MORPHOMETRIC EVIDENCE
FOR LITHIUM’S NEUROPROTECTIVE EFFECTS
Gwendolyn
Wood
Chronic
exposure to restraint stress, psychosocial stress, and systemic or oral
administration of the stress-hormone corticosterone (CORT) induces a
morphological reorganization in the hippocampus of rats, in which adrenal
steroids and excitatory amino acids mediate a reversible remodeling of apical
dendritic branch points and length on pyramidal cell neurons in the CA3 region
of the hippocampus (Wantanabe et al., 1992; Magarinos et al, 1995; Magarinos et
al, 1999; Conrad et al, 1999). This stress-induced “neuronal remodeling” can be
prevented with treatment with selective antidepressants and anticonvulsive drugs
(Magarinos et al., 1999). Lithium is commonly prescribed to patients with mood
disorders (Bowden 1996), and it is reported to regulate aspects of neuronal
signal transduction, such as the G-protein-coupled cyclic AMP (cAMP) pathway and
polyphosphoinositide generated second messengers. Lithium treatment has been
implicated in changes in glutamate activity, and shown to prevent glutamate
toxicity in cultured neurons (Nonaka, et al., 1998). Given previous reports of
opposing effects of chronic restraint stress versus lithium treatment, we
examined the effects of chronic lithium treatment on neuronal architecture of
the CA3 regions of the hippocampus. Our results indicate that chronic stress
results in a decrease of dendritic length and branch points on pyramidal cell
neurons in the CA3 subregion, and that these effects can be prevented with
chronic lithium treatment.