Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing

Mammalian target of rapamycin complex 1 (mTORC1) and cell senescence are intimately linked to each other and to organismal aging. Inhibition of mTORC1 is the best-known intervention to extend lifespan, and recent evidence suggests that clearance of senescent cells can also improve health and lifespa...

Descripción completa

Detalles Bibliográficos
Autores principales: Carroll, Bernadette, Nelson, Glyn, Rabanal-Ruiz, Yoana, Kucheryavenko, Olena, Dunhill-Turner, Natasha A., Chesterman, Charlotte C., Zahari, Qabil, Zhang, Tong, Conduit, Sarah E., Mitchell, Christina A., Maddocks, Oliver D.K., Lovat, Penny, von Zglinicki, Thomas, Korolchuk, Viktor I.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2017
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5496614/
https://www.ncbi.nlm.nih.gov/pubmed/28566325
http://dx.doi.org/10.1083/jcb.201610113
_version_ 1783248018809552896
author Carroll, Bernadette
Nelson, Glyn
Rabanal-Ruiz, Yoana
Kucheryavenko, Olena
Dunhill-Turner, Natasha A.
Chesterman, Charlotte C.
Zahari, Qabil
Zhang, Tong
Conduit, Sarah E.
Mitchell, Christina A.
Maddocks, Oliver D.K.
Lovat, Penny
von Zglinicki, Thomas
Korolchuk, Viktor I.
author_facet Carroll, Bernadette
Nelson, Glyn
Rabanal-Ruiz, Yoana
Kucheryavenko, Olena
Dunhill-Turner, Natasha A.
Chesterman, Charlotte C.
Zahari, Qabil
Zhang, Tong
Conduit, Sarah E.
Mitchell, Christina A.
Maddocks, Oliver D.K.
Lovat, Penny
von Zglinicki, Thomas
Korolchuk, Viktor I.
author_sort Carroll, Bernadette
collection PubMed
description Mammalian target of rapamycin complex 1 (mTORC1) and cell senescence are intimately linked to each other and to organismal aging. Inhibition of mTORC1 is the best-known intervention to extend lifespan, and recent evidence suggests that clearance of senescent cells can also improve health and lifespan. Enhanced mTORC1 activity drives characteristic phenotypes of senescence, although the underlying mechanisms responsible for increased activity are not well understood. We have identified that in human fibroblasts rendered senescent by stress, replicative exhaustion, or oncogene activation, mTORC1 is constitutively active and resistant to serum and amino acid starvation. This is driven in part by depolarization of senescent cell plasma membrane, which leads to primary cilia defects and a resultant failure to inhibit growth factor signaling. Further, increased autophagy and high levels of intracellular amino acids may act to support mTORC1 activity in starvation conditions. Interventions to correct these phenotypes restore sensitivity to the mTORC1 signaling pathway and cause death, indicating that persistent signaling supports senescent cell survival.
format Online
Article
Text
id pubmed-5496614
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher The Rockefeller University Press
record_format MEDLINE/PubMed
spelling pubmed-54966142017-07-05 Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing Carroll, Bernadette Nelson, Glyn Rabanal-Ruiz, Yoana Kucheryavenko, Olena Dunhill-Turner, Natasha A. Chesterman, Charlotte C. Zahari, Qabil Zhang, Tong Conduit, Sarah E. Mitchell, Christina A. Maddocks, Oliver D.K. Lovat, Penny von Zglinicki, Thomas Korolchuk, Viktor I. J Cell Biol Research Articles Mammalian target of rapamycin complex 1 (mTORC1) and cell senescence are intimately linked to each other and to organismal aging. Inhibition of mTORC1 is the best-known intervention to extend lifespan, and recent evidence suggests that clearance of senescent cells can also improve health and lifespan. Enhanced mTORC1 activity drives characteristic phenotypes of senescence, although the underlying mechanisms responsible for increased activity are not well understood. We have identified that in human fibroblasts rendered senescent by stress, replicative exhaustion, or oncogene activation, mTORC1 is constitutively active and resistant to serum and amino acid starvation. This is driven in part by depolarization of senescent cell plasma membrane, which leads to primary cilia defects and a resultant failure to inhibit growth factor signaling. Further, increased autophagy and high levels of intracellular amino acids may act to support mTORC1 activity in starvation conditions. Interventions to correct these phenotypes restore sensitivity to the mTORC1 signaling pathway and cause death, indicating that persistent signaling supports senescent cell survival. The Rockefeller University Press 2017-07-03 /pmc/articles/PMC5496614/ /pubmed/28566325 http://dx.doi.org/10.1083/jcb.201610113 Text en © 2017 Carroll et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Carroll, Bernadette
Nelson, Glyn
Rabanal-Ruiz, Yoana
Kucheryavenko, Olena
Dunhill-Turner, Natasha A.
Chesterman, Charlotte C.
Zahari, Qabil
Zhang, Tong
Conduit, Sarah E.
Mitchell, Christina A.
Maddocks, Oliver D.K.
Lovat, Penny
von Zglinicki, Thomas
Korolchuk, Viktor I.
Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing
title Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing
title_full Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing
title_fullStr Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing
title_full_unstemmed Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing
title_short Persistent mTORC1 signaling in cell senescence results from defects in amino acid and growth factor sensing
title_sort persistent mtorc1 signaling in cell senescence results from defects in amino acid and growth factor sensing
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5496614/
https://www.ncbi.nlm.nih.gov/pubmed/28566325
http://dx.doi.org/10.1083/jcb.201610113
work_keys_str_mv AT carrollbernadette persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT nelsonglyn persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT rabanalruizyoana persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT kucheryavenkoolena persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT dunhillturnernatashaa persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT chestermancharlottec persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT zahariqabil persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT zhangtong persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT conduitsarahe persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT mitchellchristinaa persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT maddocksoliverdk persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT lovatpenny persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT vonzglinickithomas persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing
AT korolchukviktori persistentmtorc1signalingincellsenescenceresultsfromdefectsinaminoacidandgrowthfactorsensing

Ejemplares similares