Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function

Sphingoid bases (SBs) as bioactive sphingolipids, have been implicated in aging in yeast. However, we know neither how SBs are regulated during yeast aging nor how they, in turn, regulate it. Herein, we demonstrate that the yeast alkaline ceramidases (YPC1 and YDC1) and SB kinases (LCB4 and LCB5) co...

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Autores principales: Yi, Jae Kyo, Xu, Ruijuan, Jeong, Eunmi, Mileva, Izolda, Truman, Jean-Philip, Lin, Chih-li, Wang, Kai, Snider, Justin, Wen, Sally, Obeid, Lina M., Hannun, Yusuf A., Mao, Cungui
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper: Gerotarget (Focus on Aging)
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5008273/
https://www.ncbi.nlm.nih.gov/pubmed/27008706
http://dx.doi.org/10.18632/oncotarget.8195
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author Yi, Jae Kyo
Xu, Ruijuan
Jeong, Eunmi
Mileva, Izolda
Truman, Jean-Philip
Lin, Chih-li
Wang, Kai
Snider, Justin
Wen, Sally
Obeid, Lina M.
Hannun, Yusuf A.
Mao, Cungui
author_facet Yi, Jae Kyo
Xu, Ruijuan
Jeong, Eunmi
Mileva, Izolda
Truman, Jean-Philip
Lin, Chih-li
Wang, Kai
Snider, Justin
Wen, Sally
Obeid, Lina M.
Hannun, Yusuf A.
Mao, Cungui
author_sort Yi, Jae Kyo
collection PubMed
description Sphingoid bases (SBs) as bioactive sphingolipids, have been implicated in aging in yeast. However, we know neither how SBs are regulated during yeast aging nor how they, in turn, regulate it. Herein, we demonstrate that the yeast alkaline ceramidases (YPC1 and YDC1) and SB kinases (LCB4 and LCB5) cooperate in regulating SBs during the aging process and that SBs shortens chronological life span (CLS) by compromising mitochondrial functions. With a lipidomics approach, we found that SBs were increased in a time-dependent manner during yeast aging. We also demonstrated that among the enzymes known for being responsible for the metabolism of SBs, YPC1 was upregulated whereas LCB4/5 were downregulated in the course of aging. This inverse regulation of YPC1 and LCB4/5 led to the aging-related upregulation of SBs in yeast and a reduction in CLS. With the proteomics-based approach (SILAC), we revealed that increased SBs altered the levels of proteins related to mitochondria. Further mechanistic studies demonstrated that increased SBs inhibited mitochondrial fusion and caused fragmentation, resulting in decreases in mtDNA copy numbers, ATP levels, mitochondrial membrane potentials, and oxygen consumption. Taken together, these results suggest that increased SBs mediate the aging process by impairing mitochondrial structural integrity and functions.
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spelling pubmed-50082732016-09-12 Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function Yi, Jae Kyo Xu, Ruijuan Jeong, Eunmi Mileva, Izolda Truman, Jean-Philip Lin, Chih-li Wang, Kai Snider, Justin Wen, Sally Obeid, Lina M. Hannun, Yusuf A. Mao, Cungui Oncotarget Research Paper: Gerotarget (Focus on Aging) Sphingoid bases (SBs) as bioactive sphingolipids, have been implicated in aging in yeast. However, we know neither how SBs are regulated during yeast aging nor how they, in turn, regulate it. Herein, we demonstrate that the yeast alkaline ceramidases (YPC1 and YDC1) and SB kinases (LCB4 and LCB5) cooperate in regulating SBs during the aging process and that SBs shortens chronological life span (CLS) by compromising mitochondrial functions. With a lipidomics approach, we found that SBs were increased in a time-dependent manner during yeast aging. We also demonstrated that among the enzymes known for being responsible for the metabolism of SBs, YPC1 was upregulated whereas LCB4/5 were downregulated in the course of aging. This inverse regulation of YPC1 and LCB4/5 led to the aging-related upregulation of SBs in yeast and a reduction in CLS. With the proteomics-based approach (SILAC), we revealed that increased SBs altered the levels of proteins related to mitochondria. Further mechanistic studies demonstrated that increased SBs inhibited mitochondrial fusion and caused fragmentation, resulting in decreases in mtDNA copy numbers, ATP levels, mitochondrial membrane potentials, and oxygen consumption. Taken together, these results suggest that increased SBs mediate the aging process by impairing mitochondrial structural integrity and functions. Impact Journals LLC 2016-03-19 /pmc/articles/PMC5008273/ /pubmed/27008706 http://dx.doi.org/10.18632/oncotarget.8195 Text en Copyright: © 2016 Yi 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: Gerotarget (Focus on Aging)
Yi, Jae Kyo
Xu, Ruijuan
Jeong, Eunmi
Mileva, Izolda
Truman, Jean-Philip
Lin, Chih-li
Wang, Kai
Snider, Justin
Wen, Sally
Obeid, Lina M.
Hannun, Yusuf A.
Mao, Cungui
Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function
title Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function
title_full Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function
title_fullStr Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function
title_full_unstemmed Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function
title_short Aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function
title_sort aging-related elevation of sphingoid bases shortens yeast chronological life span by compromising mitochondrial function
topic Research Paper: Gerotarget (Focus on Aging)
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5008273/
https://www.ncbi.nlm.nih.gov/pubmed/27008706
http://dx.doi.org/10.18632/oncotarget.8195
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