Abstract
The identification of mechanisms that mediate stress-induced hippocampal damage may shed new light into the pathophysiology of depressive disorders and provide new targets for therapeutic intervention. We focused on the secreted glycoprotein Dickkopf-1 (Dkk-1), an inhibitor of the canonical Wnt pathway, involved in neurodegeneration. Mice exposed to mild restraint stress showed increased hippocampal levels of Dkk-1 and reduced expression of β-catenin, an intracellular protein positively regulated by the canonical Wnt signalling pathway. In adrenalectomized mice, Dkk-1 was induced by corticosterone injection, but not by exposure to stress. Corticosterone also induced Dkk-1 in mouse organotypic hippocampal cultures and primary cultures of hippocampal neurons and, at least in the latter model, the action of corticosterone was reversed by the type-2 glucocorticoid receptor antagonist mifepristone. To examine whether induction of Dkk-1 was causally related to stress-induced hippocampal damage, we used doubleridge mice, which are characterized by a defective induction of Dkk-1. As compared to control mice, doubleridge mice showed a paradoxical increase in basal hippocampal Dkk-1 levels, but no Dkk-1 induction in response to stress. In contrast, stress reduced Dkk-1 levels in doubleridge mice. In control mice, chronic stress induced a reduction in hippocampal volume associated with neuronal loss and dendritic atrophy in the CA1 region, and a reduced neurogenesis in the dentate gyrus. Doubleridge mice were resistant to the detrimental effect of chronic stress and, instead, responded to stress with increases in dendritic arborisation and neurogenesis. Thus, the outcome of chronic stress was tightly related to changes in Dkk-1 expression in the hippocampus. These data indicate that induction of Dkk-1 is causally related to stress-induced hippocampal damage and provide the first evidence that Dkk-1 expression is regulated by corticosteroids in the central nervous system. Drugs that rescue the canonical Wnt pathway may attenuate hippocampal damage in major depression and other stress-related disorders.
Highlights
Abnormalities in mechanisms of resilience to stress are implicated in the pathophysiology of major depressive disorders [1]
The canonical Wnt pathway controls the stability of the intracellular protein, b-catenin, which, if no degraded, translocates to the nucleus, binds to lymphoid enhancer-binding factor (LEF) and T cell factor (TCF) proteins, and acts as a transcriptional co-activator to regulate the expression of Wnt-dependent genes
We show that (i) acute and chronic mild restraint stress selectively enhances Dkk-1 expression in the hippocampus; (ii) the action of stress requires the integrity of the HPA axis and is mimicked by exogenous corticosterone; and (iii) mice with hypomorphic Dkk-1 alleles are protected against stressinduced hippocampal damage
Summary
Abnormalities in mechanisms of resilience to stress are implicated in the pathophysiology of major depressive disorders [1]. The canonical Wnt pathway controls the stability of the intracellular protein, b-catenin, which, if no degraded, translocates to the nucleus, binds to lymphoid enhancer-binding factor (LEF) and T cell factor (TCF) proteins, and acts as a transcriptional co-activator to regulate the expression of Wnt-dependent genes. Induction of Dkk-1 with the ensuing inhibition of the canonical Wnt pathway has been linked to processes of neuronal death in cultures challenged with excitotoxins or b-amyloid, and in animal models of global and focal brain ischemia or temporal lobe epilepsy. Expression of Dkk-1 is increased in degenerating neurons of the Alzheimer’s brain and in hippocampal neurons of patients with mesial temporal lobe epilepsy associated with Ammon’s horn sclerosis [33,34,35,36,37]. We show that (i) acute and chronic mild restraint stress selectively enhances Dkk-1 expression in the hippocampus; (ii) the action of stress requires the integrity of the HPA axis and is mimicked by exogenous corticosterone; and (iii) mice with hypomorphic Dkk-1 alleles are protected against stressinduced hippocampal damage
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