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Glycoproteomics-based signatures for tumor subtyping and clinical outcome prediction of high-grade serous ovarian cancer

机译:基于糖蛋白质的肿瘤亚型签名和高级浆液癌的临床结果预测

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Inter-tumor heterogeneity is a result of genomic, transcriptional, translational, and post-translational molecular features. To investigate the roles of protein glycosylation in the heterogeneity of high-grade serous ovarian carcinoma (HGSC), we perform mass spectrometry-based glycoproteomic characterization of 119 TCGA HGSC tissues. Cluster analysis of intact glycoproteomic profiles delineates 3 major tumor clusters and 5 groups of intact glycopeptides. It also shows a strong relationship between N-glycan structures and tumor molecular subtypes, one example of which being the association of fucosylation with mesenchymal subtype. Further survival analysis reveals that intact glycopeptide signatures of mesenchymal subtype are associated with a poor clinical outcome of HGSC. In addition, we study the expression of mRNAs, proteins, glycosites, and intact glycopeptides, as well as the expression levels of glycosylation enzymes involved in glycoprotein biosynthesis pathways in each tumor. The results show that glycoprotein levels are mainly controlled by the expression of their individual proteins, and, furthermore, that the glycoprotein-modifying glycans correspond to the protein levels of glycosylation enzymes. The variation in glycan types further shows coordination to the tumor heterogeneity. Deeper understanding of the glycosylation process and glycosylation production in different subtypes of HGSC may provide important clues for precision medicine and tumor-targeted therapy.
机译:肿瘤间异质性是基因组,转录,平移和翻译后分子特征的结果。为了探讨蛋白质糖基化在高级浆液癌(HGSC)的异质性中的作用,我们进行119型TCGA HGSC组织的质谱基糖蛋白表征。完整糖蛋白曲线的聚类分析描绘了3个主要肿瘤簇和5组完整的糖肽。它还显示了N-聚糖结构和肿瘤分子亚型之间的强烈关系,其中一个实例是岩藻糖基化与间充质亚型的关系。进一步的生存分析表明,内置密闭亚型的完整糖肽鉴定与HGSC的临床结果不良相关。此外,我们研究MRNA,蛋白,血糖上和完整的糖肽的表达,以及参与每个肿瘤中糖蛋白生物合成途径中涉及的糖基化酶的表达水平。结果表明,糖蛋白水平主要由其各个蛋白质的表达控制,并且此外,糖蛋白改性聚糖对应于糖基化酶的蛋白质水平。聚糖类型的变化进一步显示与肿瘤异质性的协调。更深入地理解HGSC的不同亚型中的糖基化方法和糖基化产生可以为精密药物和肿瘤靶向治疗提供重要的线索。

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