Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
3318371 | Pancreatology | 2007 | 8 Pages |
Abstract
Background/Aims: To co-evaluate topoisomerase Ila (Topo Ila) protein expression and gene status in pancreatic ductal adenocarcinoma, determining the potential prognostic impact of its alterations. Methods: Using tissue microarrays, 50 sporadic, primary pancreatic ductal adenocarcinomas were cored twice and re-embedded into one paraffin block with a core diameter of 1 mm. Immunohistochemistry and chromogenic in situ hybridization were performed in serial tissue sections for the detection of protein expression levels, chromosome 17 and Topo Ila gene status, respectively. Finally using a semi-automated image analysis system we evaluated the levels of protein expression. Results: A significant proportion of the tumors showed Topo Ila overexpression (32/50 or 64%). Gene amplification and deletion were detected in 9 and 4 cases, respectively, associated with protein overexpression. Aneuploidy regarding chromosome 17 was observed in 19/50 tumors and correlated with poor survival rate (Cox regression test: p = 0.001). Topo Ila protein expression was strongly correlated with stage (p = 0.021) and grade (p = 0.034). Conclusions: Topo Ila gene amplification correlates with protein overexpression, but not vice versa. This is a crucial observation for the application of targeted chemotherapies, such as anthracyclines, only in subgroups of patients, according to molecular deregulation criteria and not only to immunohistochemical results. Also, chromosome 17 and not Topo Ila gene instability can be used as a potential independent prognostic factor.
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Authors
Evangelos Tsiambas, Andreas Karameris, Dina G. Tiniakos, Petros Karakitsos,