Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway

Haem oxygenase (HO)-1/carbon monoxide (CO) protects cancer cells from oxidative stress, but the gas-responsive signalling mechanisms remain unknown. Here we show using metabolomics that CO-sensitive methylation of PFKFB3, an enzyme producing fructose 2,6-bisphosphate (F-2,6-BP), serves as a switch t...

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Autores principales: Yamamoto, Takehiro, Takano, Naoharu, Ishiwata, Kyoko, Ohmura, Mitsuyo, Nagahata, Yoshiko, Matsuura, Tomomi, Kamata, Aki, Sakamoto, Kyoko, Nakanishi, Tsuyoshi, Kubo, Akiko, Hishiki, Takako, Suematsu, Makoto
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Pub. Group 2014
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3959213/
https://www.ncbi.nlm.nih.gov/pubmed/24633012
http://dx.doi.org/10.1038/ncomms4480
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author Yamamoto, Takehiro
Takano, Naoharu
Ishiwata, Kyoko
Ohmura, Mitsuyo
Nagahata, Yoshiko
Matsuura, Tomomi
Kamata, Aki
Sakamoto, Kyoko
Nakanishi, Tsuyoshi
Kubo, Akiko
Hishiki, Takako
Suematsu, Makoto
author_facet Yamamoto, Takehiro
Takano, Naoharu
Ishiwata, Kyoko
Ohmura, Mitsuyo
Nagahata, Yoshiko
Matsuura, Tomomi
Kamata, Aki
Sakamoto, Kyoko
Nakanishi, Tsuyoshi
Kubo, Akiko
Hishiki, Takako
Suematsu, Makoto
author_sort Yamamoto, Takehiro
collection PubMed
description Haem oxygenase (HO)-1/carbon monoxide (CO) protects cancer cells from oxidative stress, but the gas-responsive signalling mechanisms remain unknown. Here we show using metabolomics that CO-sensitive methylation of PFKFB3, an enzyme producing fructose 2,6-bisphosphate (F-2,6-BP), serves as a switch to activate phosphofructokinase-1, a rate-limiting glycolytic enzyme. In human leukaemia U937 cells, PFKFB3 is asymmetrically di-methylated at R131 and R134 through modification by protein arginine methyltransferase 1. HO-1 induction or CO results in reduced methylation of PFKFB3 in varied cancer cells to suppress F-2,6-BP, shifting glucose utilization from glycolysis toward the pentose phosphate pathway. Loss of PFKFB3 methylation depends on the inhibitory effects of CO on haem-containing cystathionine β-synthase (CBS). CBS modulates remethylation metabolism, and increases NADPH to supply reduced glutathione, protecting cells from oxidative stress and anti-cancer reagents. Once the methylation of PFKFB3 is reduced, the protein undergoes polyubiquitination and is degraded in the proteasome. These results suggest that the CO/CBS-dependent regulation of PFKFB3 methylation determines directional glucose utilization to ensure resistance against oxidative stress for cancer cell survival.
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spelling pubmed-39592132014-03-20 Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway Yamamoto, Takehiro Takano, Naoharu Ishiwata, Kyoko Ohmura, Mitsuyo Nagahata, Yoshiko Matsuura, Tomomi Kamata, Aki Sakamoto, Kyoko Nakanishi, Tsuyoshi Kubo, Akiko Hishiki, Takako Suematsu, Makoto Nat Commun Article Haem oxygenase (HO)-1/carbon monoxide (CO) protects cancer cells from oxidative stress, but the gas-responsive signalling mechanisms remain unknown. Here we show using metabolomics that CO-sensitive methylation of PFKFB3, an enzyme producing fructose 2,6-bisphosphate (F-2,6-BP), serves as a switch to activate phosphofructokinase-1, a rate-limiting glycolytic enzyme. In human leukaemia U937 cells, PFKFB3 is asymmetrically di-methylated at R131 and R134 through modification by protein arginine methyltransferase 1. HO-1 induction or CO results in reduced methylation of PFKFB3 in varied cancer cells to suppress F-2,6-BP, shifting glucose utilization from glycolysis toward the pentose phosphate pathway. Loss of PFKFB3 methylation depends on the inhibitory effects of CO on haem-containing cystathionine β-synthase (CBS). CBS modulates remethylation metabolism, and increases NADPH to supply reduced glutathione, protecting cells from oxidative stress and anti-cancer reagents. Once the methylation of PFKFB3 is reduced, the protein undergoes polyubiquitination and is degraded in the proteasome. These results suggest that the CO/CBS-dependent regulation of PFKFB3 methylation determines directional glucose utilization to ensure resistance against oxidative stress for cancer cell survival. Nature Pub. Group 2014-03-17 /pmc/articles/PMC3959213/ /pubmed/24633012 http://dx.doi.org/10.1038/ncomms4480 Text en Copyright © 2014, Nature Publishing Group, a division of Macmillan Publishers Limited. All Rights Reserved. http://creativecommons.org/licenses/by-nc-nd/3.0/ This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivs 3.0 Unported License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by-nc-nd/3.0/
spellingShingle Article
Yamamoto, Takehiro
Takano, Naoharu
Ishiwata, Kyoko
Ohmura, Mitsuyo
Nagahata, Yoshiko
Matsuura, Tomomi
Kamata, Aki
Sakamoto, Kyoko
Nakanishi, Tsuyoshi
Kubo, Akiko
Hishiki, Takako
Suematsu, Makoto
Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway
title Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway
title_full Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway
title_fullStr Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway
title_full_unstemmed Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway
title_short Reduced methylation of PFKFB3 in cancer cells shunts glucose towards the pentose phosphate pathway
title_sort reduced methylation of pfkfb3 in cancer cells shunts glucose towards the pentose phosphate pathway
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3959213/
https://www.ncbi.nlm.nih.gov/pubmed/24633012
http://dx.doi.org/10.1038/ncomms4480
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