The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells

BACKGROUND: Colorectal cancer (CRC) is a leading cause of cancer death globally and new biomarkers and treatments are severely needed. METHODS: Here, we employed HCT116 and LoVo human CRC cells made resistant to either SN38 or oxaliplatin, to investigate whether altered expression of the high affini...

Descripción completa

Detalles Bibliográficos
Autores principales: Pedraz-Cuesta, Elena, Christensen, Sandra, Jensen, Anders A., Jensen, Niels Frank, Bunch, Lennart, Romer, Maria Unni, Brünner, Nils, Stenvang, Jan, Pedersen, Stine Falsig
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4445981/
https://www.ncbi.nlm.nih.gov/pubmed/25981639
http://dx.doi.org/10.1186/s12885-015-1405-8
_version_ 1782373352454750208
author Pedraz-Cuesta, Elena
Christensen, Sandra
Jensen, Anders A.
Jensen, Niels Frank
Bunch, Lennart
Romer, Maria Unni
Brünner, Nils
Stenvang, Jan
Pedersen, Stine Falsig
author_facet Pedraz-Cuesta, Elena
Christensen, Sandra
Jensen, Anders A.
Jensen, Niels Frank
Bunch, Lennart
Romer, Maria Unni
Brünner, Nils
Stenvang, Jan
Pedersen, Stine Falsig
author_sort Pedraz-Cuesta, Elena
collection PubMed
description BACKGROUND: Colorectal cancer (CRC) is a leading cause of cancer death globally and new biomarkers and treatments are severely needed. METHODS: Here, we employed HCT116 and LoVo human CRC cells made resistant to either SN38 or oxaliplatin, to investigate whether altered expression of the high affinity glutamate transporters Solute Carrier (SLC)-1A1 and -1A3 (EAAT3, EAAT1) is associated with the resistant phenotypes. Analyses included real-time quantitative PCR, immunoblotting and immunofluorescence analyses, radioactive tracer flux measurements, and biochemical analyses of cell viability and glutathione content. Results were evaluated using one- and two-way ANOVA and Students two-tailed t-test, as relevant. RESULTS: In SN38-resistant HCT116 and LoVo cells, SLC1A1 expression was down-regulated ~60 % and up-regulated ~4-fold, respectively, at both mRNA and protein level, whereas SLC1A3 protein was undetectable. The changes in SLC1A1 expression were accompanied by parallel changes in DL-Threo-β-Benzyloxyaspartic acid (TBOA)-sensitive, UCPH101-insensitive [(3)H]-D-Aspartate uptake, consistent with increased activity of SLC1A1 (or other family members), yet not of SLC1A3. DL-TBOA co-treatment concentration-dependently augmented loss of cell viability induced by SN38, while strongly counteracting that induced by oxaliplatin, in both HCT116 and LoVo cells. This reflected neither altered expression of the oxaliplatin transporter Cu(2+)-transporter-1 (CTR1), nor changes in cellular reduced glutathione (GSH), although HCT116 cell resistance per se correlated with increased cellular GSH. DL-TBOA did not significantly alter cellular levels of p21, cleaved PARP-1, or phospho-Retinoblastoma protein, yet altered SLC1A1 subcellular localization, and reduced chemotherapy-induced p53 induction. CONCLUSIONS: SLC1A1 expression and glutamate transporter activity are altered in SN38-resistant CRC cells. Importantly, the non-selective glutamate transporter inhibitor DL-TBOA reduces chemotherapy-induced p53 induction and augments CRC cell death induced by SN38, while attenuating that induced by oxaliplatin. These findings may point to novel treatment options in treatment-resistant CRC. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12885-015-1405-8) contains supplementary material, which is available to authorized users.
format Online
Article
Text
id pubmed-4445981
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-44459812015-05-28 The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells Pedraz-Cuesta, Elena Christensen, Sandra Jensen, Anders A. Jensen, Niels Frank Bunch, Lennart Romer, Maria Unni Brünner, Nils Stenvang, Jan Pedersen, Stine Falsig BMC Cancer Research Article BACKGROUND: Colorectal cancer (CRC) is a leading cause of cancer death globally and new biomarkers and treatments are severely needed. METHODS: Here, we employed HCT116 and LoVo human CRC cells made resistant to either SN38 or oxaliplatin, to investigate whether altered expression of the high affinity glutamate transporters Solute Carrier (SLC)-1A1 and -1A3 (EAAT3, EAAT1) is associated with the resistant phenotypes. Analyses included real-time quantitative PCR, immunoblotting and immunofluorescence analyses, radioactive tracer flux measurements, and biochemical analyses of cell viability and