Prostanoids and colorectal cancer
In: I. Gustafsson A, Hansson E, Kressner U, Nordgren S, Andersson M, Wang W, Lönnroth C and Lundholm K. (2007) EP1-4 subtype, COX and PPARgamma receptor expression in colorectal cancer in prediction of disease-specific mortality. International Journal of Cancer, 121; 232-240 ::PMID::17290397; II. Gustafsson A, Hansson E, Kressner U, Nordgren S, Andersson M, Wang W, Lönnroth C and Lundholm K. (2007). Prostanoid receptor expression in colorectal cancer related to tumor stage, differentiation and progression. Acta Oncologica, 46; 1107-1112 ::PMID::17943472; III. Gustafsson A, Hansson E, Kressner U, Nordgren S, Andersson M, Lönnroth C, Lagerstedt KK and Lundholm K. (2010). Receptor and enzyme expression for prostanoid metabolism in colorectal camcer as related to tumor tissue PGE2. International Journal of Oncology, 36(2); 469-78 ::PMID::20043083; IV. Gustafsson Asting A, Carén H, Andersson M, Lönnroth C, Lagerstedt KK and Lundholm K. COX-2 gene expression in colorectal cancer tissue related to regulating factors and promoter methylation status. Submitted.;; (2010)
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Hochschulschrift
Zugriff:
Tumor disease is a main cause of death in Western countries and a most common malignancy is colorectal cancer (CRC). Growing tumors are dependent on interactions among several different cells as well as signaling pathways. Many tumors display increased expression of the enzyme cyclooxygenase-2 (COX-2) in conjunction with changes in tissue levels of prostanoids. However, COX-2 expression is usually unevenly distributed among cells in tumor tissue and several cell clones display little or no COX-2 expression. A frequent change of prostanoid metabolism in CRC is increased PGE2 production, which appears to be involved in several different steps of tumor progression. Prostanoids bind to receptors on cell membranes with subsequent activation of different intracellular signaling pathways. Therefore, a general aim of this work was to evaluate changes in expression of prostanoid receptors and related factors involved in prostanoid metabolism in human CRC suggesting possible specific targets for interventions on prostanoid metabolism to attenuate progression. This aim was partly performed by analyses with realtime-PCR of tumor and normal colon tissue samples from human CRC obtained at surgery. Uneven distribution of COX-2 expression, as confirmed by IHC, could hypothetically be explained by gene silencing following DNA methylation. Therefore, methylation analysis of the COX-2 promoter was also performed. Furthermore, our patients received short-term pre-operative treatment with non-selective COX-inhibition (indomethacin) to evaluate changes in gene expression related to prostanoid levels determined by microarray. Prostanoid receptor expression was decreased in tumor tissue and reduced concentration of prostanoids had no negative effect on tissue expression of most prostanoid receptors. By contrast, tumor tissue expression of the EP2 subtype receptor showed negative prediction of patient survival. Methylation of COX-2 promoter sequences did not explain the lack of COX-2 expression in tumor tissue cells. Short-term ...
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Prostanoids and colorectal cancer
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Autor/in / Beteiligte Person: | Gustafsson Asting, Annika |
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Quelle: | I. Gustafsson A, Hansson E, Kressner U, Nordgren S, Andersson M, Wang W, Lönnroth C and Lundholm K. (2007) EP1-4 subtype, COX and PPARgamma receptor expression in colorectal cancer in prediction of disease-specific mortality. International Journal of Cancer, 121; 232-240 ::PMID::17290397; II. Gustafsson A, Hansson E, Kressner U, Nordgren S, Andersson M, Wang W, Lönnroth C and Lundholm K. (2007). Prostanoid receptor expression in colorectal cancer related to tumor stage, differentiation and progression. Acta Oncologica, 46; 1107-1112 ::PMID::17943472; III. Gustafsson A, Hansson E, Kressner U, Nordgren S, Andersson M, Lönnroth C, Lagerstedt KK and Lundholm K. (2010). Receptor and enzyme expression for prostanoid metabolism in colorectal camcer as related to tumor tissue PGE2. International Journal of Oncology, 36(2); 469-78 ::PMID::20043083; IV. Gustafsson Asting A, Carén H, Andersson M, Lönnroth C, Lagerstedt KK and Lundholm K. COX-2 gene expression in colorectal cancer tissue related to regulating factors and promoter methylation status. Submitted.;; (2010) |
Veröffentlichung: | 2010 |
Medientyp: | Hochschulschrift |
ISBN: | 978-91-628-8140-5 (print) ; 91-628-8140-X (print) |
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