Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging

Aging is characterized by a gradual functional decline of tissues with age. Adult stem and progenitor cells are responsible for tissue maintenance, repair, and regeneration, but during aging, this population of cells is decreased or its activity is reduced, compromising tissue integrity and causing...

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Autores principales: Vilas, Jéssica M., Carneiro, Carmen, Da Silva‐Álvarez, Sabela, Ferreirós, Alba, González, Patricia, Gómez, María, Ortega, Sagrario, Serrano, Manuel, García‐Caballero, Tomás, González‐Barcia, Miguel, Vidal, Anxo, Collado, Manuel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2018
Materias:
Short Take
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6156495/
https://www.ncbi.nlm.nih.gov/pubmed/30129215
http://dx.doi.org/10.1111/acel.12834
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author Vilas, Jéssica M.
Carneiro, Carmen
Da Silva‐Álvarez, Sabela
Ferreirós, Alba
González, Patricia
Gómez, María
Ortega, Sagrario
Serrano, Manuel
García‐Caballero, Tomás
González‐Barcia, Miguel
Vidal, Anxo
Collado, Manuel
author_facet Vilas, Jéssica M.
Carneiro, Carmen
Da Silva‐Álvarez, Sabela
Ferreirós, Alba
González, Patricia
Gómez, María
Ortega, Sagrario
Serrano, Manuel
García‐Caballero, Tomás
González‐Barcia, Miguel
Vidal, Anxo
Collado, Manuel
author_sort Vilas, Jéssica M.
collection PubMed
description Aging is characterized by a gradual functional decline of tissues with age. Adult stem and progenitor cells are responsible for tissue maintenance, repair, and regeneration, but during aging, this population of cells is decreased or its activity is reduced, compromising tissue integrity and causing pathologies that increase vulnerability, and ultimately lead to death. The causes of stem cell exhaustion during aging are not clear, and whether a reduction in stem cell function is a cause or a consequence of aging remains unresolved. Here, we took advantage of a mouse model of induced adult Sox2+ stem cell depletion to address whether accelerated stem cell depletion can promote premature aging. After a short period of partial repetitive depletion of this adult stem cell population in mice, we observed increased kyphosis and hair graying, and reduced fat mass, all of them signs of premature aging. It is interesting that cellular senescence was identified in kidney after this partial repetitive Sox2+ cell depletion. To confirm these observations, we performed a prolonged protocol of partial repetitive depletion of Sox2+ cells, forcing regeneration from the remaining Sox2+ cells, thereby causing their exhaustion. Senescence specific staining and the analysis of the expression of genetic markers clearly corroborated that adult stem cell exhaustion can lead to cellular senescence induction and premature aging.
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spelling pubmed-61564952018-10-01 Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging Vilas, Jéssica M. Carneiro, Carmen Da Silva‐Álvarez, Sabela Ferreirós, Alba González, Patricia Gómez, María Ortega, Sagrario Serrano, Manuel García‐Caballero, Tomás González‐Barcia, Miguel Vidal, Anxo Collado, Manuel Aging Cell Short Take Aging is characterized by a gradual functional decline of tissues with age. Adult stem and progenitor cells are responsible for tissue maintenance, repair, and regeneration, but during aging, this population of cells is decreased or its activity is reduced, compromising tissue integrity and causing pathologies that increase vulnerability, and ultimately lead to death. The causes of stem cell exhaustion during aging are not clear, and whether a reduction in stem cell function is a cause or a consequence of aging remains unresolved. Here, we took advantage of a mouse model of induced adult Sox2+ stem cell depletion to address whether accelerated stem cell depletion can promote premature aging. After a short period of partial repetitive depletion of this adult stem cell population in mice, we observed increased kyphosis and hair graying, and reduced fat mass, all of them signs of premature aging. It is interesting that cellular senescence was identified in kidney after this partial repetitive Sox2+ cell depletion. To confirm these observations, we performed a prolonged protocol of partial repetitive depletion of Sox2+ cells, forcing regeneration from the remaining Sox2+ cells, thereby causing their exhaustion. Senescence specific staining and the analysis of the expression of genetic markers clearly corroborated that adult stem cell exhaustion can lead to cellular senescence induction and premature aging. John Wiley and Sons Inc. 2018-08-20 2018-10 /pmc/articles/PMC6156495/ /pubmed/30129215 http://dx.doi.org/10.1111/acel.12834 Text en © 2018 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Short Take
Vilas, Jéssica M.
Carneiro, Carmen
Da Silva‐Álvarez, Sabela
Ferreirós, Alba
González, Patricia
Gómez, María
Ortega, Sagrario
Serrano, Manuel
García‐Caballero, Tomás
González‐Barcia, Miguel
Vidal, Anxo
Collado, Manuel
Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging
title Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging
title_full Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging
title_fullStr Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging
title_full_unstemmed Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging
title_short Adult Sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging
title_sort adult sox2+ stem cell exhaustion in mice results in cellular senescence and premature aging
topic Short Take
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6156495/
https://www.ncbi.nlm.nih.gov/pubmed/30129215
http://dx.doi.org/10.1111/acel.12834
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