Your search keyword '"Engebråten, Olav"' showing total 4 results

1. Molecular Features of Subtype-Specific Progression from Ductal Carcinoma In Situ to Invasive Breast Cancer

Author

Lesurf, Robert, Aure, Miriam Ragle, Mørk, Hanne Håberg, Vitelli, Valeria, Sauer, Torill, Geisler, Jürgen, Hofvind, Solveig, Borgen, Elin, Børresen-Dale, Anne-Lise, Engebråten, Olav, Fodstad, Øystein, Garred, Øystein, Geitvik, Gry Aarum, Kåresen, Rolf, Naume, Bjørn, Mælandsmo, Gunhild Mari, Russnes, Hege G., Schlichting, Ellen, Sørlie, Therese, Lingjærde, Ole Christian, Kristensen, Vessela, Sahlberg, Kristine Kleivi, Skjerven, Helle Kristine, Fritzman, Britt, Lundgren, Steinar, Børresen-Dale, Anne-Lise, Kristensen, Vessela, Wärnberg, Fredrik, Hallett, Michael, and Sørlie, Therese

Abstract

Breast cancer consists of at least five main molecular “intrinsic” subtypes that are reflected in both pre-invasive and invasive disease. Although previous studies have suggested that many of the molecular features of invasive breast cancer are established early, it is unclear what mechanisms drive progression and whether the mechanisms of progression are dependent or independent of subtype. We have generated mRNA, miRNA, and DNA copy-number profiles from a total of 59 in situ lesions and 85 invasive tumors in order to comprehensively identify those genes, signaling pathways, processes, and cell types that are involved in breast cancer progression. Our work provides evidence that there are molecular features associated with disease progression that are unique to the intrinsic subtypes. We additionally establish subtype-specific signatures that are able to identify a small proportion of pre-invasive tumors with expression profiles that resemble invasive carcinoma, indicating a higher likelihood of future disease progression.

Published

2016

2. Dynamic 18F-FDG PET for Assessment of Tumor Physiology in Two Breast Carcinoma Xenografts

Author

Kristian, Alexandr, Nilsen, Line, Røe, Kathrine, Revheim, Mona-Elisabeth, Engebråten, Olav, Mælandsmo, Gunhild, Holm, Ruth, Malinen, Eirik, and Seierstad, Therese

Abstract

To compare dynamic 2-deoxy-2-[18F]fluoro-D-glucose positron emission tomography (18F-FDG PET) parameters in two selected human breast cancer xenografts and to evaluate associations with immunohistochemistry and histology.Dynamic 18F-FDG PET of luminal-like MAS98.06 and basal-like MAS98.12 xenografts was performed, and the compartmental transfer rates (k1,k2,k3), blood volume fraction (vB) and metabolic rate of 18F-FDG(MRFDG) were estimated from pharmacokinetic model analysis. After sacrifice, analyses of hypoxia (pimonidazole), proliferation (Ki-67), vascularization (CD31), glucose transport receptor (GLUT1) and necrosis (HE) was performed. The level of hexokinase 2 (HK2) was estimated from Western blot analysis.The 18F-FDG uptake curves for the two xenografts were significantly different (p< 0.05). k1and vBwere higher for MAS98.12 (p< 0.01), while k3was higher for MAS98.06 (p< 0.01). MAS98.12 had a higher fraction of stromal tissue and higher microvessel density (MVD), and it was less necrotic and hypoxic than MAS98.06. MAS98.12 had stronger positive GLUT1 staining and lower Ki-67 than MAS98.06. In both models significant correlations were found between k1and the GLUT1 score, between k3and the level of HK2, and between vBand MVD.Significant differences in dynamic 18F-FDG parameters between the two human breast cancer xenografts were found. The differences could be explained by underlying histological and physiological characteristics.

Published

2013

3. Targeting inhibitor of apoptosis proteins in combination with dacarbazine or TRAIL in melanoma cells

Author

Engesæter, Birgit Ø., Sathermugathevan, Menaka, Hellenes, Tina, Engebråten, Olav, Holm, Ruth, Flørenes, Vivi Ann, and Mælandsmo, Gunhild M.

Abstract

Melanoma is a highly aggressive malignant tumor with an exceptional ability to develop resistance and no curative therapy is available for patients with distant metastatic disease. The inhibitor of apoptosis protein (IAP) family has been related to therapy resistance in cancer. We examined the importance of the IAPs in the resistance to the commonly used chemotherapeutic agent dacarbazine (DTIC) and the apoptosis inducer TRAIL (TNF-related apoptosis inducing ligand) in malignant melanoma. The data presented show that the expression of IAPs is universal, concomitant and generally high in melanoma cell lines and in patient samples. Depleting IAP expression by siRNA tended to reduce cell viability, with XIAP reduction being the most efficient in all four cell lines examined (FEMX-1, LOX, SKMEL-28 and WM115). The combined treatment of XIAP siRNA and DTIC showed a weak improvement in two of four cell lines, while all four cell lines showed enhanced sensitivity towards TRAIL (AdhCMV-TRAIL) after XIAP depletion. In addition, cIAP-1, cIAP-2 and survivin down-regulation sensitized to TRAIL treatment in several of the cell lines. Cells exposed to TRAIL and XIAP siRNA showed increased DNA-fragmentation and cleavage of Bid, procaspase-8, -9, -7 and -3 and PARP, and change in the balance between pro- and anti-apoptotic proteins, indicating an enhanced level of apoptosis. Furthermore, the combined treatment reduced the ability of melanoma cells to engraft and form tumors in mice, actualizing the combination for future therapy of malignant melanoma.

Published

2011

4. Human malignant melanoma harbours a large fraction of highly clonogenic cells that do not express markers associated with cancer stem cells

Author

Prasmickaite, Lina, Skrbo, Nirma, Høifødt, Hanne K., Suo, Zhenhe, Engebråten, Olav, Gullestad, Hans P., Aamdal, Steinar, Fodstad, Øystein, and Mælandsmo, Gunhild M.

Published

2010