrocytes (1) activities of both GLUT-1 and SGLT are essential for memory consolidation 30 min posttraining; (2) neuronal GLUT-3 is essential at the time of training; and (3) β2- and β3-ARs consolidate memory by different mechanisms; β3-ARs stimulate central glucose transport, whereas β2-ARs stimulate central glycogenolysis. © 2008 Nature Publishing Group All rights reserved.
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Gibbs, M. E., Hutchinson, D. S., & Summers, R. J. (2008). Role of β-adrenoceptors in memory consolidation: β3- adrenoceptors act on glucose uptake and β2-adrenoceptors on glycogenolysis. Neuropsychopharmacology, 33(10), 2384–2397. https://doi.org/10.1038/sj.npp.1301629
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