RESUMO
The function of medial entorhinal cortex layer II (MECII) excitatory neurons has been recently explored. MECII dysfunction underlies deficits in spatial navigation and working memory. MECII neurons comprise two major excitatory neuronal populations, pyramidal island and stellate ocean cells in addition to the inhibitory interneurons. Ocean cells express reelin and surround clusters of island cells that lack reelin expression. The influence of reelin expression by ocean cells and interneurons on their own morphological differentiation and that of MECII island cells remained unknown. To address this question, we used a conditional reelin knockout (RelncKO) mouse to induce reelin deficiency postnatally in vitro and in vivo. Reelin deficiency caused dendritic hypertrophy of ocean cells, interneurons, and only proximal dendritic compartments of island cells. Ca2+-recording showed that both cell types exhibited an elevation of calcium frequencies in RelncKO, indicating that the hypertrophic effect is related to excessive Ca2+-signaling. Moreover, pharmacological receptor blockade in RelncKO mouse revealed malfunctioning of GABABRs, NMDARs and AMPARs. Collectively, this study emphasizes the significance of reelin in neuronal growth and its absence results in dendrite hypertrophy of MECII neurons.
