Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study

The introduction of microarray techniques to cancer research brought great expectations for finding biomarkers that would improve patients’ treatment; however, the results of such studies are poorly reproducible and critical analyses of these methods are rare. In this study, we examined global gene...

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Autores principales: Lisowska, Katarzyna Marta, Olbryt, Magdalena, Dudaladava, Volha, Pamuła-Piłat, Jolanta, Kujawa, Katarzyna, Grzybowska, Ewa, Jarząb, Michał, Student, Sebastian, Rzepecka, Iwona Krystyna, Jarząb, Barbara, Kupryjańczyk, Jolanta
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2014
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3904181/
https://www.ncbi.nlm.nih.gov/pubmed/24478986
http://dx.doi.org/10.3389/fonc.2014.00006
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author Lisowska, Katarzyna Marta
Olbryt, Magdalena
Dudaladava, Volha
Pamuła-Piłat, Jolanta
Kujawa, Katarzyna
Grzybowska, Ewa
Jarząb, Michał
Student, Sebastian
Rzepecka, Iwona Krystyna
Jarząb, Barbara
Kupryjańczyk, Jolanta
author_facet Lisowska, Katarzyna Marta
Olbryt, Magdalena
Dudaladava, Volha
Pamuła-Piłat, Jolanta
Kujawa, Katarzyna
Grzybowska, Ewa
Jarząb, Michał
Student, Sebastian
Rzepecka, Iwona Krystyna
Jarząb, Barbara
Kupryjańczyk, Jolanta
author_sort Lisowska, Katarzyna Marta
collection PubMed
description The introduction of microarray techniques to cancer research brought great expectations for finding biomarkers that would improve patients’ treatment; however, the results of such studies are poorly reproducible and critical analyses of these methods are rare. In this study, we examined global gene expression in 97 ovarian cancer samples. Also, validation of results by quantitative RT-PCR was performed on 30 additional ovarian cancer samples. We carried out a number of systematic analyses in relation to several defined clinicopathological features. The main goal of our study was to delineate the molecular background of ovarian cancer chemoresistance and find biomarkers suitable for prediction of patients’ prognosis. We found that histological tumor type was the major source of variability in genes expression, except for serous and undifferentiated tumors that showed nearly identical profiles. Analysis of clinical endpoints [tumor response to chemotherapy, overall survival, disease-free survival (DFS)] brought results that were not confirmed by validation either on the same group or on the independent group of patients. CLASP1 was the only gene that was found to be important for DFS in the independent group, whereas in the preceding experiments it showed associations with other clinical endpoints and with BRCA1 gene mutation; thus, it may be worthy of further testing. Our results confirm that histological tumor type may be a strong confounding factor and we conclude that gene expression studies of ovarian carcinomas should be performed on histologically homogeneous groups. Among the reasons of poor reproducibility of statistical results may be the fact that despite relatively large patients’ group, in some analyses one has to compare small and unequal classes of samples. In addition, arbitrarily performed division of samples into classes compared may not always reflect their true biological diversity. And finally, we think that clinical endpoints of the tumor probably depend on subtle changes in many and, possibly, alternative molecular pathways, and such changes may be difficult to demonstrate.
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spelling pubmed-39041812014-01-29 Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study Lisowska, Katarzyna Marta Olbryt, Magdalena Dudaladava, Volha Pamuła-Piłat, Jolanta Kujawa, Katarzyna Grzybowska, Ewa Jarząb, Michał Student, Sebastian Rzepecka, Iwona Krystyna Jarząb, Barbara Kupryjańczyk, Jolanta Front Oncol Oncology The introduction of microarray techniques to cancer research brought great expectations for finding biomarkers that would improve patients’ treatment; however, the results of such studies are poorly reproducible and critical analyses of these methods are rare. In this study, we examined global gene expression in 97 ovarian cancer samples. Also, validation of results by quantitative RT-PCR was performed on 30 additional ovarian cancer samples. We carried out a number of systematic analyses in relation to several defined clinicopathological features. The main goal of our study was to delineate the molecular background of ovarian cancer chemoresistance and find biomarkers suitable for prediction of patients’ prognosis. We found that histological tumor type was the major source of variability in genes expression, except for serous and undifferentiated tumors that showed nearly identical profiles. Analysis of clinical endpoints [tumor response to chemotherapy, overall survival, disease-free survival (DFS)] brought results that were not confirmed by validation either on the same group or on the independent group of patients. CLASP1 was the only gene that was found to be important for DFS in the independent group, whereas in the preceding experiments it showed associations with other clinical endpoints and with BRCA1 gene mutation; thus, it may be worthy of further testing. Our results confirm that histological tumor type may be a strong confounding factor and we conclude that gene expression studies of ovarian carcinomas should be performed on histologically homogeneous groups. Among the reasons of poor reproducibility of statistical results may be the fact that despite relatively large patients’ group, in some analyses one has to compare small and unequal classes of samples. In addition, arbitrarily performed division of samples into classes compared may not always reflect their true biological diversity. And finally, we think that clinical endpoints of the tumor probably depend on subtle changes in many and, possibly, alternative molecular pathways, and such changes may be difficult to demonstrate. Frontiers Media S.A. 2014-01-28 /pmc/articles/PMC3904181/ /pubmed/24478986 http://dx.doi.org/10.3389/fonc.2014.00006 Text en Copyright © 2014 Lisowska, Olbryt, Dudaladava, Pamuła-Piłat, Kujawa, Grzybowska, Jarząb, Student, Rzepecka, Jarząb and Kupryjańczyk. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Lisowska, Katarzyna Marta
Olbryt, Magdalena
Dudaladava, Volha
Pamuła-Piłat, Jolanta
Kujawa, Katarzyna
Grzybowska, Ewa
Jarząb, Michał
Student, Sebastian
Rzepecka, Iwona Krystyna
Jarząb, Barbara
Kupryjańczyk, Jolanta
Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study
title Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study
title_full Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study
title_fullStr Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study
title_full_unstemmed Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study
title_short Gene Expression Analysis in Ovarian Cancer – Faults and Hints from DNA Microarray Study
title_sort gene expression analysis in ovarian cancer – faults and hints from dna microarray study
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3904181/
https://www.ncbi.nlm.nih.gov/pubmed/24478986
http://dx.doi.org/10.3389/fonc.2014.00006
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