p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli

Constitutive p16(Ink4a) expression, along with senescence-associated β-galactosidase (SAβG), are commonly accepted biomarkers of senescent cells (SCs). Recent reports attributed improvement of the healthspan of aged mice following p16(Ink4a)-positive cell killing to the eradication of accumulated SC...

Descripción completa

Detalles Bibliográficos
Autores principales: Hall, Brandon M., Balan, Vitaly, Gleiberman, Anatoli S., Strom, Evguenia, Krasnov, Peter, Virtuoso, Lauren P., Rydkina, Elena, Vujcic, Slavoljub, Balan, Karina, Gitlin, Ilya I., Leonova, Katerina I., Consiglio, Camila R., Gollnick, Sandra O., Chernova, Olga B., Gudkov, Andrei V.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2017
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5611982/
https://www.ncbi.nlm.nih.gov/pubmed/28768895
http://dx.doi.org/10.18632/aging.101268
_version_ 1783266040103305216
author Hall, Brandon M.
Balan, Vitaly
Gleiberman, Anatoli S.
Strom, Evguenia
Krasnov, Peter
Virtuoso, Lauren P.
Rydkina, Elena
Vujcic, Slavoljub
Balan, Karina
Gitlin, Ilya I.
Leonova, Katerina I.
Consiglio, Camila R.
Gollnick, Sandra O.
Chernova, Olga B.
Gudkov, Andrei V.
author_facet Hall, Brandon M.
Balan, Vitaly
Gleiberman, Anatoli S.
Strom, Evguenia
Krasnov, Peter
Virtuoso, Lauren P.
Rydkina, Elena
Vujcic, Slavoljub
Balan, Karina
Gitlin, Ilya I.
Leonova, Katerina I.
Consiglio, Camila R.
Gollnick, Sandra O.
Chernova, Olga B.
Gudkov, Andrei V.
author_sort Hall, Brandon M.
collection PubMed
description Constitutive p16(Ink4a) expression, along with senescence-associated β-galactosidase (SAβG), are commonly accepted biomarkers of senescent cells (SCs). Recent reports attributed improvement of the healthspan of aged mice following p16(Ink4a)-positive cell killing to the eradication of accumulated SCs. However, detection of p16(Ink4a)/SAβG-positive macrophages in the adipose tissue of old mice and in the peritoneal cavity of young animals following injection of alginate-encapsulated SCs has raised concerns about the exclusivity of these markers for SCs. Here we report that expression of p16(Ink4a) and SAβG in macrophages is acquired as part of a physiological response to immune stimuli rather than through senescence, consistent with reports that p16(Ink4a) plays a role in macrophage polarization and response. Unlike SCs, p16(Ink4a)/SAβG-positive macrophages can be induced in p53-null mice. Macrophages, but not mesenchymal SCs, lose both markers in response to M1- [LPS, IFN-α, Poly(I:C)] and increase their expression in response to M2-inducing stimuli (IL-4, IL-13). Moreover, interferon-inducing agent Poly(I:C) dramatically reduced p16(Ink4a) expression in vivo in our alginate bead model and in the adipose tissue of aged mice. These observations suggest that the antiaging effects following eradication of p16(Ink4a)-positive cells may not be solely attributed to SCs but also to non-senescent p16(Ink4a)/SAβG-positive macrophages.
format Online
Article
Text
id pubmed-5611982
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Impact Journals LLC
record_format MEDLINE/PubMed
spelling pubmed-56119822017-09-28 p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli Hall, Brandon M. Balan, Vitaly Gleiberman, Anatoli S. Strom, Evguenia Krasnov, Peter Virtuoso, Lauren P. Rydkina, Elena Vujcic, Slavoljub Balan, Karina Gitlin, Ilya I. Leonova, Katerina I. Consiglio, Camila R. Gollnick, Sandra O. Chernova, Olga B. Gudkov, Andrei V. Aging (Albany NY) Research Paper Constitutive p16(Ink4a) expression, along with senescence-associated β-galactosidase (SAβG), are commonly accepted biomarkers of senescent cells (SCs). Recent reports attributed improvement of the healthspan of aged mice following p16(Ink4a)-positive cell killing to the eradication of accumulated SCs. However, detection of p16(Ink4a)/SAβG-positive macrophages in the adipose tissue of old mice and in the peritoneal cavity of young animals following injection of alginate-encapsulated SCs has raised concerns about the exclusivity of these markers for SCs. Here we report that expression of p16(Ink4a) and SAβG in macrophages is acquired as part of a physiological response to immune stimuli rather than through senescence, consistent with reports that p16(Ink4a) plays a role in macrophage polarization and response. Unlike SCs, p16(Ink4a)/SAβG-positive macrophages can be induced in p53-null mice. Macrophages, but not mesenchymal SCs, lose both markers in response to M1- [LPS, IFN-α, Poly(I:C)] and increase their expression in response to M2-inducing stimuli (IL-4, IL-13). Moreover, interferon-inducing agent Poly(I:C) dramatically reduced p16(Ink4a) expression in vivo in our alginate bead model and in the adipose tissue of aged mice. These observations suggest that the antiaging effects following eradication of p16(Ink4a)-positive cells may not be solely attributed to SCs but also to non-senescent p16(Ink4a)/SAβG-positive macrophages. Impact Journals LLC 2017-08-02 /pmc/articles/PMC5611982/ /pubmed/28768895 http://dx.doi.org/10.18632/aging.101268 Text en Copyright: © 2017 Hall et al. http://creativecommons.org/licenses/by/3.0/ This article is distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0/) (CC-BY), which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Research Paper
Hall, Brandon M.
Balan, Vitaly
Gleiberman, Anatoli S.
Strom, Evguenia
Krasnov, Peter
Virtuoso, Lauren P.
Rydkina, Elena
Vujcic, Slavoljub
Balan, Karina
Gitlin, Ilya I.
Leonova, Katerina I.
Consiglio, Camila R.
Gollnick, Sandra O.
Chernova, Olga B.
Gudkov, Andrei V.
p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli
title p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli
title_full p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli
title_fullStr p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli
title_full_unstemmed p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli
title_short p16(Ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli
title_sort p16(ink4a) and senescence-associated β-galactosidase can be induced in macrophages as part of a reversible response to physiological stimuli
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5611982/
https://www.ncbi.nlm.nih.gov/pubmed/28768895
http://dx.doi.org/10.18632/aging.101268
work_keys_str_mv AT hallbrandonm p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT balanvitaly p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT gleibermananatolis p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT stromevguenia p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT krasnovpeter p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT virtuosolaurenp p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT rydkinaelena p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT vujcicslavoljub p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT balankarina p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT gitlinilyai p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT leonovakaterinai p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT consigliocamilar p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT gollnicksandrao p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT chernovaolgab p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli
AT gudkovandreiv p16ink4aandsenescenceassociatedbgalactosidasecanbeinducedinmacrophagesaspartofareversibleresponsetophysiologicalstimuli

Ejemplares similares