Functional and transcriptomic characterization of carboplatin-resistant A2780 ovarian cancer cell line

Viscarra, Tamara; Buchegger, Kurt; Jofre, Ignacio; Riquelme, Ismael; Zanella, Louise; Abanto, Michel; Parker, Alyssa C; Piccolo, Stephen R; Roa, Juan Carlos; Ili, Carmen; Brebi, Priscilla

Viscarra, Tamara; Buchegger, Kurt; Jofre, Ignacio; Riquelme, Ismael; Zanella, Louise; Abanto, Michel; Parker, Alyssa C; Piccolo, Stephen R; Roa, Juan Carlos; Ili, Carmen; Brebi, Priscilla.

Viscarra, Tamara; Universidad de La Frontera. Centro de Excelencia en Medicina Traslacional-Scientific and Technological Bioresource Nucleus (CEMT-BIOREN). Laboratorio de Patología Molecular. Temuco. CL
Buchegger, Kurt; Universidad de La Frontera. Centro de Excelencia en Medicina Traslacional-Scientific and Technological Bioresource Nucleus (CEMT-BIOREN). Laboratorio de Patología Molecular. Temuco. CL
Jofre, Ignacio; Universidad de La Frontera. Faculty of Medicine. Department of Preclinical Sciences. Temuco. CL
Riquelme, Ismael; Universidad Autónoma de Chile. Facultad de Ciencias de la Salud. Instituto de Ciencias Biomédicas. Temuco. CL
Zanella, Louise; Universidad de La Frontera. Centro de Excelencia en Medicina Traslacional-Scientific and Technological Bioresource Nucleus (CEMT-BIOREN). Laboratorio de Patología Molecular. Temuco. CL
Abanto, Michel; Universidad de La Frontera. Temuco. CL
Parker, Alyssa C; Brigham Young University. Department of Biology. Provo. US
Piccolo, Stephen R; Brigham Young University. Department of Biology. Provo. US
Roa, Juan Carlos; Pontificia Universidad Católica de Chile. The Millennium Institute on Immunology and Immunotherapy. Advanced Centre for Chronic Diseases. CL
Ili, Carmen; Universidad de La Frontera. Centro de Excelencia en Medicina Traslacional-Scientific and Technological Bioresource Nucleus (CEMT-BIOREN). Laboratorio de Patología Molecular. Temuco. CL
Brebi, Priscilla; Universidad de La Frontera. Centro de Excelencia en Medicina Traslacional-Scientific and Technological Bioresource Nucleus (CEMT-BIOREN). Laboratorio de Patología Molecular. Temuco. CL

Biol. Res ; 52: 13, 2019. graf

Article in English | LILACS | ID: biblio-1011415

ABSTRACT

ABSTRACT

BACKGROUND:

Ovarian cancer is a significant cancer-related cause of death in women worldwide. The most used chemotherapeutic regimen is based on carboplatin (CBDCA). However, CBDCA resistance is the main obstacle to a better prognosis. An in vitro drug-resistant cell model would help in the understanding of molecular mechanisms underlying this drug-resistance phenomenon. The aim of this study was to characterize cellular and molecular changes of induced CBDCA-resistant ovarian cancer cell line A2780.

METHODS:

The cell selection strategy used in this study was a dose-per-pulse method using a concentration of 100 µM for 2 h. Once 20 cycles of exposure to the drug were completed, the cell cultures showed a resistant phenotype. Then, the ovarian cancer cell line A2780 was grown with 100 µM of CBDCA (CBDCA-resistant cells) or without CBDCA (parental cells). After, a drug sensitivity assay, morphological analyses, cell death assays and a RNA-seq analysis were performed in CBDCA-resistant A2780 cells.

RESULTS:

Microscopy on both parental and CBDCA-resistant A2780 cells showed similar characteristics in morphology and F-actin distribution within cells. In cell-death assays, parental A2780 cells showed a significant increase in phosphatidylserine translocation and caspase-3/7 cleavage compared to CBDCA-resistant A2780 cells (P < 0.05 and P < 0.005, respectively). Cell viability in parental A2780 cells was significantly decreased compared to CBDCA-resistant A2780 cells (P < 0.0005). The RNA-seq analysis showed 156 differentially expressed genes (DEGs) associated mainly to molecular functions.

CONCLUSION:

CBDCA-resistant A2780 ovarian cancer cells is a reliable model of CBDCA resistance that shows several DEGs involved in molecular functions such as transmembrane activity, protein binding to cell surface receptor and catalytic activity. Also, we found that the Wnt/3-catenin and integrin signaling pathway are the main metabolic pathway dysregulated in CBDCA-resistant A2780 cells.

Subject(s)

Humans; Female; Ovarian Neoplasms/genetics; Gene Expression Regulation, Neoplastic/drug effects; Carboplatin/pharmacology; Drug Resistance, Neoplasm/genetics; Transcriptome/drug effects; Antineoplastic Agents/pharmacology; Ovarian Neoplasms/pathology; Ovarian Neoplasms/drug therapy; Phenotype; Signal Transduction; Cell Death/drug effects; Cell Death/genetics; Sequence Analysis, RNA; Cell Line, Tumor; Transcriptome/genetics

A2780 cell line; Carboplatin; Drug resistance; Integrin signaling pathway; Ovarian cancer; Wnt/ß-catenin-signaling pathway

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Full text: Available Index: LILACS (Americas) Main subject: Ovarian Neoplasms / Gene Expression Regulation, Neoplastic / Carboplatin / Drug Resistance, Neoplasm / Transcriptome / Antineoplastic Agents Type of study: Prognostic study Limits: Female / Humans Language: English Journal: Biol. Res Journal subject: Biology Year: 2019 Type: Article Affiliation country: Chile / United States Institution/Affiliation country: Brigham Young University/US / Pontificia Universidad Católica de Chile/CL / Universidad Autónoma de Chile/CL / Universidad de La Frontera/CL

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