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An integrative framework identifies alternative splicing events in colorectal cancer development

机译:整合框架确定了大肠癌发展过程中的其他剪接事件

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摘要

Alternative splicing (AS) is a common mechanism which creates diverse RNA isoforms from a single gene, potentially increasing protein variety. Growing evidence suggests that this mechanism is closely related to cancer progression. In this study, whole transcriptome analysis was performed with GeneChip Human exon 1.0 ST Array from 80 samples comprising 23 normal colon mucosa, 30 primary colorectal cancer and 27 liver metastatic specimens from 46 patients, to identify AS events in colorectal cancer progression. Differentially expressed genes and exons were estimated and AS events were reconstructed by combining exon‐level analyses with AltAnalyze algorithms and transcript‐level estimations (MMBGX probabilistic method). The number of AS genes in the transition from normal colon mucosa to primary tumor was the most abundant, but fell considerably in the next transition to liver metastasis. 206 genes with probable AS events in colon cancer development and progression were identified, that are involved in processes and pathways relevant to tumor biology, as cell–cell and cell‐matrix interactions. Several AS events in VCL, CALD1, B3GNT6 and CTHRC1 genes, differentially expressed during tumor development were validated, at RNA and at protein level. Taken together, these results demonstrate that cancer‐specific AS is common in early phases of colorectal cancer natural history.
机译:选择性剪接(AS)是一种常见的机制,可从单个基因产生多种RNA亚型,从而可能增加蛋白质的多样性。越来越多的证据表明,这种机制与癌症进展密切相关。在这项研究中,使用GeneChip Human exon 1.0 ST Array进行了完整的转录组分析,从80个样本(包括23例正常结肠粘膜,30例原发性结直肠癌和27例来自46例患者的肝转移标本)中鉴定了结直肠癌进展中的AS事件。估计差异表达的基因和外显子,并通过将外显子水平分析与AltAnalyze算法和转录本水平估计(MMBGX概率方法)相结合,重建AS事件。从正常结肠粘膜到原发性肿瘤的转移中AS基因的数量最多,但在下一次肝转移的转移中,AS基因的数目大大减少。鉴定了206个可能在结肠癌发生和发展中发生AS事件的基因,这些基因参与了与细胞生物学和细胞基质相互作用相关的与肿瘤生物学相关的过程和途径。在RNA和蛋白质水平上,验证了在肿瘤发生过程中差异表达的VCL,CALD1,B3GNT6和CTHRC1基因中的几个AS事件。综上所述,这些结果表明,在大肠癌自然病程的早期阶段,常见于癌症的AS是常见的。

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