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Identifying DCN and HSPD1 as Potential Biomarkers in Colon Cancer Using 2D-LC-MS/MS Combined with iTRAQ Technology

机译:使用2D-LC-MS / MS和iTRAQ技术相结合将DCN和HSPD1鉴定为结肠癌的潜在生物标记

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摘要

Colon cancer is one of the most common types of gastrointestinal cancers and the fourth cause of cancer death worldwide. To discover novel diagnostic biomarkers for colon cancer and investigate potential mechanisms of oncogenesis, quantitative proteomic approach using iTRAQ-tagging and 2D-LC-MS/MS was performed to characterize proteins alterations in colon cancer and non-neoplastic colonic mucosa (NNCM) using laser capture microdissection-harvested from the two types of tissues, respectively. As a result, 188 DEPs were identified, and the differential expression of two DEPs (DCN and HSPD1) was further verified by Western blotting and immunohistochemistry. KEGG pathway analysis disclosed that the DEPs were related to signaling pathways associated with cancer; furthermore, DCN and HSPD1 are in the relative central hub position among protein-protein interaction subnetwork of the DEPs. The results not only shed light on the mechanism by the DEPs contributed to colonic carcinogenesis, but also showed that DCN and HSPD1 are novel potential biomarkers for the diagnosis of colon cancer.
机译:结肠癌是最常见的胃肠道癌症类型之一,也是全世界癌症死亡的第四大原因。为了发现结肠癌的新型诊断生物标记物并研究肿瘤发生的潜在机制,使用iTRAQ标签和2D-LC-MS / MS进行了定量蛋白质组学方法,使用激光表征了结肠癌和非肿瘤性结肠黏膜(NNCM)中蛋白质的变化分别从两种类型的组织中捕获显微解剖。结果,鉴定出188个DEP,并且通过Western印迹和免疫组织化学进一步证实了两种DEP(DCN和HSPD1)的差异表达。 KEGG通路分析表明,DEP与癌症相关的信号通路有关。此外,DCN和HSPD1在DEP的蛋白质-蛋白质相互作用子网络之间的相对中心枢纽位置。结果不仅阐明了DEPs导致结肠癌发生的机理,而且还表明DCN和HSPD1是诊断结肠癌的新型潜在生物标志物。

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