Loss of Cholinergic Phenotype in Basal Forebrain Coincides with Cognitive Decline in a Mouse Model of Down's Syndrome

• Published in: Experimental neurology Vol. 161; no. 2; pp. 647 - 663
• Main Authors: Granholm, Ann-Charlotte E., Sanders, Linda A., Crnic, Linda S.
• Format: Journal Article
• Language: English
• Published: United States Elsevier Inc 01.02.2000
• Subjects: acetylcholine; Animals; basal forebrain; Choline O-Acetyltransferase - analysis; Chromosome Mapping; Cognition Disorders - etiology; Cognition Disorders - physiopathology; Crosses, Genetic; Discrimination Learning; Disease Models, Animal; Down Syndrome - genetics; Down Syndrome - physiopathology; Down Syndrome - psychology; Female; Functional Laterality; Male; Maze Learning; memory and learning; Mice; Mice, Inbred C57BL; Mice, Inbred DBA; Mice, Mutant Strains; nerve growth factor receptors; neurodegeneration; Neurons - pathology; Neurons - physiology; Prosencephalon - enzymology; Prosencephalon - pathology; Prosencephalon - physiopathology; Receptor, trkA - analysis; Space Perception; Testis - radiation effects; Trisomy; neurodegeneration; nerve growth factor receptors; acetylcholine; memory and learning; basal forebrain
• ISSN: 0014-4886; 1090-2430
• DOI: 10.1006/exnr.1999.7289

Mice with segmental trisomy of chromosome 16 (Ts65Dn) have been used as a model for Down's syndrome. These mice are born with a normal density of basal forebrain cholinergic neurons but, like patients with Down's syndrome, undergo a significant deterioration of these neurons later in life. The time course for this degeneration of cholinergic neurons has not been studied, nor is it known if it correlates with the progressive memory and learning deficits described. Ts65Dn mice that were 4, 6, 8, and 10 months old were sacrificed for evaluation of basal forebrain morphology. Separate groups of mice were tested on visual or spatial discrimination learning and reversal. We found no alterations in cholinergic markers in 4-month-old Ts65Dn mice, but thereafter a progressive decline in density of cholinergic neurons, as well as significant shrinkage of cell body size, was seen. A parallel loss of staining for the high-affinity nerve growth factor receptor, trkA, was observed at all time points, suggesting a biological mechanism for the cell loss involving this growth factor. Other than transient difficulty in learning the task requirements, there was no impairment of trisomic mice on visual discrimination learning and reversal, whereas spatial learning and reversal showed significant deficits, particularly in the mice over 6 months of age. Thus, the loss of ChAT-immunoreactive neurons in the basal forebrain was coupled with simultaneous deficits in behavioral flexibility on a spatial task occurring for the first time around 6 months of age. These findings suggest that the loss of cholinergic function and the simultaneous decrease in trkA immunoreactivity in basal forebrain may directly correlate with cognitive impairment in the Ts65Dn mouse