Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits

We describe age-related molecular and neuronal changes that disrupt mobility or energy balance based on brain region and genetic background. Compared to young mice, aged C57BL/6 mice exhibit marked locomotor (but not energy balance) impairments. In contrast, aged BALB mice exhibit marked energy bala...

Descripción completa

Detalles Bibliográficos
Autores principales: Bonasera, Stephen J., Arikkath, Jyothi, Boska, Michael D., Chaudoin, Tammy R., DeKorver, Nicholas W., Goulding, Evan H., Hoke, Traci A., Mojtahedzedah, Vahid, Reyelts, Crystal D., Sajja, Balasrinivasa, Schenk, A. Katrin, Tecott, Laurence H., Volden, Tiffany A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5076456/
https://www.ncbi.nlm.nih.gov/pubmed/27689748
http://dx.doi.org/10.18632/aging.101040
_version_ 1782462032073719808
author Bonasera, Stephen J.
Arikkath, Jyothi
Boska, Michael D.
Chaudoin, Tammy R.
DeKorver, Nicholas W.
Goulding, Evan H.
Hoke, Traci A.
Mojtahedzedah, Vahid
Reyelts, Crystal D.
Sajja, Balasrinivasa
Schenk, A. Katrin
Tecott, Laurence H.
Volden, Tiffany A.
author_facet Bonasera, Stephen J.
Arikkath, Jyothi
Boska, Michael D.
Chaudoin, Tammy R.
DeKorver, Nicholas W.
Goulding, Evan H.
Hoke, Traci A.
Mojtahedzedah, Vahid
Reyelts, Crystal D.
Sajja, Balasrinivasa
Schenk, A. Katrin
Tecott, Laurence H.
Volden, Tiffany A.
author_sort Bonasera, Stephen J.
collection PubMed
description We describe age-related molecular and neuronal changes that disrupt mobility or energy balance based on brain region and genetic background. Compared to young mice, aged C57BL/6 mice exhibit marked locomotor (but not energy balance) impairments. In contrast, aged BALB mice exhibit marked energy balance (but not locomotor) impairments. Age-related changes in cerebellar or hypothalamic gene expression accompany these phenotypes. Aging evokes upregulation of immune pattern recognition receptors and cell adhesion molecules. However, these changes do not localize to microglia, the major CNS immunocyte. Consistent with a neuronal role, there is a marked age-related increase in excitatory synapses over the cerebellum and hypothalamus. Functional imaging of these regions is consistent with age-related synaptic impairments. These studies suggest that aging reactivates a developmental program employed during embryogenesis where immune molecules guide synapse formation and pruning. Renewed activity in this program may disrupt excitatory neurotransmission, causing significant behavioral deficits.
format Online
Article
Text
id pubmed-5076456
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher Impact Journals LLC
record_format MEDLINE/PubMed
spelling pubmed-50764562016-10-27 Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits Bonasera, Stephen J. Arikkath, Jyothi Boska, Michael D. Chaudoin, Tammy R. DeKorver, Nicholas W. Goulding, Evan H. Hoke, Traci A. Mojtahedzedah, Vahid Reyelts, Crystal D. Sajja, Balasrinivasa Schenk, A. Katrin Tecott, Laurence H. Volden, Tiffany A. Aging (Albany NY) Research Paper We describe age-related molecular and neuronal changes that disrupt mobility or energy balance based on brain region and genetic background. Compared to young mice, aged C57BL/6 mice exhibit marked locomotor (but not energy balance) impairments. In contrast, aged BALB mice exhibit marked energy balance (but not locomotor) impairments. Age-related changes in cerebellar or hypothalamic gene expression accompany these phenotypes. Aging evokes upregulation of immune pattern recognition receptors and cell adhesion molecules. However, these changes do not localize to microglia, the major CNS immunocyte. Consistent with a neuronal role, there is a marked age-related increase in excitatory synapses over the cerebellum and hypothalamus. Functional imaging of these regions is consistent with age-related synaptic impairments. These studies suggest that aging reactivates a developmental program employed during embryogenesis where immune molecules guide synapse formation and pruning. Renewed activity in this program may disrupt excitatory neurotransmission, causing significant behavioral deficits. Impact Journals LLC 2016-09-20 /pmc/articles/PMC5076456/ /pubmed/27689748 http://dx.doi.org/10.18632/aging.101040 Text en Copyright: © 2016 Bonasera et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Bonasera, Stephen J.
Arikkath, Jyothi
Boska, Michael D.
Chaudoin, Tammy R.
DeKorver, Nicholas W.
Goulding, Evan H.
Hoke, Traci A.
Mojtahedzedah, Vahid
Reyelts, Crystal D.
Sajja, Balasrinivasa
Schenk, A. Katrin
Tecott, Laurence H.
Volden, Tiffany A.
Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits
title Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits
title_full Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits
title_fullStr Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits
title_full_unstemmed Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits
title_short Age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits
title_sort age-related changes in cerebellar and hypothalamic function accompany non-microglial immune gene expression, altered synapse organization, and excitatory amino acid neurotransmission deficits
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5076456/
https://www.ncbi.nlm.nih.gov/pubmed/27689748
http://dx.doi.org/10.18632/aging.101040
work_keys_str_mv AT bonaserastephenj agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT arikkathjyothi agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT boskamichaeld agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT chaudointammyr agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT dekorvernicholasw agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT gouldingevanh agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT hoketracia agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT mojtahedzedahvahid agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT reyeltscrystald agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT sajjabalasrinivasa agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT schenkakatrin agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT tecottlaurenceh agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits
AT voldentiffanya agerelatedchangesincerebellarandhypothalamicfunctionaccompanynonmicroglialimmunegeneexpressionalteredsynapseorganizationandexcitatoryaminoacidneurotransmissiondeficits

Ejemplares similares