glutathione content. Results were evaluated using one- and two-way ANOVA and Students two-tailed t-test, as relevant. RESULTS: In SN38-resistant HCT116 and LoVo cells, SLC1A1 expression was down-regulated ~60 % and up-regulated ~4-fold, respectively, at both mRNA and protein level, whereas SLC1A3 protein was undetectable. The changes in SLC1A1 expression were accompanied by parallel changes in DL-Threo-β-Benzyloxyaspartic acid (TBOA)-sensitive, UCPH101-insensitive [(3)H]-D-Aspartate uptake, consistent with increased activity of SLC1A1 (or other family members), yet not of SLC1A3. DL-TBOA co-treatment concentration-dependently augmented loss of cell viability induced by SN38, while strongly counteracting that induced by oxaliplatin, in both HCT116 and LoVo cells. This reflected neither altered expression of the oxaliplatin transporter Cu(2+)-transporter-1 (CTR1), nor changes in cellular reduced glutathione (GSH), although HCT116 cell resistance per se correlated with increased cellular GSH. DL-TBOA did not significantly alter cellular levels of p21, cleaved PARP-1, or phospho-Retinoblastoma protein, yet altered SLC1A1 subcellular localization, and reduced chemotherapy-induced p53 induction. CONCLUSIONS: SLC1A1 expression and glutamate transporter activity are altered in SN38-resistant CRC cells. Importantly, the non-selective glutamate transporter inhibitor DL-TBOA reduces chemotherapy-induced p53 induction and augments CRC cell death induced by SN38, while attenuating that induced by oxaliplatin. These findings may point to novel treatment options in treatment-resistant CRC. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12885-015-1405-8) contains supplementary material, which is available to authorized users. BioMed Central 2015-05-16 /pmc/articles/PMC4445981/ /pubmed/25981639 http://dx.doi.org/10.1186/s12885-015-1405-8 Text en © Pedraz-Cuesta et al.; licensee BioMed Central. 2015 This article is published under license to BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research Article
Pedraz-Cuesta, Elena
Christensen, Sandra
Jensen, Anders A.
Jensen, Niels Frank
Bunch, Lennart
Romer, Maria Unni
Brünner, Nils
Stenvang, Jan
Pedersen, Stine Falsig
The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells
title The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells
title_full The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells
title_fullStr The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells
title_full_unstemmed The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells
title_short The glutamate transport inhibitor DL-Threo-β-Benzyloxyaspartic acid (DL-TBOA) differentially affects SN38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells
title_sort glutamate transport inhibitor dl-threo-β-benzyloxyaspartic acid (dl-tboa) differentially affects sn38- and oxaliplatin-induced death of drug-resistant colorectal cancer cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4445981/
https://www.ncbi.nlm.nih.gov/pubmed/25981639
http://dx.doi.org/10.1186/s12885-015-1405-8
work_keys_str_mv AT pedrazcuestaelena theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT christensensandra theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT jensenandersa theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT jensennielsfrank theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT bunchlennart theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT romermariaunni theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT brunnernils theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT stenvangjan theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT pedersenstinefalsig theglutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT pedrazcuestaelena glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT christensensandra glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT jensenandersa glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT jensennielsfrank glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT bunchlennart glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT romermariaunni glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT brunnernils glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT stenvangjan glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells
AT pedersenstinefalsig glutamatetransportinhibitordlthreobbenzyloxyasparticaciddltboadifferentiallyaffectssn38andoxaliplatininduceddeathofdrugresistantcolorectalcancercells

Ejemplares similares