Lohals R, Veng LM (2005) Cholinergic therapy does not rescue spatial learning deficits induced by ICV injection of 192 IgG-saporin. Neuroscience 2005 Abstracts 653.5. Society for Neuroscience, Washington, DC.
Summary: The cholinergic hypothesis states that central cholinergic dysfunction is responsible for age-dependent cognitive decline. To model this in rats, we induced cholinergic basal forebrain loss the neurotoxin IgG192-saporin (SAP). Following ICV infusion of 2.5 or 5 microgram (ug) SAP, or saline, rats were tested in the radial 12-arm water maze (RAWM), a spatial learning and memory task. While saline sham or 2.5 ug SAP lesioned rats showed normal learning over 4 trials in the RAWM, 5 ug SAP rats were impaired. However, when trained over 20 trials, 5 ug SAP rats eventually attained the same level of performance as 2.5 ug SAP or saline sham rats, and 28 days later all rats showed intact memory for this platform location. In the open field, 5 ug SAP rats failed to habituate. However, SAP or saline sham lesioned rats did not differ in basal activity, rotarod, or visually cued RAWM performance. SAP lesion resulted in severe depletion of ChAT activity in hippocampus and cortex, which significantly correlated with learning impairment in the RAWM. In a second experiment, we used 5 ug ICV SAP to investigate the effect of cholinergic therapy on SAP-induced spatial learning deficits in the RAWM. However, neither galantamine (0.30, 1.25, 5.0 mg/kg) nor RJR-2403 (0.08, 0.31, 1.25 mg/kg) could reverse the SAP induced deficit in RAWM learning. In conclusion, we found that spatial learning in the RAWM was consistently impaired following severe (5.0 ug SAP) cholinergic basal forebrain lesion in rats. This learning deficit was not confounded by general behavioral disturbances. However, with excessive training SAP lesioned rats could learn and later recall spatial information, suggesting that recall is intact in cholinergic lesioned animals. Severe SAP lesion also impaired habituation in an open field and this was not due to hyperactivity. Finally, treatment with galantamine and RJR-2403 did not alleviate the cognitive deficit induced by the SAP lesion, likely due to the severity of cholinergic depletion.
Related Products: 192-IgG-SAP (Cat. #IT-01)