Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults

Compensation implies the recruitment of additional neuronal resources to prevent the detrimental effect of age-related neuronal decline on cognition. Recently suggested statistical models comprise behavioral performance, brain activation, and measures related to aging- or disease-specific pathologic...

Descripción completa

Detalles Bibliográficos
Autores principales: Scheller, Elisa, Schumacher, Lena V., Peter, Jessica, Lahr, Jacob, Wehrle, Julius, Kaller, Christoph P., Gaser, Christian, Klöppel, Stefan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Neuroscience
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5869204/
https://www.ncbi.nlm.nih.gov/pubmed/29615896
http://dx.doi.org/10.3389/fnagi.2018.00074
_version_ 1783309239290167296
author Scheller, Elisa
Schumacher, Lena V.
Peter, Jessica
Lahr, Jacob
Wehrle, Julius
Kaller, Christoph P.
Gaser, Christian
Klöppel, Stefan
author_facet Scheller, Elisa
Schumacher, Lena V.
Peter, Jessica
Lahr, Jacob
Wehrle, Julius
Kaller, Christoph P.
Gaser, Christian
Klöppel, Stefan
author_sort Scheller, Elisa
collection PubMed
description Compensation implies the recruitment of additional neuronal resources to prevent the detrimental effect of age-related neuronal decline on cognition. Recently suggested statistical models comprise behavioral performance, brain activation, and measures related to aging- or disease-specific pathological burden to characterize compensation. Higher chronological age as well as the APOE ε4 allele are risk factors for Alzheimer's disease. A more biological approach to characterize aging compared with chronological age is the brain age gap estimation (BrainAGE), taking into account structural brain characteristics. We utilized this estimate in an fMRI experiment together with APOE variant as measures related to pathological burden and aimed at identifying compensatory regions during working memory (WM) processing in a group of 34 healthy older adults. According to published compensation criteria, better performance along with increased brain activation would indicate successful compensation. We examined the moderating effects of BrainAGE on the relationship between task performance and brain activation in prefrontal cortex, as previous studies suggest predominantly frontal compensatory activation. Then we statistically compared them to the effects of chronological age (CA) tested in a previous study. Moreover, we examined the effects of adding APOE variant as a further moderator. Herewith, we strived to uncover neuronal compensation in healthy older adults at risk for neurodegenerative disease. Higher BrainAGE alone was not associated with an increased recruitment in prefrontal cortex. When adding APOE variant as a second moderator, we found an interaction of BrainAGE and APOE variant, such that ε4 carriers recruited right inferior frontal gyrus with higher BrainAGE to maintain WM performance, thus showing a pattern compatible with successful neuronal compensation. Exploratory analyses yielded similar patterns in left inferior and bilateral middle frontal gyrus. These results contrast those from a previous study, where we found no indication of compensation in prefrontal cortex in ε4 carriers with increasing CA. We conclude that BrainAGE together with APOE variant can help to reveal potential neuronal compensation in healthy older adults. Previous results on neuronal compensation in frontal areas corroborate our findings. Compensatory brain regions could be targeted in affected individuals by training or stimulation protocols to maintain cognitive functioning as long as possible.
format Online
Article
Text
id pubmed-5869204
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-58692042018-04-03 Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults Scheller, Elisa Schumacher, Lena V. Peter, Jessica Lahr, Jacob Wehrle, Julius Kaller, Christoph P. Gaser, Christian Klöppel, Stefan Front Aging Neurosci Neuroscience Compensation implies the recruitment of additional neuronal resources to prevent the detrimental effect of age-related neuronal decline on cognition. Recently suggested statistical models comprise behavioral performance, brain activation, and measures related to aging- or disease-specific pathological burden to characterize compensation. Higher chronological age as well as the APOE ε4 allele are risk factors for Alzheimer's disease. A more biological approach to characterize aging compared with chronological age is the brain age gap estimation (BrainAGE), taking into account structural brain characteristics. We utilized this estimate in an fMRI experiment together with APOE variant as measures related to pathological burden and aimed at identifying compensatory regions during working memory (WM) processing in a group of 34 healthy older adults. According to published compensation criteria, better performance along with increased brain activation would indicate successful compensation. We examined the moderating effects of BrainAGE on the relationship between task performance and brain activation in prefrontal cortex, as previous studies suggest predominantly frontal compensatory activation. Then we statistically compared them to the effects of chronological age (CA) tested in a previous study. Moreover, we examined the effects of adding APOE variant as a further moderator. Herewith, we strived to uncover neuronal compensation in healthy older adults at risk for neurodegenerative disease. Higher BrainAGE alone was not associated with an increased recruitment in prefrontal cortex. When adding APOE variant as a second moderator, we found an interaction of BrainAGE and APOE variant, such that ε4 carriers recruited right inferior frontal gyrus with higher BrainAGE to maintain WM performance, thus showing a pattern compatible with successful neuronal compensation. Exploratory analyses yielded similar patterns in left inferior and bilateral middle frontal gyrus. These results contrast those from a previous study, where we found no indication of compensation in prefrontal cortex in ε4 carriers with increasing CA. We conclude that BrainAGE together with APOE variant can help to reveal potential neuronal compensation in healthy older adults. Previous results on neuronal compensation in frontal areas corroborate our findings. Compensatory brain regions could be targeted in affected individuals by training or stimulation protocols to maintain cognitive functioning as long as possible. Frontiers Media S.A. 2018-03-20 /pmc/articles/PMC5869204/ /pubmed/29615896 http://dx.doi.org/10.3389/fnagi.2018.00074 Text en Copyright © 2018 Scheller, Schumacher, Peter, Lahr, Wehrle, Kaller, Gaser and Klöppel. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Neuroscience
Scheller, Elisa
Schumacher, Lena V.
Peter, Jessica
Lahr, Jacob
Wehrle, Julius
Kaller, Christoph P.
Gaser, Christian
Klöppel, Stefan
Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults
title Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults
title_full Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults
title_fullStr Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults
title_full_unstemmed Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults
title_short Brain Aging and APOE ε4 Interact to Reveal Potential Neuronal Compensation in Healthy Older Adults
title_sort brain aging and apoe ε4 interact to reveal potential neuronal compensation in healthy older adults
topic Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5869204/
https://www.ncbi.nlm.nih.gov/pubmed/29615896
http://dx.doi.org/10.3389/fnagi.2018.00074
work_keys_str_mv AT schellerelisa brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults
AT schumacherlenav brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults
AT peterjessica brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults
AT lahrjacob brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults
AT wehrlejulius brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults
AT kallerchristophp brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults
AT gaserchristian brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults
AT kloppelstefan brainagingandapoee4interacttorevealpotentialneuronalcompensationinhealthyolderadults

Ejemplares similares