Deleterious effects of soluble beta amyloid on cognition, antagonism by saline and noradrenaline, a role for microglia

Abstract

Small oligomeric beta amyloid (Aβ1–42) injected 45min prior to single-trial bead discrimination training resulted in impaired learning in day-old chickens. A new experimental protocol was used where the injections of drugs were at times around the time of injection of Aβ. It was found that the Na+ levels of the saline used to dissolve Aβ affected cognitive impairment. Na+ levels above the normal plasma value (140mM) reduced Aβ-induced learning deficits whereas levels below increased sensitivity to Aβ. The new protocol was also used to examine the ability of certain noradrenergic adrenoceptor antagonist and agonists, insulin, glucose and minocycline to reduce learning disruption caused by Aβ. The drugs (made up in 154mM sodium chloride) were injected before, at the same time or after the injection of Aβ and although all drugs prevented Aβ-induced disruption of learning when given in the same injection as Aβ, some injected before could prevent Aβ disrupting learning, whereas others could rescue learning ability when given after Aβ injection. These results are interpreted in the light of possible actions of noradrenaline on microglia and various processes: astrocytic metabolism, cerebral microcirculation, and removal of Aβ away from the site of injection. The possible importance of hypernatremia and hyponatremia in the incidence of Alzheimer’s disease is discussed.