ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines

ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines

Abstract Background Hypoxia is an important factor that contributes to tumour aggressiveness and correlates with poor prognosis and resistance to conventional therapy. Therefore, identifying hypoxic environments within tumours is extremely useful for understanding cancer biology and developing novel...

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Main Authors: Norio Takei, Akihiro Yoneda, Marina Kosaka, Kaori Sakai-Sawada, Yasuaki Tamura
Format: Article
Language:English
Published: BMC 2019-05-01
Series:BMC Cancer
Subjects:
ERO1α
Hypoxia
Biomarker
CA9
Cancer
Online Access:http://link.springer.com/article/10.1186/s12885-019-5727-9
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spelling doaj-92ce05cc698f4491be1e24a9f88eed042020-11-25T02:52:33ZengBMCBMC Cancer1471-24072019-05-0119111010.1186/s12885-019-5727-9ERO1α is a novel endogenous marker of hypoxia in human cancer cell linesNorio Takei0Akihiro Yoneda1Marina Kosaka2Kaori Sakai-Sawada3Yasuaki Tamura4Department of Molecular Therapeutics, Center for Food and Medical Innovation, Institute for the Promotion of Business-Regional Collaboration, Hokkaido UniversityDepartment of Molecular Therapeutics, Center for Food and Medical Innovation, Institute for the Promotion of Business-Regional Collaboration, Hokkaido UniversityDepartment of Molecular Therapeutics, Center for Food and Medical Innovation, Institute for the Promotion of Business-Regional Collaboration, Hokkaido UniversityDepartment of Molecular Therapeutics, Center for Food and Medical Innovation, Institute for the Promotion of Business-Regional Collaboration, Hokkaido UniversityDepartment of Molecular Therapeutics, Center for Food and Medical Innovation, Institute for the Promotion of Business-Regional Collaboration, Hokkaido UniversityAbstract Background Hypoxia is an important factor that contributes to tumour aggressiveness and correlates with poor prognosis and resistance to conventional therapy. Therefore, identifying hypoxic environments within tumours is extremely useful for understanding cancer biology and developing novel therapeutic strategies. Several studies have suggested that carbonic anhydrase 9 (CA9) is a reliable biomarker of hypoxia and a potential therapeutic target, while pimonidazole has been identified as an exogenous hypoxia marker. However, other studies have suggested that CA9 expression is not directly induced by hypoxia and it is not expressed in all types of tumours. Thus, in this study, we focused on endoplasmic reticulum disulphide oxidase 1α (ERO1α), a protein that localises in the endoplasmic reticulum and is involved in the formation of disulphide bonds in proteins, to determine whether it could serve as a potential tumour-hypoxia biomarker. Methods Using quantitative real-time polymerase chain reaction, we analysed the mRNA expression of ERO1α and CA9 in different normal and cancer cell lines. We also determined the protein expression levels of ERO1α and CA9 in these cell lines by western blotting. We then investigated the hypoxia-inducible ERO1α and CA9 expression and localisation in HCT116 and HeLa cells, which express low (CA9-low) and high (CA9-high) levels of CA9, respectively. A comparative analysis was performed using pimonidazole, an exogenous hypoxic marker, as a positive control. The expression and localisation of ERO1α and CA9 in tumour spheres during hypoxia were analysed by a tumour sphere formation assay. Finally, we used a mouse model to investigate the localisation of ERO1α and CA9 in tumour xenografts using several cell lines. Results We found that ERO1α expression increased under chronic hypoxia. Our results show that ERO1α was hypoxia-induced in all the tested cancer cell lines. Furthermore, in the comparative analysis using CA9 and pimonidazole, ERO1α had a similar localisation to pimonidazole in both CA9-low and CA9-high cell lines. Conclusion ERO1α can serve as a novel endogenous chronic hypoxia marker that is more reliable than CA9 and can be used as a diagnostic biomarker and therapeutic target for cancer.http://link.springer.com/article/10.1186/s12885-019-5727-9ERO1αHypoxiaBiomarkerCA9Cancer
collection DOAJ
language English
format Article
sources DOAJ
author Norio Takei
Akihiro Yoneda
Marina Kosaka
Kaori Sakai-Sawada
Yasuaki Tamura
spellingShingle Norio Takei
Akihiro Yoneda
Marina Kosaka
Kaori Sakai-Sawada
Yasuaki Tamura
ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines
BMC Cancer
ERO1α
Hypoxia
Biomarker
CA9
Cancer
author_facet Norio Takei
Akihiro Yoneda
Marina Kosaka
Kaori Sakai-Sawada
Yasuaki Tamura
author_sort Norio Takei
title ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines
title_short ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines
title_full ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines
title_fullStr ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines
title_full_unstemmed ERO1α is a novel endogenous marker of hypoxia in human cancer cell lines
title_sort ero1α is a novel endogenous marker of hypoxia in human cancer cell lines
publisher BMC
series BMC Cancer
issn 1471-2407
publishDate 2019-05-01
description Abstract Background Hypoxia is an important factor that contributes to tumour aggressiveness and correlates with poor prognosis and resistance to conventional therapy. Therefore, identifying hypoxic environments within tumours is extremely useful for understanding cancer biology and developing novel therapeutic strategies. Several studies have suggested that carbonic anhydrase 9 (CA9) is a reliable biomarker of hypoxia and a potential therapeutic target, while pimonidazole has been identified as an exogenous hypoxia marker. However, other studies have suggested that CA9 expression is not directly induced by hypoxia and it is not expressed in all types of tumours. Thus, in this study, we focused on endoplasmic reticulum disulphide oxidase 1α (ERO1α), a protein that localises in the endoplasmic reticulum and is involved in the formation of disulphide bonds in proteins, to determine whether it could serve as a potential tumour-hypoxia biomarker. Methods Using quantitative real-time polymerase chain reaction, we analysed the mRNA expression of ERO1α and CA9 in different normal and cancer cell lines. We also determined the protein expression levels of ERO1α and CA9 in these cell lines by western blotting. We then investigated the hypoxia-inducible ERO1α and CA9 expression and localisation in HCT116 and HeLa cells, which express low (CA9-low) and high (CA9-high) levels of CA9, respectively. A comparative analysis was performed using pimonidazole, an exogenous hypoxic marker, as a positive control. The expression and localisation of ERO1α and CA9 in tumour spheres during hypoxia were analysed by a tumour sphere formation assay. Finally, we used a mouse model to investigate the localisation of ERO1α and CA9 in tumour xenografts using several cell lines. Results We found that ERO1α expression increased under chronic hypoxia. Our results show that ERO1α was hypoxia-induced in all the tested cancer cell lines. Furthermore, in the comparative analysis using CA9 and pimonidazole, ERO1α had a similar localisation to pimonidazole in both CA9-low and CA9-high cell lines. Conclusion ERO1α can serve as a novel endogenous chronic hypoxia marker that is more reliable than CA9 and can be used as a diagnostic biomarker and therapeutic target for cancer.
topic ERO1α
Hypoxia
Biomarker
CA9
Cancer
url http://link.springer.com/article/10.1186/s12885-019-5727-9
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AT akihiroyoneda ero1aisanovelendogenousmarkerofhypoxiainhumancancercelllines
AT marinakosaka ero1aisanovelendogenousmarkerofhypoxiainhumancancercelllines
AT kaorisakaisawada ero1aisanovelendogenousmarkerofhypoxiainhumancancercelllines
AT yasuakitamura ero1aisanovelendogenousmarkerofhypoxiainhumancancercelllines
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