Maturation and maintenance of cholinergic medial septum neurons require glucocorticoid receptor signaling.
Department of Anatomy and Cell Biology, University of Freiburg, D-79104 Freiburg, Germany.
Glucocorticoids
have been shown to influence trophic processes in the nervous system.
In particular, they seem to be important for the development of
cholinergic neurons in various brain regions. Here, we applied a
genetic approach to investigate the role of the glucocorticoid receptor
(GR) on the maturation and maintenance of cholinergic medial septal
neurons between P15 and one year of age by using a mouse model carrying
a CNS-specific conditional inactivation of the GR gene (GRNesCre). The
number of choline acetyltransferase and p75NTR immuno-positive neurons
in the medial septum (MS) was analyzed by stereology in controls versus
mutants. In addition, cholinergic fiber density, acetylcholine release
and cholinergic key enzyme activity of these neurons were determined in
the hippocampus. We found that in GRNesCre animals the number of medial
septal cholinergic neurons was significantly reduced during
development. In addition, cholinergic cell number further decreased
with aging in these mutants. The functional GR gene is therefore
required for the proper maturation and maintenance of medial septal
cholinergic neurons. However, the loss of cholinergic neurons in the
medial septum is not accompanied by a loss of functional cholinergic
parameters of these neurons in their target region, the hippocampus.
This pinpoints to plasticity of the septo-hippocampal system, that
seems to compensate for the septal cell loss by sprouting of the
remaining neurons.
PMID: 16573657 [PubMed - indexed for MEDLINE]
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