Increased levels of XPA might be the basis of cisplatin resistance in germ cell tumours

Zuzana Cierna; Vera Miskovska; Jan Roska; Dana Jurkovicova; Lucia Borszekova Pulzova; Zuzana Sestakova; Lenka Hurbanova; Katarina Machalekova; Michal Chovanec; Katarina Rejlekova; Daniela Svetlovska; Katarina Kalavska; Karol Kajo; Pavel Babal; Jozef Mardiak; Thomas A. Ward; Michal Mego; Miroslav Chovanec

doi:10.1186/s12885-019-6496-1

BMC Cancer (Jan 2020)

Increased levels of XPA might be the basis of cisplatin resistance in germ cell tumours

Zuzana Cierna,
Vera Miskovska,
Jan Roska,
Dana Jurkovicova,
Lucia Borszekova Pulzova,
Zuzana Sestakova,
Lenka Hurbanova,
Katarina Machalekova,
Michal Chovanec,
Katarina Rejlekova,
Daniela Svetlovska,
Katarina Kalavska,
Karol Kajo,
Pavel Babal,
Jozef Mardiak,
Thomas A. Ward,
Michal Mego,
Miroslav Chovanec

Affiliations

Zuzana Cierna: Department of Pathology, Faculty of Medicine, Comenius University
Vera Miskovska: 1st Department of Oncology, Faculty of Medicine, Comenius University
Jan Roska: Department of Genetics, Cancer Research Institute, Biomedical Research Center, University Science Park for Biomedicine, Slovak Academy of Sciences
Dana Jurkovicova: Department of Genetics, Cancer Research Institute, Biomedical Research Center, University Science Park for Biomedicine, Slovak Academy of Sciences
Lucia Borszekova Pulzova: Department of Genetics, Cancer Research Institute, Biomedical Research Center, University Science Park for Biomedicine, Slovak Academy of Sciences
Zuzana Sestakova: Department of Genetics, Cancer Research Institute, Biomedical Research Center, University Science Park for Biomedicine, Slovak Academy of Sciences
Lenka Hurbanova: Department of Genetics, Cancer Research Institute, Biomedical Research Center, University Science Park for Biomedicine, Slovak Academy of Sciences
Katarina Machalekova: St. Elisabeth Cancer Institute
Michal Chovanec: 2nd Department of Oncology, Faculty of Medicine, Comenius University
Katarina Rejlekova: St. Elisabeth Cancer Institute
Daniela Svetlovska: St. Elisabeth Cancer Institute
Katarina Kalavska: St. Elisabeth Cancer Institute
Karol Kajo: St. Elisabeth Cancer Institute
Pavel Babal: Department of Pathology, Faculty of Medicine, Comenius University
Jozef Mardiak: St. Elisabeth Cancer Institute
Thomas A. Ward: Department of Biomedical and Life Sciences, Faculty of Health and Medicine, Lancaster University
Michal Mego: Department of Genetics, Cancer Research Institute, Biomedical Research Center, University Science Park for Biomedicine, Slovak Academy of Sciences
Miroslav Chovanec: Department of Genetics, Cancer Research Institute, Biomedical Research Center, University Science Park for Biomedicine, Slovak Academy of Sciences

DOI: https://doi.org/10.1186/s12885-019-6496-1
Journal volume & issue: Vol. 20, no. 1
pp. 1 – 12

Abstract

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Abstract Background Germ cell tumours (GCTs) represent a highly curable malignity as they respond well to cisplatin (CDDP)-based chemotherapy. Nevertheless, a small proportion of GCT patients relapse or do not respond to therapy. As this might be caused by an increased capacity to repair CDDP-induced DNA damage, identification of DNA repair biomarkers predicting inadequate or aberrant response to CDDP, and thus poor prognosis for GCT patients, poses a challenge. The objective of this study is to examine the expression levels of the key nucleotide excision repair (NER) factors, XPA, ERCC1 and XPF, in GCT patients and cell lines. Methods Two hundred seven GCT patients’ specimens with sufficient follow-up clinical-pathological data and pairwise combinations of CDDP-resistant and -sensitive GCT cell lines were included. Immunohistochemistry was used to detect the ERCC1, XPF and XPA protein expression levels in GCT patients’ specimen and Western blot and qRT-PCR examined the protein and mRNA expression levels in GCT cell lines. Results GCT patients with low XPA expression had significantly better overall survival than patients with high expression (hazard ratio = 0.38, 95% confidence interval: 0.12–1.23, p = 0.0228). In addition, XPA expression was increased in the non-seminomatous histological subtype, IGCCCG poor prognosis group, increasing S stage, as well as the presence of lung, liver and non-pulmonary visceral metastases. Importantly, a correlation between inadequate or aberrant CDDP response and XPA expression found in GCT patients was also seen in GCT cell lines. Conclusions XPA expression is an additional independent prognostic biomarker for stratifying GCT patients, allowing for improvements in decision-making on treatment for those at high risk of refractoriness or relapse. In addition, it could represent a novel therapeutic target in GCTs.

Published in BMC Cancer

ISSN: 1471-2407 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: http://bmccancer.biomedcentral.com

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