Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension

Invasive bladder tumours express the cell-surface Sialyl-Tn (STn) antigen, which stems from a premature stop in protein O-glycosylation. The STn antigen favours invasion, immune escape, and possibly chemotherapy resistance, making it attractive for target therapeutics. However, the events leading to...

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Autores principales: Peixoto, Andreia, Fernandes, Elisabete, Gaiteiro, Cristiana, Lima, Luís, Azevedo, Rita, Soares, Janine, Cotton, Sofia, Parreira, Beatriz, Neves, Manuel, Amaro, Teresina, Tavares, Ana, Teixeira, Filipe, Palmeira, Carlos, Rangel, Maria, Silva, André M.N., Reis, Celso A., Santos, Lúcio Lara, Oliveira, Maria José, Ferreira, José Alexandre
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5325352/
https://www.ncbi.nlm.nih.gov/pubmed/27542232
http://dx.doi.org/10.18632/oncotarget.11257
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author Peixoto, Andreia
Fernandes, Elisabete
Gaiteiro, Cristiana
Lima, Luís
Azevedo, Rita
Soares, Janine
Cotton, Sofia
Parreira, Beatriz
Neves, Manuel
Amaro, Teresina
Tavares, Ana
Teixeira, Filipe
Palmeira, Carlos
Rangel, Maria
Silva, André M.N.
Reis, Celso A.
Santos, Lúcio Lara
Oliveira, Maria José
Ferreira, José Alexandre
author_facet Peixoto, Andreia
Fernandes, Elisabete
Gaiteiro, Cristiana
Lima, Luís
Azevedo, Rita
Soares, Janine
Cotton, Sofia
Parreira, Beatriz
Neves, Manuel
Amaro, Teresina
Tavares, Ana
Teixeira, Filipe
Palmeira, Carlos
Rangel, Maria
Silva, André M.N.
Reis, Celso A.
Santos, Lúcio Lara
Oliveira, Maria José
Ferreira, José Alexandre
author_sort Peixoto, Andreia
collection PubMed
description Invasive bladder tumours express the cell-surface Sialyl-Tn (STn) antigen, which stems from a premature stop in protein O-glycosylation. The STn antigen favours invasion, immune escape, and possibly chemotherapy resistance, making it attractive for target therapeutics. However, the events leading to such deregulation in protein glycosylation are mostly unknown. Since hypoxia is a salient feature of advanced stage tumours, we searched into how it influences bladder cancer cells glycophenotype, with emphasis on STn expression. Therefore, three bladder cancer cell lines with distinct genetic and molecular backgrounds (T24, 5637 and HT1376) were submitted to hypoxia. To disclose HIF-1α-mediated events, experiments were also conducted in the presence of Deferoxamine Mesilate (Dfx), an inhibitor of HIF-1α proteasomal degradation. In both conditions all cell lines overexpressed HIF-1α and its transcriptionally-regulated protein CA-IX. This was accompanied by increased lactate biosynthesis, denoting a shift toward anaerobic metabolism. Concomitantly, T24 and 5637 cells acquired a more motile phenotype, consistent with their more mesenchymal characteristics. Moreover, hypoxia promoted STn antigen overexpression in all cell lines and enhanced the migration and invasion of those presenting more mesenchymal characteristics, in an HIF-1α-dependent manner. These effects were reversed by reoxygenation, demonstrating that oxygen affects O-glycan extension. Glycoproteomics studies highlighted that STn was mainly present in integrins and cadherins, suggesting a possible role for this glycan in adhesion, cell motility and invasion. The association between HIF-1α and STn overexpressions and tumour invasion was further confirmed in bladder cancer patient samples. In conclusion, STn overexpression may, in part, result from a HIF-1α mediated cell-survival strategy to adapt to the hypoxic challenge, favouring cell invasion. In addition, targeting STn-expressing glycoproteins may offer potential to treat tumour hypoxic niches harbouring more malignant cells.
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spelling pubmed-53253522017-03-23 Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension Peixoto, Andreia Fernandes, Elisabete Gaiteiro, Cristiana Lima, Luís Azevedo, Rita Soares, Janine Cotton, Sofia Parreira, Beatriz Neves, Manuel Amaro, Teresina Tavares, Ana Teixeira, Filipe Palmeira, Carlos Rangel, Maria Silva, André M.N. Reis, Celso A. Santos, Lúcio Lara Oliveira, Maria José Ferreira, José Alexandre Oncotarget Research Paper Invasive bladder tumours express the cell-surface Sialyl-Tn (STn) antigen, which stems from a premature stop in protein O-glycosylation. The STn antigen favours invasion, immune escape, and possibly chemotherapy resistance, making it attractive for target therapeutics. However, the events leading to such deregulation in protein glycosylation are mostly unknown. Since hypoxia is a salient feature of advanced stage tumours, we searched into how it influences bladder cancer cells glycophenotype, with emphasis on STn expression. Therefore, three bladder cancer cell lines with distinct genetic and molecular backgrounds (T24, 5637 and HT1376) were submitted to hypoxia. To disclose HIF-1α-mediated events, experiments were also conducted in the presence of Deferoxamine Mesilate (Dfx), an inhibitor of HIF-1α proteasomal degradation. In both conditions all cell lines overexpressed HIF-1α and its transcriptionally-regulated protein CA-IX. This was accompanied by increased lactate biosynthesis, denoting a shift toward anaerobic metabolism. Concomitantly, T24 and 5637 cells acquired a more motile phenotype, consistent with their more mesenchymal characteristics. Moreover, hypoxia promoted STn antigen overexpression in all cell lines and enhanced the migration and invasion of those presenting more mesenchymal characteristics, in an HIF-1α-dependent manner. These effects were reversed by reoxygenation, demonstrating that oxygen affects O-glycan extension. Glycoproteomics studies highlighted that STn was mainly present in integrins and cadherins, suggesting a possible role for this glycan in adhesion, cell motility and invasion. The association between HIF-1α and STn overexpressions and tumour invasion was further confirmed in bladder cancer patient samples. In conclusion, STn overexpression may, in part, result from a HIF-1α mediated cell-survival strategy to adapt to the hypoxic challenge, favouring cell invasion. In addition, targeting STn-expressing glycoproteins may offer potential to treat tumour hypoxic niches harbouring more malignant cells. Impact Journals LLC 2016-08-12 /pmc/articles/PMC5325352/ /pubmed/27542232 http://dx.doi.org/10.18632/oncotarget.11257 Text en Copyright: © 2016 Peixoto 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
Peixoto, Andreia
Fernandes, Elisabete
Gaiteiro, Cristiana
Lima, Luís
Azevedo, Rita
Soares, Janine
Cotton, Sofia
Parreira, Beatriz
Neves, Manuel
Amaro, Teresina
Tavares, Ana
Teixeira, Filipe
Palmeira, Carlos
Rangel, Maria
Silva, André M.N.
Reis, Celso A.
Santos, Lúcio Lara
Oliveira, Maria José
Ferreira, José Alexandre
Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension
title Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension
title_full Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension
title_fullStr Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension
title_full_unstemmed Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension
title_short Hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein O-glycosylation extension
title_sort hypoxia enhances the malignant nature of bladder cancer cells and concomitantly antagonizes protein o-glycosylation extension
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5325352/
https://www.ncbi.nlm.nih.gov/pubmed/27542232
http://dx.doi.org/10.18632/oncotarget.11257
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