Specific Mechanisms of Chromosomal Instability Indicate Therapeutic Sensitivities in High-Grade Serous Ovarian Carcinoma

Tamura, Naoka; Shaikh, Nadeem; Muliaditan, Daniel; Soliman, Tanya; McGuinness, Jennifer R.; Maniati, Eleni; Moralli, Daniela; Durin, Mary-Anne; Green, Catherine; Balkwill, Frances R.; Wang, Jun; Curtius, Kit; McClelland, Sarah E.

doi:10.1158/0008-5472.can-19-0852

Cited by 37 publications

(53 citation statements)

References 64 publications

(97 reference statements)

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“…AOCS1 was also established from a patient with HGSOC and kept at a low passage number. Both cell lines showed genetic changes characteristic of HGSOC (Tamura et al, 2020). The original tissue biopsies for both cell lines showed malignant cell PAX8 positivity and cell lines cultured in vitro maintained PAX8 nuclear positivity (Figure 3A).…”

Section: Malignant Cells Upregulate Tgfb3 and Heterogeneously Express Matrisome Moleculesmentioning

confidence: 95%

“…The G164 cell line was established in our laboratory from an omental HGSOC tumor collected during interval debulking surgery in 2015. G164 cells were TP53 and PAX8 positive (Tamura et al, 2020). Malignant cells were cultured in DMEM:F12 (Gibco), 10% FCS, 1% penicillin and streptomycin in a 5% CO2 humidified incubator at 37 C. The immortalized human FTSE cell line, wild-type FT318, was kindly given by Professor Ronny Drapkin (Perelman School of Medicine, University of Pennsylvania) and grown in serum-free WIT-P medium (Cellaria) without antibiotics and 100ng/ml cholera toxin (Sigma-Aldrich).…”

Section: Supplemental Informationmentioning

confidence: 98%

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Modelling TGFβR and Hh pathway regulation of prognostic matrisome molecules in ovarian cancer

et al. 2021

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In a multi-level ''deconstruction'' of omental metastases, we previously identified a prognostic matrisome gene expression signature in high-grade serous ovarian cancer (HGSOC) and twelve other malignancies. Here, our aim was to understand how six of these extracellular matrix (ECM) molecules, COL11A1, cartilage oligomeric matrix protein, FN1, versican, cathepsin B, and COL1A1, are upregulated in cancer. Using biopsies, we identified significant associations between TGFbR activity, Hedgehog (Hh) signaling, and these ECM molecules and studied the associations in mono-, co-, and tri-culture. Activated omental fibroblasts (OFs) produced more matrix than malignant cells, directed by TGFbR and Hh signaling cross talk. We ''reconstructed'' omental metastases in tri-cultures of HGSOC cells, OFs, and adipocytes. This combination was sufficient to generate all six ECM proteins and the matrisome expression signature. TGFbR and Hh inhibitor combinations attenuated fibroblast activation and gel and ECM remodeling in these models. The tri-culture model reproduces key features of omental metastases and allows study of diseased-associated ECM.

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Section: Malignant Cells Upregulate Tgfb3 and Heterogeneously Express Matrisome Moleculesmentioning

confidence: 95%

Section: Supplemental Informationmentioning

confidence: 98%

Modelling TGFβR and Hh pathway regulation of prognostic matrisome molecules in ovarian cancer

et al. 2021

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“…HGSOC is characterized by highly abnormal karyotypes along with other features of genomic instability including numerical and structural variants 32 – 35 . CIN has also be demonstrated in ovarian cancer cell lines and in ascites derived from patients with HGSOC and several underlying mechanisms have been suggested, including DNA replication stress and elevated microtubule dynamics 33 , 36 .…”

Section: Discussionmentioning

confidence: 99%

Effects of long-term norepinephrine treatment on normal immortalized ovarian and fallopian tube cells

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et al. 2021

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Sustained adrenergic stimulation by norepinephrine (NE) contributes to ovarian carcinoma metastasis and impairment of chemotherapy response. Although the effect of sustained NE stimulation in cancer progression is well established, less is known about its role in cancer initiation. To determine the extent to which stress hormones influence ovarian cancer initiation, we conducted a long-term (> 3 months; > 40 population doublings) experiment in which normal immortalized fallopian tube secretory (iFTSEC283) and ovarian surface epithelial (iOSE11) cell lines and their isogenic pairs containing a p53 mutation (iFTSEC283p53R175H; iOSE11p53R175H), were continuously exposed to NE (100 nM, 1 μM, 10 μM). Fallopian tube cells displayed a p53-independent increase in proliferation and colony-forming ability in response to NE, while ovarian surface epithelial cells displayed a p53-independent decrease in both assays. Fallopian tube cells with mutant p53 showed a mild loss of chromosomes and TP53 status was also a defining factor in transcriptional response of fallopian tube cells to long-term NE treatment.

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“…The medium was then replaced with 200 ml of mesothelial cell medium (Medium 199 (Gibco) with insulin-transferrin-selenium (Gibco), 10% heat-inactivated FBS (Hyclone) and penicillin-streptomycin (Sigma-Aldric)) containing 200,000 human primary mesothelial cells and incubated for 24 hr. G164 or AOCS1 ovarian cancer cells (Tamura et al, 2020) were then seeded at 40,000 cells per gel and incubated for 24 hr before loosening and transferring the gels to a 24 well dish in growth medium. To make up the penta-culture model, a ratio of 1:100 cancer cells:isolated platelets was added to the culture.…”

Section: Star+methodsmentioning

confidence: 99%

“…(H) Hierarchical cluster analysis of tetra-and penta-culture illustrates that both cluster more closely with historic HGSOC RNASeq (Pearce et al, 2018) Next we asked if we could use this cell model to study malignant cell invasion. We added HGSOC cell lines AOCS1 (Milagre et al, 2015) (Figure 1F) or G164 (Tamura et al, 2020) (Figure 1G) as a single cell suspension, creating an omental metastasis tetra-culture model. We found that both AOCS1 and G164 malignant cells attached to the surface of the cultures forming colonies (Figure 1G), similar to what we observed in patient tissues of early metastatic lesions (Figure S1A), where they could be clearly defined from other cells present in the model using nuclear PAX8 as a marker.…”

Section: Design and Establishment Of A Multi-cellular Model Of Hgsoc Metastasismentioning

confidence: 99%

A human multi-cellular model shows how platelets drive production of diseased extracellular matrix and tissue invasion

et al. 2021

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Specific Mechanisms of Chromosomal Instability Indicate Therapeutic Sensitivities in High-Grade Serous Ovarian Carcinoma

Cited by 37 publications

References 64 publications

Modelling TGFβR and Hh pathway regulation of prognostic matrisome molecules in ovarian cancer

Modelling TGFβR and Hh pathway regulation of prognostic matrisome molecules in ovarian cancer

Effects of long-term norepinephrine treatment on normal immortalized ovarian and fallopian tube cells

A human multi-cellular model shows how platelets drive production of diseased extracellular matrix and tissue invasion

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