Integrated Genome-Wide DNA Copy Number and Expression Analysis Identifies Distinct Mechanisms of Primary Chemoresistance in Ovarian Carcinomas

Etemadmoghadam, Dariush; deFazio, Anna; Beroukhim, Rameen; Mermel, Craig H.; George, Joshy; Getz, Gad; Tothill, Richard W.; Okamoto, Aikou; Ræder, Maria B.; Harnett, Paul; Lade, Stephen; Akslen, Lars A.; Tinker, Anna V.; Locandro, Bianca; Alsop, Kathryn; Chiew, Yoke-Eng; Traficante, Nadia; Fereday, Sián; Johnson, Daryl; Fox, Stephen B.; Sellers, William R.; Urashima, Mitsuyoshi; Salvesen, Helga B.; Meyerson, Matthew; Bowtell, David D.L.

doi:10.1158/1078-0432.ccr-08-1564

Cited by 257 publications

(259 citation statements)

References 49 publications

(74 reference statements)

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“…Our recent results indicate that Dex could enhance cell adhesion by increasing the expression of some ECM components, such as collagen I and hyaluronic acid, in . This finding is in line with the latest report that the enhanced ECM deposition may play a direct role in primary chemoresistance in ovarian carcinoma (Etemadmoghadam et al 2009). …”

Section: Discussionsupporting

confidence: 92%

Dexamethasone enhances cell resistance to chemotherapy by increasing adhesion to extracellular matrix in human ovarian cancer cells

Chen¹,

Wang²,

Fu³

et al. 2010

Endocrine-Related Cancer

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Glucocorticoids (GCs) are widely used as co-medication in the therapy of solid malignant tumors to relieve some of the side effects of chemotherapeutic drugs. However, recent studies have shown that GCs could render cancer cells more resistant to cytotoxic drug-induced apoptosis, but the mechanism is largely unknown. In the present study, we found that the treatment of human ovarian cancer cell lines HO-8910 and SKOV3 with synthetic GCs dexamethasone (Dex) significantly increased their adhesion to extracellular matrix (ECM) and their resistance to apoptosis induced by cytotoxic drugs cisplatin and paclitaxel. Dex also increased the protein levels of adhesion molecules integrins b1, a4, and a5 in HO-8910 cells. The neutralizing antibody against integrin b1 prevented Dex-induced adhesion and significantly abrogated the protective effect of Dex toward cytotoxic agents. We further found that transforming growth factor-b1 (TGF-b1) alone not only increased cell adhesion and cell survival of HO-8910 cells in the presence of cisplatin, but also had synergistic pro-adhesion and pro-survival effects with Dex. Moreover, TGF-b1-neutralizing antibody that could block TGF-b1-induced cell adhesion and apoptosis resistance markedly abrogated the synergistic pro-adhesion and pro-survival effects of Dex and TGF-b1. Finally, we further demonstrated that Dex could up-regulate the expression of TGF-b receptor type II and enhance the responsiveness of cells to TGF-b1. In conclusion, our results indicate that increased adhesion to ECM through the enhancement of integrin b1 signaling and TGF-b1 signaling plays an important role in chemoresistance induced by GCs in ovarian cancer cells.

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Section: Discussionsupporting

confidence: 92%

Dexamethasone enhances cell resistance to chemotherapy by increasing adhesion to extracellular matrix in human ovarian cancer cells

Chen¹,

Wang²,

Fu³

et al. 2010

Endocrine-Related Cancer

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“…2-7 Several studies on gene profiling of the primary tumor using microarray technology have described potential genes/pathways contributing to chemotherapy resistance and their association with risk stratification/overall survival. [8][9][10][11][12][13][14][15][16][17][18] Unlike the clinical impact of gene profiling on treatment decisions for several solid tumors there has been limited progress with the prediction or the clinical management of recurrent HGSOC.Studies with recurrent ovarian tumors 19 have described surgical and second-line chemotherapy options for the clinical management of the disease. Chromosomal aberrations associated with risk for recurrence have been identified by using comparative genomic hybridization (CGH) analysis.…”

mentioning

confidence: 99%

Expression profile of COL2A1 and the pseudogene SLC6A10P predicts tumor recurrence in high‐grade serous ovarian cancer

