Conditionally immortal neuroepithelial stem cell grafts restore
spatial learning in rats with lesions at the source of cholinergic forebrain
projections cholinergic forebrain projections Conditionally immortal
neuroepithelial stem cell grafts restore spatial leaming in rats with lesions
at the source of cholinergic forebrain projections
Affiliations: Department of Psychology, Institute of Psychiatry,
King's College London, De Crespigny Park, Denmark Hill, London SE5 8AF UK | ReNeuron Ltd., Institute of Psychiatry, King's College
London, De Crespigny Park, Denmark Hill, London SE5 8AF UK
Abstract: Purpose: Loss of cholinergic projections from the basal forebrain
(BF) to the cortex and from the medial septal area (MSA) to tbe hippocampus is
a reliable correlate of cognitive deficits in aging and Alzheimer's disease
(AD). We assessed the capacity of grafts of the conditionally immortal MHP36
clonal stem cell line to improve spatial learning in rats showing profound
deficits after lesions to these projections. Methods: Rats were lesioned by
infusions of S-AMPA unilaterally into BF or bilaterally into both BF and MSA.
MHP36 cells were implanted ipsilaterally in cortex or basal forebrain two weeks
after unilateral BF lesions, and in cortex and hippocampus bilaterally six
months after bilateral BF-MSA lesions. Intact and lesion-only controls received
vehicle. Six weeks later rats were assessed in spatial learning and memory
tasks in the water maze, and then perfused for identification of grafted cells
by β-galactosidase immunohistocheniistry. Results: Lesioned rats with
MHP36 grafts, whether implanted two weeks or six months after lesioning,
learned to find a submerged platform in the water maze as rapidly as intact
controls, and showed a strong preference for the platform quadrant on probe
trials, whereas lesioned controls were impaired in all measures. Grafted cells
of both neuronal and glial morphologies, migrated away from cortical
implantation sites in BF Lesioned rats to the striatum, thalamus and basal
forebrain lesion area. Cells implanted in basal forebrain showed a similar
distribution. In rats with bilateral BF-MSA lesions, grafts implanted in the
hippocampus migrated widely through all layers but cortical grafts largely
escaped up the needle tract into the meninges. Conclusions: Although MHP36
grafts were functionally effective in both lesion models, the site and age of
lesions and site of implantation influenced the pattern of engraftment. This
flexibility encourages the development of conditionally immortal human stem
cell lines with similar capacities for functional repair of variable neuronal
degeneration in AD or aging.
Keywords: cholinergic lesions, conditionally immortal stem cells, water maze, β-galactosidase
