Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice

Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice

Stroke remains a leading cause of disability worldwide. Recently, we have established an animal model of stroke that results in delayed impairment in spatial memory, allowing us to better investigate cognitive deficits. Young and aged brains show different recovery profiles after stroke; therefore,...

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Main Authors: Josh Houlton, Lisa Y. Y. Zhou, Deanna Barwick, Emma K. Gowing, Andrew N. Clarkson
Format: Article
Language:English
Published: Hindawi Limited 2019-01-01
Series:Neural Plasticity
Online Access:http://dx.doi.org/10.1155/2019/1460890
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spelling doaj-dac2e9ee5327498790b343f51b6a645b2020-11-25T02:33:51ZengHindawi LimitedNeural Plasticity2090-59041687-54432019-01-01201910.1155/2019/14608901460890Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged MiceJosh Houlton0Lisa Y. Y. Zhou1Deanna Barwick2Emma K. Gowing3Andrew N. Clarkson4Department of Anatomy, Brain Health Research Centre and Brain Research New Zealand, University of Otago, Dunedin 9054, New ZealandDepartment of Anatomy, Brain Health Research Centre and Brain Research New Zealand, University of Otago, Dunedin 9054, New ZealandDepartment of Anatomy, Brain Health Research Centre and Brain Research New Zealand, University of Otago, Dunedin 9054, New ZealandDepartment of Anatomy, Brain Health Research Centre and Brain Research New Zealand, University of Otago, Dunedin 9054, New ZealandDepartment of Anatomy, Brain Health Research Centre and Brain Research New Zealand, University of Otago, Dunedin 9054, New ZealandStroke remains a leading cause of disability worldwide. Recently, we have established an animal model of stroke that results in delayed impairment in spatial memory, allowing us to better investigate cognitive deficits. Young and aged brains show different recovery profiles after stroke; therefore, we assessed aged-related differences in poststroke cognition. As neurotrophic support diminishes with age, we also investigated the involvement of brain-derived neurotrophic factor (BDNF) in these differences. Young (3-6 months old) and aged (16-21 months old) mice were trained in operant touchscreen chambers to complete a visual pairwise discrimination (VD) task. Stroke or sham surgery was induced using the photothrombotic model to induce a bilateral prefrontal cortex stroke. Five days poststroke, an additional cohort of aged stroke animals were treated with intracerebral hydrogels loaded with the BDNF decoy, TrkB-Fc. Following treatment, animals underwent the reversal and rereversal task to identify stroke-induced cognitive deficits at days 17 and 37 poststroke, respectively. Assessment of sham animals using Cox regression and log-rank analyses showed aged mice exhibit an increased impairment on VD reversal and rereversal learning compared to young controls. Stroke to young mice revealed no impairment on either task. In contrast, stroke to aged mice facilitated a significant improvement in reversal learning, which was dampened in the presence of the BDNF decoy, TrkB-Fc. In addition, aged stroke control animals required significantly less consecutive days and correction trials to master the reversal task, relative to aged shams, an effect dampened by TrkB-Fc. Our findings support age-related differences in recovery of cognitive function after stroke. Interestingly, aged stroke animals outperformed their sham counterparts, suggesting reopening of a critical window for recovery that is being mediated by BDNF.http://dx.doi.org/10.1155/2019/1460890
collection DOAJ
language English
format Article
sources DOAJ
author Josh Houlton
Lisa Y. Y. Zhou
Deanna Barwick
Emma K. Gowing
Andrew N. Clarkson
spellingShingle Josh Houlton
Lisa Y. Y. Zhou
Deanna Barwick
Emma K. Gowing
Andrew N. Clarkson
Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice
Neural Plasticity
author_facet Josh Houlton
Lisa Y. Y. Zhou
Deanna Barwick
Emma K. Gowing
Andrew N. Clarkson
author_sort Josh Houlton
title Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice
title_short Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice
title_full Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice
title_fullStr Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice
title_full_unstemmed Stroke Induces a BDNF-Dependent Improvement in Cognitive Flexibility in Aged Mice
title_sort stroke induces a bdnf-dependent improvement in cognitive flexibility in aged mice
publisher Hindawi Limited
series Neural Plasticity
issn 2090-5904
1687-5443
publishDate 2019-01-01
description Stroke remains a leading cause of disability worldwide. Recently, we have established an animal model of stroke that results in delayed impairment in spatial memory, allowing us to better investigate cognitive deficits. Young and aged brains show different recovery profiles after stroke; therefore, we assessed aged-related differences in poststroke cognition. As neurotrophic support diminishes with age, we also investigated the involvement of brain-derived neurotrophic factor (BDNF) in these differences. Young (3-6 months old) and aged (16-21 months old) mice were trained in operant touchscreen chambers to complete a visual pairwise discrimination (VD) task. Stroke or sham surgery was induced using the photothrombotic model to induce a bilateral prefrontal cortex stroke. Five days poststroke, an additional cohort of aged stroke animals were treated with intracerebral hydrogels loaded with the BDNF decoy, TrkB-Fc. Following treatment, animals underwent the reversal and rereversal task to identify stroke-induced cognitive deficits at days 17 and 37 poststroke, respectively. Assessment of sham animals using Cox regression and log-rank analyses showed aged mice exhibit an increased impairment on VD reversal and rereversal learning compared to young controls. Stroke to young mice revealed no impairment on either task. In contrast, stroke to aged mice facilitated a significant improvement in reversal learning, which was dampened in the presence of the BDNF decoy, TrkB-Fc. In addition, aged stroke control animals required significantly less consecutive days and correction trials to master the reversal task, relative to aged shams, an effect dampened by TrkB-Fc. Our findings support age-related differences in recovery of cognitive function after stroke. Interestingly, aged stroke animals outperformed their sham counterparts, suggesting reopening of a critical window for recovery that is being mediated by BDNF.
url http://dx.doi.org/10.1155/2019/1460890
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AT deannabarwick strokeinducesabdnfdependentimprovementincognitiveflexibilityinagedmice
AT emmakgowing strokeinducesabdnfdependentimprovementincognitiveflexibilityinagedmice
AT andrewnclarkson strokeinducesabdnfdependentimprovementincognitiveflexibilityinagedmice
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