| Literature DB >> 31884883 |
Karen Krukowski1,2, Amber Nolan1,2,3, Elma S Frias1,2,4, Katherine Grue1,2, McKenna Becker1,2, Gonzalo Ureta5, Luz Delgado5, Sebastian Bernales5, Vikaas S Sohal6, Peter Walter7,8, Susanna Rosi1,2,9,10,11.
Abstract
Mild repetitive traumatic brain injury (rTBI) induces chronic behavioral and cognitive alterations and increases the risk for dementia. Currently, there are no therapeutic strategies to prevent or mitigate chronic deficits associated with rTBI. Previously we developed an animal model of rTBI that recapitulates the cognitive and behavioral deficits observed in humans. We now report that rTBI results in an increase in risk-taking behavior in male but not female mice. This behavioral phenotype is associated with chronic activation of the integrated stress response and cell-specific synaptic alterations in the type A subtype of layer V pyramidal neurons in the medial prefrontal cortex. Strikingly, by briefly treating animals weeks after injury with ISRIB, a selective inhibitor of the integrated stress response (ISR), we (1) relieve ISR activation, (2) reverse the increased risk-taking behavioral phenotype and maintain this reversal, and (3) restore cell-specific synaptic function in the affected mice. Our results indicate that targeting the ISR even at late time points after injury can permanently reverse behavioral changes. As such, pharmacological inhibition of the ISR emerges as a promising avenue to combat rTBI-induced behavioral dysfunction.Entities:
Keywords: integrated stress response; prefrontal cortex; repetitive mild traumatic brain injury; risk-taking behavior; synaptic function
Year: 2020 PMID: 31884883 PMCID: PMC7249463 DOI: 10.1089/neu.2019.6827
Source DB: PubMed Journal: J Neurotrauma ISSN: 0897-7151 Impact factor: 5.269