首页> 外文期刊>Molecular & cellular proteomics: MCP >Glycoproteomic Analysis of Prostate Cancer Tissues by SWATH Mass Spectrometry Discovers N-acylethanolamine Acid Amidase and Protein Tyrosine Kinase 7 as Signatures for Tumor Aggressiveness
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Glycoproteomic Analysis of Prostate Cancer Tissues by SWATH Mass Spectrometry Discovers N-acylethanolamine Acid Amidase and Protein Tyrosine Kinase 7 as Signatures for Tumor Aggressiveness

机译:通过SWATH质谱对前列腺癌组织进行糖组学分析,发现N-酰基乙醇胺酸酰胺酶和蛋白酪氨酸激酶7是肿瘤侵袭性的标志。

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The identification of biomarkers indicating the level of aggressiveness of prostate cancer (PCa) will address the urgent clinical need to minimize the general over-treatment of patients with non-aggressive PCa, who account for the majority of PCa cases. Here, we isolated formerly N-linked glycopeptides from normal prostate (n = 10) and from non-aggressive (n = 24), aggressive (n = 16), and metastatic (n = 25) PCa tumor tissues and analyzed the samples using SWATH mass spectrometry, an emerging data-independent acquisition method that generates a single file containing fragment ion spectra of all ionized species of a sample. The resulting datasets were searched using a targeted data analysis strategy in which an a priori spectral reference library representing known N-glycosites of the human proteome was used to identify groups of signals in the SWATH mass spectrometry data. On average we identified 1430 N-glycosites from each sample. Out of those, 220 glycoproteins showed significant quantitative changes associated with diverse biological processes involved in PCa aggressiveness and metastasis and indicated functional relationships. Two glycoproteins, N-acylethanolamine acid amidase and protein tyrosine kinase 7, that were significantly associated with aggressive PCa in the initial sample cohort were further validated in an independent set of patient tissues using tissue microarray analysis. The results suggest that N-acylethanolamine acid amidase and protein tyrosine kinase 7 may be used as potential tissue biomarkers to avoid overtreatment of non-aggressive PCa.
机译:鉴定指示前列腺癌(PCa)侵略性水平的生物标记物将解决迫切的临床需求,以最大程度地减少占非多数PCa病例的非攻击性PCa患者的一般过度治疗。在这里,我们从正常前列腺(n = 10)和非侵袭性(n = 24),侵袭性(n = 16)和转移性(n = 25)PCa肿瘤组织中分离了以前的N-连接糖肽,并使用SWATH质谱法,一种新兴的与数据无关的采集方法,可生成一个包含文件中所有离子化物种的碎片离子光谱的单个文件。使用目标数据分析策略搜索得到的数据集,在该策略中,代表人类蛋白质组已知N-糖苷的先验光谱参考库用于识别SWATH质谱数据中的信号组。平均而言,我们从每个样品中鉴定出1430种N-糖苷。其中220种糖蛋白显示出与PCa侵袭和转移所涉及的多种生物学过程相关的显着定量变化,并表明了功能关系。使用组织芯片分析在一组独立的患者组织中进一步验证了两种糖蛋白,即N-酰基乙醇胺酸酰胺酶和蛋白酪氨酸激酶7,它们与初始样本队列中的侵略性PCa显着相关。结果表明,N-酰基乙醇胺酸酰胺酶和蛋白酪氨酸激酶7可用作潜在的组织生物标志物,以避免过度治疗非攻击性PCa。

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