4.5 Article

Differential Regulation of Wnt Signaling Components During Hippocampal Reorganization After Entorhinal Cortex Lesion

Journal

CELLULAR AND MOLECULAR NEUROBIOLOGY
Volume 41, Issue 3, Pages 537-549

Publisher

SPRINGER/PLENUM PUBLISHERS
DOI: 10.1007/s10571-020-00870-x

Keywords

Wnt signaling; Wnt7a; Hippocampal reorganization; Entorhinal cortex lesion; Perforant pathway

Funding

  1. CONACYT [254792, A1-S-9559]
  2. PAPIIT
  3. DGAPA [IN202318]

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Entorhinal cortex lesions have been found to affect the reorganization of the dentate gyrus, with Wnt signaling components playing a crucial role in this process. The activation of the canonical Wnt pathway after lesion correlates with structural adaptations in the dentate gyrus, indicating the potential of modulating this pathway for neuronal tissue regeneration.
Entorhinal cortex lesions have been established as a model for hippocampal deafferentation and have provided valuable information about the mechanisms of synapse reorganization and plasticity. Although several molecules have been proposed to contribute to these processes, the role of Wnt signaling components has not been explored, despite the critical roles that Wnt molecules play in the formation and maintenance of neuronal and synaptic structure and function in the adult brain. In this work, we assessed the reorganization process of the dentate gyrus (DG) at 1, 3, 7, and 30 days after an excitotoxic lesion in layer II of the entorhinal cortex. We found that cholinergic fibers sprouted into the outer molecular layer of the DG and revealed an increase of the developmental regulated MAP2C isoform 7 days after lesion. These structural changes were accompanied by the differential regulation of the Wnt signaling components Wnt7a, Wnt5a, Dkk1, and Sfrp1 over time. The progressive increase in the downstream Wnt-regulated elements, active-beta-catenin, and cyclin D1 suggested the activation of the canonical Wnt pathway beginning on day 7 after lesion, which correlates with the structural adaptations observed in the DG. These findings suggest the important role of Wnt signaling in the reorganization processes after brain lesion and indicate the modulation of this pathway as an interesting target for neuronal tissue regeneration.

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