Clinical and molecular studies of liposarcoma

dc.contributor.authorEngström, Katarina
dc.date.accessioned2007-05-21T09:16:52Z
dc.date.available2007-05-21T09:16:52Z
dc.date.issued2007-05-21T09:16:52Z
dc.description.abstractAims: (1) To analyse clinicopathological characteristics, treatment and outcome of liposarcoma, and to determine whether, and how, the Scandinavian Sarcoma Group (SSG) treatment guidelines were followed; (2) to analyse tumour volume and morphology response after radiotherapy in myxoid/round cell liposarcoma (MLS/RCLS); (3) to examine the role of the MLS-specific fusion gene FUS-DDIT3 in development of liposarcomas; and (4) to analyse expression patterns of cell cycle regulating proteins in MLS. Methods: (1) A total of 319 liposarcomas reported between 1986−1998 to the SSG Register were reviewed. Altogether 237 patients without metastasis were analyzed for local recurrences in relation to surgical margins and radiotherapy, metastasis and survival. (2) Thirty-three primary or metastatic MLSs/RCLSs were treated with radiotherapy. Tumour size was measured by MRI or CT. Histopathology was performed of both non-irradiated and irradiated lesions. (3) The fibrosarcoma cell line HT1080 was transfected with the recombinant vectors pFUS-DDIT3-EGFP, pDDIT3-EGFP and pFUSa-EGFP. The tranfectants and the HT1080 cell line were injected into SCID mice, followed by histopathology. The transfected and non-transfected cells were cultured with adipogenic induction medium and microarray-based expression comparison of the different cell lines was performed. (4) Cell cycle controlling factors were analysed by immunohistochemistry and Western blotting in non-irradiated and irradiated MLSs/RCLSs. Results: (1) Altogether 78% were primarily operated at a sarcoma centre, 45% with wide margins. Only 58% of high-grade (Grades III-IV) lesions with non-wide surgery had postoperative radiotherapy. The risk of local recurrence in this group was 47%, if not irradiated. The estimated 10-year local recurrence-free and metastasis-free survival in the low-grade (Grades I-II) group was 87% and 95% respectively, while in the high-grade group it was 75% and 61%, respectively. Independent adverse prognostic factors for local recurrence were surgery outside a sarcoma centre and dedifferentiated liposarcoma. For metastases, they were old age, large tumour size, high grade and histological type MLS /RCLS. (2) Irradiated MLS/RCLS showed median tumour volume reduction of 52% in 23 tumours. The morphology showed paucicellularity, hyalinization and lipoma-like appearance. There were no obvious differences in volume reduction or morphologic response in MLSs/RCLSs in comparison with MLSs. (3) Cells expressing FUS-DDIT3 and DDIT3 grew in SCID mice as liposarcomas and the capillary network was similar to that found in MLSs/RCLSs. Cells transfected with DDIT3 responded in vitro to adipogenic factors by accumulation of fat, and microarray-based comparison showed that the DDIT3 and FUS-DDIT3 transfected variants shifted toward an MLS/RCLS-like expression pattern. (4) High expression of cyclin D1 and E, their kinases and kinase-inhibitors P16, P27 and P57 was observed, together with low Ki67 and normal cyclin A. Conclusion: Liposarcoma should be treated at specialized centres and postoperative radiotherapy is indicated for high-grade lesions, at least after non-wide surgery. Low-grade MLSs have high radio-responsiveness, and radiotherapy is indicated after non-wide surgery or in a preoperative setting. The fusion oncogene FUS-DDIT3 and DDIT3 may induce a liposarcoma phenotype, with DDIT3 being the tumour type-determining part of the fusion oncogene. Deregulation of G1-controlling proteins is common and indicates that MLS cells accumulate in late G1 phase.eng
dc.gup.defencemåndagen den 11 juni 2007, kl 13:00 i sal Arvid Carlsson, Medicinaregatan 3eng
dc.gup.departmentInst of Clincial Sciences. Dept of Oncologyeng
dc.gup.dissdb-fakultetSA
dc.gup.mailkatarina.engstrom@oncology.gu.seeng
dc.gup.originGöteborg University. Sahlgrenska Academyeng
dc.identifier.isbn978-91-628-7193-2
dc.identifier.urihttp://hdl.handle.net/2077/4424
dc.language.isoengeng
dc.relation.haspartI. Katarina Engström, Peter Bergh, Pelle Gustafson, Ragnar Hultborn, Helena Johansson, Rickard Löfvenberg, Kirsten Sundby Hall, Clement Trovik, Ola Wahlström, Henrik C,F. Bauer. Liposarcoma-outcome based on 237 patients from the Scandinavian Sarcoma Group Register. Manuscript;eng
dc.relation.haspartII. Katarina Engström, Peter Bergh, Claes-Göran Cederlund, Ragnar Hultborn, Helena Willén, Pierre Åman, Lars-Gunnar Kindblom, Jeanne M. Meis-Kindblom. Irradiation of myxoid/round cell liposarcoma induces volume reduction and lipoma-like morphology. Acta Oncol 2007, 22 January.::pubmed::17653909eng
dc.relation.haspartIII. Katarina Engström, Helena Willén, Christina Kåbjörn-Gustafsson, Carola Andersson, Marita Olsson, Melker Göransson, Sofia Järnum, Anita Olofsson, Elisabeth Warnhammar, Pierre Åman. The myxoid/round cell liposarcoma (MLS/RCLS) fusion oncogene FUS-DDIT3 and the normal DDIT3 induce a liposarcoma phenotype in transfected human fibrosarcoma cells. Am J Pathol 2006, 168:5::doi::10.2353/ajpath.2006.050872eng
dc.relation.haspartIV. Anita Olofsson, Helena Willén, Melker Göransson, Katarina Engström, Jeane Meis-Kindblom, Göran Stenman, Lars-Gunnar Kindblom, Pierre Åman. Abnormal expression of cell cycle regulators in FUS-CHOP carrying liposarcomas. Int J Oncology 2004, 25:1349-1355::pubmed::15492825eng
dc.subjectLiposarcomaeng
dc.subjectradiotherapyeng
dc.subjectprognostic factorseng
dc.subjecttransfectioneng
dc.subjectFUD-DDIT3eng
dc.subjectadipogenesiseng
dc.subjectmicroarray expression analysiseng
dc.subjectcell cycleeng
dc.subjectimmunohistochemistryeng
dc.titleClinical and molecular studies of liposarcomaeng
dc.typetexteng
dc.type.degreeDoctor of Philosophy (Medicine)eng
dc.type.svepDoctoral thesiseng

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