Transcriptional epigenetic regulation of Fkbp1/Pax9 genes is associated with impaired sensitivity to platinum treatment in ovarian cancer
Entidad
UAM. Departamento de Obstetricia y GinecologíaEditor
BioMed Central Ltd.Fecha de edición
2021-08-28Cita
10.1186/s13148-021-01149-8
Clinical Epigenetics 13 (2021): 167
ISSN
1868-7075 (print); 1868-7083 (online)DOI
10.1186/s13148-021-01149-8Financiado por
The study was financially supported by FIS (ISCIII) and ERDF/FSE funds (PI15/00186, PI18/0050, and ERDF/FSE, A way to make Europe). The authors gratefully acknowledge the Colombian Ministry for Science, Technology and Innovation (MINCIENCIAS), Code 568-2012, for providing J.S. with partial funding for this study.Proyecto
Gobierno de España. PI15/00186; Gobierno de España. PI18/0050Materias
FKBP1B; Methylation; Ovarian cancer; PAX9; Platinum; Predictive; Therapy; MedicinaDerechos
© The Author(s) 2021Resumen
Background: In an effort to contribute to overcoming the platinum resistance exhibited by most solid tumors, we performed an array of epigenetic approaches, integrating next-generation methodologies and public clinical data to identify new potential epi-biomarkers in ovarian cancer, which is considered the most devastating of gynecological malignancies. Methods: We cross-analyzed data from methylome assessments and restoration of gene expression through microarray expression in a panel of four paired cisplatin-sensitive/cisplatin-resistant ovarian cancer cell lines, along with publicly available clinical data from selected individuals representing the state of chemoresistance. We validated the methylation state and expression levels of candidate genes in each cellular phenotype through Sanger sequencing and reverse transcription polymerase chain reaction, respectively. We tested the biological role of selected targets using an ectopic expression plasmid assay in the sensitive/resistant tumor cell lines, assessing the cell viability in the transfected groups. Epigenetic features were also assessed in 189 primary samples obtained from ovarian tumors and controls. Results: We identified PAX9 and FKBP1B as potential candidate genes, which exhibited epigenetic patterns of expression regulation in the experimental approach. Re-establishment of FKBP1B expression in the resistant OVCAR3 phenotype in which this gene is hypermethylated and inhibited allowed it to achieve a degree of platinum sensitivity similar to the sensitive phenotype. The evaluation of these genes at a translational level revealed that PAX9 hypermethylation leads to a poorer prognosis in terms of overall survival. We also set a precedent for establishing a common epigenetic signature in which the validation of a single candidate, MEST, proved the accuracy of our computational pipelines. Conclusions: Epigenetic regulation of PAX9 and FKBP1B genes shows that methylation in non-promoter areas has the potential to control gene expression and thus biological consequences, such as the loss of platinum sensitivity. At the translational level, PAX9 behaves as a predictor of chemotherapy response to platinum in patients with ovarian cancer. This study revealed the importance of the transcript-specific study of each gene under potential epigenetic regulation, which would favor the identification of new markers capable of predicting each patient’s progression and therapeutic response.
Lista de ficheros
Google Scholar:Soto, Javier Andrés
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Rodríguez-Antolín, Carlos
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Vera, Olga
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Pernía, Olga
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Esteban-Rodríguez, Isabel
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Diestro Tejada, María Dolores
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Benitez, Javier
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Sánchez-Cabo, Fátima
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Alvarez, Rafael
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De Castro, Javier
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Ibanez de Cáceres, Inmaculada
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