Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q

Mitochondrial energy production and function rely on optimal concentrations of the essential redox-active lipid, coenzyme Q (CoQ). CoQ deficiency results in mitochondrial dysfunction associated with increased mitochondrial oxidative stress and a range of pathologies. What drives CoQ deficiency in ma...

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Autores principales: Ayer, Anita, Fazakerley, Daniel J., Suarna, Cacang, Maghzal, Ghassan J., Sheipouri, Diba, Lee, Kevin J., Bradley, Michelle C., Fernández-del-Rio, Lucía, Tumanov, Sergey, Kong, Stephanie MY., van der Veen, Jelske N., Yang, Andrian, Ho, Joshua W.K., Clarke, Steven G., James, David E., Dawes, Ian W., Vance, Dennis E., Clarke, Catherine F., Jacobs, René L., Stocker, Roland
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8435697/
https://www.ncbi.nlm.nih.gov/pubmed/34521065
http://dx.doi.org/10.1016/j.redox.2021.102127
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author Ayer, Anita
Fazakerley, Daniel J.
Suarna, Cacang
Maghzal, Ghassan J.
Sheipouri, Diba
Lee, Kevin J.
Bradley, Michelle C.
Fernández-del-Rio, Lucía
Tumanov, Sergey
Kong, Stephanie MY.
van der Veen, Jelske N.
Yang, Andrian
Ho, Joshua W.K.
Clarke, Steven G.
James, David E.
Dawes, Ian W.
Vance, Dennis E.
Clarke, Catherine F.
Jacobs, René L.
Stocker, Roland
author_facet Ayer, Anita
Fazakerley, Daniel J.
Suarna, Cacang
Maghzal, Ghassan J.
Sheipouri, Diba
Lee, Kevin J.
Bradley, Michelle C.
Fernández-del-Rio, Lucía
Tumanov, Sergey
Kong, Stephanie MY.
van der Veen, Jelske N.
Yang, Andrian
Ho, Joshua W.K.
Clarke, Steven G.
James, David E.
Dawes, Ian W.
Vance, Dennis E.
Clarke, Catherine F.
Jacobs, René L.
Stocker, Roland
author_sort Ayer, Anita
collection PubMed
description Mitochondrial energy production and function rely on optimal concentrations of the essential redox-active lipid, coenzyme Q (CoQ). CoQ deficiency results in mitochondrial dysfunction associated with increased mitochondrial oxidative stress and a range of pathologies. What drives CoQ deficiency in many of these pathologies is unknown, just as there currently is no effective therapeutic strategy to overcome CoQ deficiency in humans. To date, large-scale studies aimed at systematically interrogating endogenous systems that control CoQ biosynthesis and their potential utility to treat disease have not been carried out. Therefore, we developed a quantitative high-throughput method to determine CoQ concentrations in yeast cells. Applying this method to the Yeast Deletion Collection as a genome-wide screen, 30 genes not known previously to regulate cellular concentrations of CoQ were discovered. In combination with untargeted lipidomics and metabolomics, phosphatidylethanolamine N-methyltransferase (PEMT) deficiency was confirmed as a positive regulator of CoQ synthesis, the first identified to date. Mechanistically, PEMT deficiency alters mitochondrial concentrations of one-carbon metabolites, characterized by an increase in the S-adenosylmethionine to S-adenosylhomocysteine (SAM-to-SAH) ratio that reflects mitochondrial methylation capacity, drives CoQ synthesis, and is associated with a decrease in mitochondrial oxidative stress. The newly described regulatory pathway appears evolutionary conserved, as ablation of PEMT using antisense oligonucleotides increases mitochondrial CoQ in mouse-derived adipocytes that translates to improved glucose utilization by these cells, and protection of mice from high-fat diet-induced insulin resistance. Our studies reveal a previously unrecognized relationship between two spatially distinct lipid pathways with potential implications for the treatment of CoQ deficiencies, mitochondrial oxidative stress/dysfunction, and associated diseases.
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spelling pubmed-84356972021-09-17 Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q Ayer, Anita Fazakerley, Daniel J. Suarna, Cacang Maghzal, Ghassan J. Sheipouri, Diba Lee, Kevin J. Bradley, Michelle C. Fernández-del-Rio, Lucía Tumanov, Sergey Kong, Stephanie MY. van der Veen, Jelske N. Yang, Andrian Ho, Joshua W.K. Clarke, Steven G. James, David E. Dawes, Ian W. Vance, Dennis E. Clarke, Catherine F. Jacobs, René L. Stocker, Roland Redox Biol Research Paper Mitochondrial energy production and function rely on optimal concentrations of the essential redox-active lipid, coenzyme Q (CoQ). CoQ deficiency results in mitochondrial dysfunction associated with increased mitochondrial oxidative stress and a range of pathologies. What drives CoQ deficiency in many of these pathologies is unknown, just as there currently is no effective therapeutic strategy to overcome CoQ deficiency in humans. To date, large-scale studies aimed at systematically interrogating endogenous systems that control CoQ biosynthesis and their potential utility to treat disease have not been carried out. Therefore, we developed a quantitative high-throughput method to determine CoQ concentrations in yeast cells. Applying this method to the Yeast Deletion Collection as a genome-wide screen, 30 genes not known previously to regulate cellular concentrations of CoQ were discovered. In combination with untargeted lipidomics and metabolomics, phosphatidylethanolamine N-methyltransferase (PEMT) deficiency was confirmed as a positive regulator of CoQ synthesis, the first identified to date. Mechanistically, PEMT deficiency alters mitochondrial concentrations of one-carbon metabolites, characterized by an increase in the S-adenosylmethionine to S-adenosylhomocysteine (SAM-to-SAH) ratio that reflects mitochondrial methylation capacity, drives CoQ synthesis, and is associated with a decrease in mitochondrial oxidative stress. The newly described regulatory pathway appears evolutionary conserved, as ablation of PEMT using antisense oligonucleotides increases mitochondrial CoQ in mouse-derived adipocytes that translates to improved glucose utilization by these cells, and protection of mice from high-fat diet-induced insulin resistance. Our studies reveal a previously unrecognized relationship between two spatially distinct lipid pathways with potential implications for the treatment of CoQ deficiencies, mitochondrial oxidative stress/dysfunction, and associated diseases. Elsevier 2021-09-08 /pmc/articles/PMC8435697/ /pubmed/34521065 http://dx.doi.org/10.1016/j.redox.2021.102127 Text en © 2021 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Paper
Ayer, Anita
Fazakerley, Daniel J.
Suarna, Cacang
Maghzal, Ghassan J.
Sheipouri, Diba
Lee, Kevin J.
Bradley, Michelle C.
Fernández-del-Rio, Lucía
Tumanov, Sergey
Kong, Stephanie MY.
van der Veen, Jelske N.
Yang, Andrian
Ho, Joshua W.K.
Clarke, Steven G.
James, David E.
Dawes, Ian W.
Vance, Dennis E.
Clarke, Catherine F.
Jacobs, René L.
Stocker, Roland
Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q
title Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q
title_full Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q
title_fullStr Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q
title_full_unstemmed Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q
title_short Genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme Q
title_sort genetic screening reveals phospholipid metabolism as a key regulator of the biosynthesis of the redox-active lipid coenzyme q
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8435697/
https://www.ncbi.nlm.nih.gov/pubmed/34521065
http://dx.doi.org/10.1016/j.redox.2021.102127
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