Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell

Aging, a time-dependent functional decline of biological processes, is the primary risk factor in developing diseases such as cancer, cardiovascular or degenerative diseases. There is a real need to understand the human aging process in order to increase the length of disease-free life, also known a...

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Autores principales: Infante, Arantza, Gago, Andrea, de Eguino, Garbiñe Ruiz, Calvo-Fernández, Teresa, Gómez-Vallejo, Vanessa, Llop, Jordi, Schlangen, Karin, Fullaondo, Ane, Aransay, Ana M., Martín, Abraham, Rodríguez, Clara I.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4032794/
https://www.ncbi.nlm.nih.gov/pubmed/24753226
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author Infante, Arantza
Gago, Andrea
de Eguino, Garbiñe Ruiz
Calvo-Fernández, Teresa
Gómez-Vallejo, Vanessa
Llop, Jordi
Schlangen, Karin
Fullaondo, Ane
Aransay, Ana M.
Martín, Abraham
Rodríguez, Clara I.
author_facet Infante, Arantza
Gago, Andrea
de Eguino, Garbiñe Ruiz
Calvo-Fernández, Teresa
Gómez-Vallejo, Vanessa
Llop, Jordi
Schlangen, Karin
Fullaondo, Ane
Aransay, Ana M.
Martín, Abraham
Rodríguez, Clara I.
author_sort Infante, Arantza
collection PubMed
description Aging, a time-dependent functional decline of biological processes, is the primary risk factor in developing diseases such as cancer, cardiovascular or degenerative diseases. There is a real need to understand the human aging process in order to increase the length of disease-free life, also known as “health span”. Accumulation of progerin and prelamin A are the hallmark of a group of premature aging diseases but have also been found during normal cellular aging strongly suggesting similar mechanisms between healthy aging and LMNA-linked progeroid syndromes. How this toxic accumulation contributes to aging (physiological or pathological) remains unclear. Since affected tissues in age-associated disorders and in pathological aging are mainly of mesenchymal origin we propose a model of human aging based on mesenchymal stem cells (hMSCs) which accumulate prelamin A. We demonstrate that prelamin A-accumulating hMSCs have a premature aging phenotype which affects their functional competence in vivo. The combination of prelamin A accumulation and stress conditions enhance the aging phenotype by dysregulating the activity of the octamer binding protein Oct-1This experimental model has been fundamental to identify a new role for Oct-1 in hMSCs aging.
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spelling pubmed-40327942014-06-02 Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell Infante, Arantza Gago, Andrea de Eguino, Garbiñe Ruiz Calvo-Fernández, Teresa Gómez-Vallejo, Vanessa Llop, Jordi Schlangen, Karin Fullaondo, Ane Aransay, Ana M. Martín, Abraham Rodríguez, Clara I. Aging (Albany NY) Research Paper Aging, a time-dependent functional decline of biological processes, is the primary risk factor in developing diseases such as cancer, cardiovascular or degenerative diseases. There is a real need to understand the human aging process in order to increase the length of disease-free life, also known as “health span”. Accumulation of progerin and prelamin A are the hallmark of a group of premature aging diseases but have also been found during normal cellular aging strongly suggesting similar mechanisms between healthy aging and LMNA-linked progeroid syndromes. How this toxic accumulation contributes to aging (physiological or pathological) remains unclear. Since affected tissues in age-associated disorders and in pathological aging are mainly of mesenchymal origin we propose a model of human aging based on mesenchymal stem cells (hMSCs) which accumulate prelamin A. We demonstrate that prelamin A-accumulating hMSCs have a premature aging phenotype which affects their functional competence in vivo. The combination of prelamin A accumulation and stress conditions enhance the aging phenotype by dysregulating the activity of the octamer binding protein Oct-1This experimental model has been fundamental to identify a new role for Oct-1 in hMSCs aging. Impact Journals LLC 2014-04-06 /pmc/articles/PMC4032794/ /pubmed/24753226 Text en Copyright: © 2014 Infante 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
Infante, Arantza
Gago, Andrea
de Eguino, Garbiñe Ruiz
Calvo-Fernández, Teresa
Gómez-Vallejo, Vanessa
Llop, Jordi
Schlangen, Karin
Fullaondo, Ane
Aransay, Ana M.
Martín, Abraham
Rodríguez, Clara I.
Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell
title Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell
title_full Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell
title_fullStr Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell
title_full_unstemmed Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell
title_short Prelamin A accumulation and stress conditions induce impaired Oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell
title_sort prelamin a accumulation and stress conditions induce impaired oct-1 activity and autophagy in prematurely aged human mesenchymal stem cell
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4032794/
https://www.ncbi.nlm.nih.gov/pubmed/24753226
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