Ganapathi

Jones

Sehouli

et al. 2015

Intl Journal of Cancer

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Tumor recurrence, following initial response to adjuvant chemotherapy, is a major problem in women with high-grade serous ovarian cancer (HGSOC). Microarray analysis of primary tumors has identified genes that may be useful in risk stratification/overall survival, but are of limited value in predicting the >70% rate for tumor recurrence. In this study, we performed RNA-Seq analysis of primary and recurrent HGSOC to first identify unique differentially expressed genes. From this dataset, we selected 21 archetypical coding genes and one noncoding RNA, based on statistically significant differences in their expression profile between tumors, for validation by qPCR in a larger cohort of 110 ovarian tumors (71 primary and 39 recurrent) and for testing association of specific genes with time-to-recurrence (TTR). Kaplan-Meier tests revealed that high expression of collagen type II, alpha 1 (COL2A1) was associated with delayed TTR (HR 5 0.47, 95% CI: 0.27-0.82, p 5 0.008), whereas low expression of the pseudogene, solute carrier family 6 member 10 (SLC6A10P), was associated with longer TTR (HR 5 0.53, 95% CI: 0.30-0.93, p 5 0.027). Notably, TTR was significantly delayed for tumors that simultaneously highly expressed COL2A1 and lowly expressed SLC6A10P (HR 5 0.21, 95% CI: 0.082-0.54, p 5 0.0011), an estimated median of 95 months as compared to an estimated median of 16 months for subjects expressing other levels of COL2A1 and SLC6A10P. Thus, evaluating expression levels of COL2A1 and SLC6A10P at primary surgery could be beneficial for clinically managing recurrence of HGSOC.Deaths from all gynecological malignancies are about 30% but mortality for ovarian cancer is disproportionately high approaching 65%. Epithelial ovarian cancer is a heterogeneous disease with histological subtypes that differ in tissue of origin, genetic profile and outcome.1 High-grade serous ovarian cancer (HGSOC) is the most common subtype and >70% of women are diagnosed at an advanced stage of the disease owing to the lack of reliable early detection tests. Notwithstanding this problem, the standard of care involving tumor debulking surgery followed by adjuvant platinum/taxane-based chemotherapy can lead to a favorable response in 80% of the patients, but unfortunately the rate for recurrence is >70%. While resistance to the primary adjuvant chemotherapy regimen can contribute significantly to early tumor recurrence (<6 months), there is limited information on the mechanisms or genes that could predict for late recurrence. Genomic analysis of serous ovarian cancer has been useful for distinguishing low malignant potential, low-grade and high-grade tumors and these efforts have led to identification of molecular subtypes that can be linked to outcome. 2-7 Several studies on gene profiling of the primary tumor using microarray technology have described potential genes/pathways contributing to chemotherapy resistance and their association with risk stratification/overall survival. [8][9][10][11][12][13][14][15][16][17][18] Unlike the clinical impact...

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“…The association between cyclin E amplification and poor outcome has also been identified in recent German and Japanese studies, although the correlation was not statistically significant in the latter (Mayr et al 2006, Nakayama et al 2010. Two independent labs have also suggested that amplification of the cyclin E gene was associated with primary treatment resistance and targeting cyclin E expression with siRNA reduced cell viability and increased apoptosis (Etemadmoghadam et al 2009, Nakayama et al 2010. These studies suggest that cyclin E amplification/expression may serve as both a prognostic and predictive factor in ovarian cancer as well as a therapeutic target in the treatment of ovarian cancer.…”

Section: Cell Cycle Regulatory Proteinsmentioning

confidence: 77%

Gene Amplification in Ovarian Carcinomas: Lessons from Selected Amplified Gene Families

Gaillard¹

2012

Ovarian Cancer - Basic Science Perspective

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Integrated Genome-Wide DNA Copy Number and Expression Analysis Identifies Distinct Mechanisms of Primary Chemoresistance in Ovarian Carcinomas

Cited by 257 publications

References 49 publications

Dexamethasone enhances cell resistance to chemotherapy by increasing adhesion to extracellular matrix in human ovarian cancer cells

Dexamethasone enhances cell resistance to chemotherapy by increasing adhesion to extracellular matrix in human ovarian cancer cells

Expression profile of COL2A1 and the pseudogene SLC6A10P predicts tumor recurrence in high‐grade serous ovarian cancer

Gene Amplification in Ovarian Carcinomas: Lessons from Selected Amplified Gene Families

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