Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress

Abstract Despite progress in the use of hyperthermia in clinical practice, the thermosensitivity of cancer cells is poorly understood. In a previous study, we found that sensitivity to hyperthermia varied between ovarian and uterine cancer cell lines. Upon hyperthermia, glycolytic enzymes decreased...

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Main Authors: Taisei Kanamori, Natumi Miyazaki, Shigeki Aoki, Kousei Ito, Akihiro Hisaka, Hiroto Hatakeyama
Format: Article
Language:English
Published: Nature Publishing Group 2021-07-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-94031-9
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spelling doaj-29d450f437a043cead84a8f2f6f644992021-07-25T11:24:44ZengNature Publishing GroupScientific Reports2045-23222021-07-0111111110.1038/s41598-021-94031-9Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stressTaisei Kanamori0Natumi Miyazaki1Shigeki Aoki2Kousei Ito3Akihiro Hisaka4Hiroto Hatakeyama5Laboratory of Clinical Pharmacology and Pharmacometrics, Graduate School of Pharmaceutical Sciences, Chiba UniversityLaboratory of Biopharmaceutics, Graduate School of Pharmaceutical Sciences, Chiba UniversityLaboratory of Biopharmaceutics, Graduate School of Pharmaceutical Sciences, Chiba UniversityLaboratory of Biopharmaceutics, Graduate School of Pharmaceutical Sciences, Chiba UniversityLaboratory of Clinical Pharmacology and Pharmacometrics, Graduate School of Pharmaceutical Sciences, Chiba UniversityLaboratory of Clinical Pharmacology and Pharmacometrics, Graduate School of Pharmaceutical Sciences, Chiba UniversityAbstract Despite progress in the use of hyperthermia in clinical practice, the thermosensitivity of cancer cells is poorly understood. In a previous study, we found that sensitivity to hyperthermia varied between ovarian and uterine cancer cell lines. Upon hyperthermia, glycolytic enzymes decreased in hyperthermia-resistant SKOV3 cells. However, the mechanisms of glycolysis inhibition and their relationship with thermoresistance remain to be explored. In this study, metabolomic analysis indicated the downregulation of glycolytic metabolites in SKOV3 cells after hyperthermia. Proteomic and pathway analyses predicted that the ubiquitin pathway was explicitly activated in resistant SKOV3 cells, compared with hyperthermia-sensitive A2780 cells, and STUB1, a ubiquitin ligase, potentially targeted PKM, a glycolytic rate-limiting enzyme. PKM is degraded via ubiquitination upon hyperthermia. Although glycolysis is inactivated by hyperthermia, ATP production is maintained. We observed that oxygen consumption and mitochondrial membrane potential were activated in SKOV3 cells but suppressed in A2780 cells. The activation of mitochondria could compensate for the loss of ATP production due to the suppression of glycolysis by hyperthermia. Although the physiological significance has not yet been elucidated, our results demonstrated that metabolomic adaptation from the Warburg effect to mitochondrial oxidative phosphorylation could contribute to thermoresistance in ovarian and uterine cancer cells.https://doi.org/10.1038/s41598-021-94031-9
collection DOAJ
language English
format Article
sources DOAJ
author Taisei Kanamori
Natumi Miyazaki
Shigeki Aoki
Kousei Ito
Akihiro Hisaka
Hiroto Hatakeyama
spellingShingle Taisei Kanamori
Natumi Miyazaki
Shigeki Aoki
Kousei Ito
Akihiro Hisaka
Hiroto Hatakeyama
Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress
Scientific Reports
author_facet Taisei Kanamori
Natumi Miyazaki
Shigeki Aoki
Kousei Ito
Akihiro Hisaka
Hiroto Hatakeyama
author_sort Taisei Kanamori
title Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress
title_short Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress
title_full Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress
title_fullStr Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress
title_full_unstemmed Investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress
title_sort investigation of energy metabolic dynamism in hyperthermia-resistant ovarian and uterine cancer cells under heat stress
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-07-01
description Abstract Despite progress in the use of hyperthermia in clinical practice, the thermosensitivity of cancer cells is poorly understood. In a previous study, we found that sensitivity to hyperthermia varied between ovarian and uterine cancer cell lines. Upon hyperthermia, glycolytic enzymes decreased in hyperthermia-resistant SKOV3 cells. However, the mechanisms of glycolysis inhibition and their relationship with thermoresistance remain to be explored. In this study, metabolomic analysis indicated the downregulation of glycolytic metabolites in SKOV3 cells after hyperthermia. Proteomic and pathway analyses predicted that the ubiquitin pathway was explicitly activated in resistant SKOV3 cells, compared with hyperthermia-sensitive A2780 cells, and STUB1, a ubiquitin ligase, potentially targeted PKM, a glycolytic rate-limiting enzyme. PKM is degraded via ubiquitination upon hyperthermia. Although glycolysis is inactivated by hyperthermia, ATP production is maintained. We observed that oxygen consumption and mitochondrial membrane potential were activated in SKOV3 cells but suppressed in A2780 cells. The activation of mitochondria could compensate for the loss of ATP production due to the suppression of glycolysis by hyperthermia. Although the physiological significance has not yet been elucidated, our results demonstrated that metabolomic adaptation from the Warburg effect to mitochondrial oxidative phosphorylation could contribute to thermoresistance in ovarian and uterine cancer cells.
url https://doi.org/10.1038/s41598-021-94031-9
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