Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements

BACKGROUND: Endoretroviruses account for circa 8 % of all transposable elements found in the genome of humans and other animals. They represent a genetic footprint of ancestral germ-cell infections of exoviruses that is transmittable to the progeny by Mendelian segregation. Traces of human endogenou...

Descripción completa

Detalles Bibliográficos
Autores principales: Díaz-Carballo, David, Acikelli, Ali Haydar, Klein, Jacqueline, Jastrow, Holger, Dammann, Philipp, Wyganowski, Thomas, Guemues, Cihan, Gustmann, Sebastian, Bardenheuer, Walter, Malak, Sascha, Tefett, Nora Sophia, Khosrawipour, Veria, Giger-Pabst, Urs, Tannapfel, Andrea, Strumberg, Dirk
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2015
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4542094/
https://www.ncbi.nlm.nih.gov/pubmed/26260344
http://dx.doi.org/10.1186/s13046-015-0199-5
_version_ 1782386483972276224
author Díaz-Carballo, David
Acikelli, Ali Haydar
Klein, Jacqueline
Jastrow, Holger
Dammann, Philipp
Wyganowski, Thomas
Guemues, Cihan
Gustmann, Sebastian
Bardenheuer, Walter
Malak, Sascha
Tefett, Nora Sophia
Khosrawipour, Veria
Giger-Pabst, Urs
Tannapfel, Andrea
Strumberg, Dirk
author_facet Díaz-Carballo, David
Acikelli, Ali Haydar
Klein, Jacqueline
Jastrow, Holger
Dammann, Philipp
Wyganowski, Thomas
Guemues, Cihan
Gustmann, Sebastian
Bardenheuer, Walter
Malak, Sascha
Tefett, Nora Sophia
Khosrawipour, Veria
Giger-Pabst, Urs
Tannapfel, Andrea
Strumberg, Dirk
author_sort Díaz-Carballo, David
collection PubMed
description BACKGROUND: Endoretroviruses account for circa 8 % of all transposable elements found in the genome of humans and other animals. They represent a genetic footprint of ancestral germ-cell infections of exoviruses that is transmittable to the progeny by Mendelian segregation. Traces of human endogenous retroviruses are physiologically expressed in ovarial, testicular and placental tissues as well as in stem cells. In addition, a number of these fossil viral elements have also been related to carcinogenesis. However, a relation between endoretroviruses expression and chemoresistance has not been reported yet. METHODS: Twenty colorectal carcinoma patient samples were scrutinized for HERV-W(E1) and HERV-FRD(1) endoretroviruses using immunohistochemical approaches. In order to search for differential expression of these elements in chemotherapy refractory cells, a resistant HCT8 colon carcinoma subline was developed by serial etoposide exposure. Endoretroviral elements were detected by immunocytochemical staining, qPCR and ELISA. IC(50)-values of antiviral and cytostatic drugs in HCT8 cells were determined by MTT proliferation assay. The antivirals-cytostatics interaction was evaluated by the isobologram method. RESULTS: In this work, we show for the first time that HERV-W(E1), HERV-FRD(1), HERV-3(1), and HERV-V(1) are a) simultaneously expressed in treatment-naïve colon carcinoma cells and b) upregulated after cytostatic exposure, suggesting that these retroviral elements are intimately related to chemotherapy resistance. We found a number of antiviral drugs to have cytotoxic activity and the ability to force the downregulation of HERV proteins in vitro. We also demonstrate that the use of different antiviral compounds alone or in combination with anticancer agents results in a synergistic antiproliferative effect and downregulation of different endoretroviral elements in highly chemotherapy-resistant colorectal tumor cells. CONCLUSIONS: Enhanced HERV-expression is associated with chemoresistance in colon carcinomas which can be overcome by antiviral drugs alone or in combination with anticancer drugs. Therefore, the introduction of antiviral compounds to the current chemotherapy regimens potentially improves patient outcomes. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13046-015-0199-5) contains supplementary material, which is available to authorized users.
format Online
Article
Text
id pubmed-4542094
