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The Impact of the PI3K/Akt Signaling Pathway in Anxiety and Working Memory in Young and Middle-Aged PDK1 K465E Knock-In Mice

Lydia Giménez‐Llort, Mikel Santana-Santana, José R. Bayascas

2020Frontiers in Behavioral Neuroscience23 citationsDOIOpen Access PDF

Abstract

Dysfunction and dysregulation at genetic, neural and behavioral level points at fine-tuning of broadly spread networks as critical for a wide array of behaviors and mental processes though life span. This brain-based evidence, from basic to behavioral neuroscience levels, is leading to a new conceptualization of mental health and disease. Thus, the Research Domain Criteria considers phenotypic differences observed among disorders as explained by variations in the nature and degree of neural circuitry disruptions, under the modulation of several developmental, compensatory, environmental and epigenetic factors. In this context, we aimed to describe for the first time the in vivo behavioral impact of tweaking the PI3K/Akt signaling pathway known to play an essential role in the regulation of cellular processes, leading to diverse physiological responses. We explored the effects in young (YA, 3-4 months of age) and mature (MA, 11-14 months of age) male and female PDK1 K465E knock-in mice in a battery of tests under different anxiogenic conditions. The results evidenced that the double mutation of the PDK1 PH-domain resulted in an enhancement of negative valence system shown as an increase of responses of fear and anxiety-like behaviors in anxiogenic situations. Interestingly, this seemed to be specific of YA, and found regulated at middle-age. In contrast, cognitive deficits, as measured in a spatial working memory task, were found in both YA and MA mutants, and independently of the level of their anxious-like profiles. These distinct age- and function-dependent impacts would be in agreement with the distinct cortical and limbic deficits in the Akt signaling in the brain we have recently described in these same animals. The elicitation of age- and neuronal-dependent specific patterns suggests that fine-tuning the intensity of the PKB/Akt signal that enables diverse physiological response has also its in vivo translation into the negative valence system and age is a key regulatory factor.

Topics & Concepts

AnxiogenicNeuroscienceAnxietyPI3K/AKT/mTOR pathwayPsychologyContext (archaeology)Pleckstrin homology domainWorking memoryProtein kinase BArousalCognitionBiologySignal transductionGeneticsPsychiatryAnxiolyticPaleontologyGenetics and Neurodevelopmental DisordersReceptor Mechanisms and SignalingNeuroscience and Neuropharmacology Research