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A strategy for discovery of cancer glyco-biomarkers in serum using newly developed technologies for glycoproteomics

机译:使用新开发的糖蛋白组学技术在血清中发现癌症糖生物标志物的策略

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摘要

Detection of cancer at early stages that can be treated through surgery is a difficult task. One methodology for cancer biomarker discovery exploits the fact that glycoproteins produced by cancer cells have altered glycan structures, although the proteins themselves are common, ubiquitous, abundant, and familiar. However, as cancer tissue at the early stage probably constitutes less than 1% of the normal tissue in the relevant organ, only 1% of the relevant glycoproteins in the serum should have altered glycan structures. Here, we describe our strategy to approach the detection of these low-level glycoproteins: (a) a quantitative real-time PCR array for glycogenes to predict the glycan structures of secreted glycoproteins; (b) analysis by lectin microarray to select lectins that distinguish cancer-related glycan structures on secreted glycoproteins; and (c) an isotope-coded glycosylation site-specific tagging high-throughput method to identify carrier proteins with the specific lectin epitope. Using this strategy, we have identified many glycoproteins containing glycan structures that are altered in cancer cells. These candidate glycoproteins were immunoprecipitated from serum using commercially available antibodies, and their glycan alteration was examined by a lectin microarray. Finally, they were analyzed by multistage tandem MS.
机译:早期发现可以通过手术治疗的癌症是一项艰巨的任务。癌症生物标志物发现的一种方法是利用癌细胞产生的糖蛋白改变了聚糖结构这一事实,尽管这些蛋白本身是常见,普遍存在,丰富且熟悉的。但是,由于早期癌症组织可能构成相关器官中正常组织的不到1%,因此血清中只有1%的相关糖蛋白应具有改变的聚糖结构。在这里,我们描述了检测这些低水平糖蛋白的策略:(a)糖基因定量实时PCR阵列,以预测分泌糖蛋白的聚糖结构; (b)通过凝集素微阵列分析以选择能够区分分泌的糖蛋白上与癌症相关的聚糖结构的凝集素; (c)同位素编码的糖基化位点特异性标记高通量方法,以鉴定具有特定凝集素表位的载体蛋白。使用这种策略,我们已经鉴定出许多含有在癌细胞中改变的聚糖结构的糖蛋白。使用市售抗体从血清中免疫沉淀这些候选糖蛋白,并通过凝集素微阵列检查其聚糖变化。最后,通过多级串联质谱对其进行分析。

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