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Integration of zebrafish fin regeneration genes with expression data of human tumors in silico uncovers potential novel melanoma markers

机译:斑马鱼鳍再生基因与人类肿瘤在计算机上的表达数据整合发现潜在的新型黑色素瘤标志物

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摘要

Tissue regeneration requires expression of a large, unknown number of genes to initiate and maintain cellular processes such as proliferation, extracellular matrix synthesis, differentiation and migration. A unique model to simulate this process in a controlled manner is the re-growth of the caudal fin of zebrafish after amputation. Within this tissue stem cells differentiate into fibroblasts, epithelial and endothelial cells as well as melanocytes. Many genes implicated in the regeneration process are deregulated in cancer. We therefore undertook a systematic gene expression study to identify genes upregulated during the re-growth of caudal fin tissue. By applying a high stringency cut-off value of 4-fold change, we identified 54 annotated genes significantly overexpressed in regenerating blastema. Further bioinformatics data mining studies showed that 22 out of the 54 regeneration genes where overexpressed in melanoma compared to normal skin or other cancers. Whereas the role of TNC (tenascin C) and FN1 (fibronectin 1) in melanoma development is well documented, implication of MARCKS, RCN3, BAMBI, PEA3/ETV4 and the FK506 family members FKBP7, FKBP10 and FKBP11 in melanoma progression is unclear. Corresponding proteins were detected in melanoma tissue but not in normal skin. High expression of FKBP7, DPYSL5 and MDK was significantly associated with poor survival. We discuss a potential role of these novel melanoma genes, which have promising potential as new therapeutic targets or diagnostic markers.
机译:组织再生需要表达大量未知基因来启动和维持细胞过程,例如增殖,细胞外基质合成,分化和迁移。以受控方式模拟此过程的独特模型是截肢后斑马鱼尾鳍的重新生长。在该组织内,干细胞分化为成纤维细胞,上皮和内皮细胞以及黑素细胞。与再生过程有关的许多基因在癌症中被失调。因此,我们进行了一项系统的基因表达研究,以鉴定在尾鳍组织重新生长期间上调的基因。通过应用4倍变化的高严格截止值,我们确定了54个带注释的基因在再生胚泡中显着过表达。进一步的生物信息学数据挖掘研究表明,与正常皮肤或其他癌症相比,黑色素瘤中54个再生基因中有22个过度表达。尽管TNC(肌腱蛋白C)和FN1(纤连蛋白1)在黑色素瘤发展中的作用已得到充分证明,但MARCKS,RCN3,BAMBI,PEA3 / ETV4和FK506家族成员FKBP7,FKBP10和FKBP11在黑色素瘤进展中的意义尚不清楚。在黑色素瘤组织中检测到相应的蛋白质,但在正常皮肤中未检测到。 FKBP7,DPYSL5和MDK的高表达与不良的存活率显着相关。我们讨论了这些新颖的黑色素瘤基因的潜在作用,这些基因作为新的治疗靶标或诊断标记物具有广阔的前景。

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