| Literature DB >> 27613436 |
Marie Hébert1, Antoine Anfray1, Arnaud Chevilley1, Sara Martinez de Lizarrondo1, Aurélien Quenault1, Morgane Louessard1, Benoit D Roussel1, Pauline Obiang1, Etienne Save2, Cyrille Orset1, Eric Maubert1, Denis Vivien1,3, Véronique Agin1.
Abstract
In humans, spatial cognition and navigation impairments are a frequent situation during physiological and pathological aging, leading to a dramatic deterioration in the quality of life. Despite the discovery of neurons with location-specific activity in rodents, that is, place cells in the hippocampus and later on grid cells in the entorhinal cortex (EC), the molecular mechanisms underlying spatial cognition are still poorly known. Our present data bring together in an unusual combination 2 molecules of primary biological importance: a major neuronal excitatory receptor, N-methyl-D-aspartate receptor (NMDAR), and an extracellular protease, tissue plasminogen activator (tPA), in the control of spatial navigation. By using tPA-deficient mice and a structure-selective pharmacological approach, we demonstrate that the tPA-dependent NMDAR signaling potentiation in the EC plays a key and selective role in the encoding and the subsequent use of distant landmarks during spatial learning. We also demonstrate that this novel function of tPA in the EC is reduced during aging. Overall, these results argue for the concept that encoding of proximal versus distal landmarks is mediated not only by different anatomical pathways but also by different molecular mechanisms, with the tPA-dependent potentiation of NMDAR signaling in the EC that plays an important role.Entities:
Keywords: N-methyl-D-aspartate receptor; aging; entorhinal cortex; spatial cognition; tissue plasminogen activator
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Year: 2017 PMID: 27613436 DOI: 10.1093/cercor/bhw275
Source DB: PubMed Journal: Cereb Cortex ISSN: 1047-3211 Impact factor: 5.357