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-45420942015-08-21 Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements Díaz-Carballo, David Acikelli, Ali Haydar Klein, Jacqueline Jastrow, Holger Dammann, Philipp Wyganowski, Thomas Guemues, Cihan Gustmann, Sebastian Bardenheuer, Walter Malak, Sascha Tefett, Nora Sophia Khosrawipour, Veria Giger-Pabst, Urs Tannapfel, Andrea Strumberg, Dirk J Exp Clin Cancer Res Research BACKGROUND: Endoretroviruses account for circa 8 % of all transposable elements found in the genome of humans and other animals. They represent a genetic footprint of ancestral germ-cell infections of exoviruses that is transmittable to the progeny by Mendelian segregation. Traces of human endogenous retroviruses are physiologically expressed in ovarial, testicular and placental tissues as well as in stem cells. In addition, a number of these fossil viral elements have also been related to carcinogenesis. However, a relation between endoretroviruses expression and chemoresistance has not been reported yet. METHODS: Twenty colorectal carcinoma patient samples were scrutinized for HERV-W(E1) and HERV-FRD(1) endoretroviruses using immunohistochemical approaches. In order to search for differential expression of these elements in chemotherapy refractory cells, a resistant HCT8 colon carcinoma subline was developed by serial etoposide exposure. Endoretroviral elements were detected by immunocytochemical staining, qPCR and ELISA. IC(50)-values of antiviral and cytostatic drugs in HCT8 cells were determined by MTT proliferation assay. The antivirals-cytostatics interaction was evaluated by the isobologram method. RESULTS: In this work, we show for the first time that HERV-W(E1), HERV-FRD(1), HERV-3(1), and HERV-V(1) are a) simultaneously expressed in treatment-naïve colon carcinoma cells and b) upregulated after cytostatic exposure, suggesting that these retroviral elements are intimately related to chemotherapy resistance. We found a number of antiviral drugs to have cytotoxic activity and the ability to force the downregulation of HERV proteins in vitro. We also demonstrate that the use of different antiviral compounds alone or in combination with anticancer agents results in a synergistic antiproliferative effect and downregulation of different endoretroviral elements in highly chemotherapy-resistant colorectal tumor cells. CONCLUSIONS: Enhanced HERV-expression is associated with chemoresistance in colon carcinomas which can be overcome by antiviral drugs alone or in combination with anticancer drugs. Therefore, the introduction of antiviral compounds to the current chemotherapy regimens potentially improves patient outcomes. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13046-015-0199-5) contains supplementary material, which is available to authorized users. BioMed Central 2015-08-12 /pmc/articles/PMC4542094/ /pubmed/26260344 http://dx.doi.org/10.1186/s13046-015-0199-5 Text en © Díaz-Carballo et al. 2015 Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/ (http://creativecommons.org/licenses/by/4.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. 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
Díaz-Carballo, David
Acikelli, Ali Haydar
Klein, Jacqueline
Jastrow, Holger
Dammann, Philipp
Wyganowski, Thomas
Guemues, Cihan
Gustmann, Sebastian
Bardenheuer, Walter
Malak, Sascha
Tefett, Nora Sophia
Khosrawipour, Veria
Giger-Pabst, Urs
Tannapfel, Andrea
Strumberg, Dirk
Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements
title Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements
title_full Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements
title_fullStr Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements
title_full_unstemmed Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements
title_short Therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements
title_sort therapeutic potential of antiviral drugs targeting chemorefractory colorectal adenocarcinoma cells overexpressing endogenous retroviral elements
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4542094/
https://www.ncbi.nlm.nih.gov/pubmed/26260344
http://dx.doi.org/10.1186/s13046-015-0199-5
work_keys_str_mv AT diazcarballodavid therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT acikellialihaydar therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT kleinjacqueline therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT jastrowholger therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT dammannphilipp therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT wyganowskithomas therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT guemuescihan therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT gustmannsebastian therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT bardenheuerwalter therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT malaksascha therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT tefettnorasophia therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT khosrawipourveria therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT gigerpabsturs therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT tannapfelandrea therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements
AT strumbergdirk therapeuticpotentialofantiviraldrugstargetingchemorefractorycolorectaladenocarcinomacellsoverexpressingendogenousretroviralelements

Ejemplares similares