mRNA coexpression patterns of Wnt pathway components and their clinicopathological associations in breast and colorectal cancer

PATHOLOGY RESEARCH AND PRACTICE(2021)

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摘要
Aberrant Wnt signaling is implicated in carcinogenesis triggering efforts for the development of new therapeutic agents, many of which have entered clinical trials. We extend our previous analysis of WNT3, FZD7, LEFI expression levels in breast and colorectal cancer including WNT2, FZD4 and beta-catenin expression, in an effort to delineate their relative expression levels along with concurrent expression patterns and possible prognostic value. We analyzed 82 breast and 102 colorectal carcinomas for relative mRNA expression levels of the investigated genes by RT-PCR relative quantification with the Delta Delta Ct method. Statistical analysis was performed in order to determine associations of relative mRNA expression and linear correlations. beta-catenin expression was determined by immunochemistry. Regarding breast carcinomas, decreased relative mRNA expression levels of WNT2, FZD4 were found frequently and WNT2 expression was correlated with ER/ PR status (p = 0.045/p = 0.028), whereas beta-catenin with grade (p = 0.026). In colorectal carcinomas, increased relative mRNA expression levels of WNT2 and FZD4 were found in 59% and 32% of cases respectively, whereas beta-catenin showed decreased mRNA expression levels in 57% of cases and a correlation with pN-category (p = 0.037). Linear correlations were observed between WNT2/FZD4 (R=0.542, p < 0.001), WNT2/beta-catenin (R=0.254, p = 0.010), FZD4/beta-catenin (R=0.406, p < 0.001) expression and a correlation between mRNA expression and membranous/cytoplasmic beta-catenin emerged (p = 0.039/0.046). Our results suggest a possible clinical significance for Wnt pathway gene expression levels in both tumour types. The concurrent expression of the investigated genes as well as the different expression profiles, underlines the complexity of this pathway and the necessity of patient selection in order to maximize the efficacy of drugs targeting Wnt pathway.
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关键词
Wnt2, Frizzled 4, beta-Catenin, Breast cancer, Colorectal cancer
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