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Proteomic identification of potential prognostic biomarkers in resectable pancreatic ductal adenocarcinoma

机译:蛋白质组学鉴定可切除胰腺导管腺癌中潜在的预后生物标志物

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摘要

Pancreatic cancer is a devastating disease with a mortality rate almost identical with its incidence. In this context, the investigation of the pancreatic cancer proteome has gained considerable attention because profiles of proteins may be able to identify disease states and progression more accurately. Therefore, our objective was to investigate the changes in the proteome of patients suffering from pancreatic ductal adenocarcinoma (PDAC) by a comprehensive quantitative approach. Comparative proteomic profiling by label-free LC-MS/MS analysis of nine matched pairs of tumor and nontumor pancreas samples was used to identify differences in protein levels characteristic for PDAC. In this analysis, 488 proteins were quantified by at least two peptides of which 99 proteins displayed altered levels in PDAC (p < 0.01, fold change >1.3). Screening of data revealed a number of molecules that had already been related to PDAC such as galectin-1 (LEG1), major vault protein, adenylyl cyclase-associated protein 1 (CAP1), but also a potential new prognostic biomarker prolargin (PRELP). The Kaplan-Meier survival analysis revealed a significant correlation of protein abundance of PRELP with postoperative survival of patients with PDAC. For selected proteins the findings were verified by targeted proteomics (SRM), validated by immunohistochemistry and Western blotting and their value as candidate biomarkers is discussed.
机译:胰腺癌是一种破坏性疾病,死亡率与其发病率几乎相同。在这种情况下,胰腺癌蛋白质组学的研究已引起了广泛的关注,因为蛋白质谱可能能够更准确地识别疾病状态和进展。因此,我们的目标是通过一种全面的定量方法来研究胰腺导管腺癌(PDAC)患者蛋白质组的变化。通过对九对匹配的肿瘤和非肿瘤胰腺样品对进行无标记LC-MS / MS分析,进行比较蛋白质组分析,以鉴定PDAC的蛋白水平差异。在此分析中,通过至少两个肽对488种蛋白质进行了定量,其中99种蛋白质在PDAC中显示出变化的水平(p <0.01,倍数变化> 1.3)。数据筛选显示了一些已经与PDAC相关的分子,例如半乳凝素1(LEG1),主要穹ault蛋白,腺苷酸环化酶相关蛋白1(CAP1),而且还有潜在的新预后生物标志物prolargin(PRELP)。 Kaplan-Meier生存分析表明,PRELP的蛋白质丰度与PDAC患者的术后生存密切相关。对于选定的蛋白质,结果通过靶向蛋白质组学(SRM)进行了验证,并通过免疫组织化学和Western印迹进行了验证,并讨论了它们作为候选生物标志物的价值。

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