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A metabolic labeling approach for glycoproteomic analysis reveals altered glycoprotein expression upon GALNT3 knockdown in ovarian cancer cells

机译:糖蛋白组学分析的代谢标记方法揭示了敲除GALNT3后卵巢癌细胞中糖蛋白表达的改变

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摘要

Epithelial ovarian cancer (EOC) is a disease responsible for more deaths among women in the Western world than all other gynecologic malignancies. There is urgent need for new therapeutic targets and a better understanding of EOC initiation and progression. We have previously identified the polypeptide N-acetylgalactosaminyltransferase 3 (GALNT3) gene, a member of the GalNAc-transferases (GalNAc-Ts) gene family, as hypomethylated and overexpressed in high-grade serous EOC tumors, compared to low malignant potential EOC tumors and normal ovarian tissues. This data also suggested for a role of GALNT3 in aberrant EOC glycosylation, possibly implicated in disease progression. To evaluate differential glycosylation in EOC caused by modulations in GALNT3 expression, we used a metabolic labeling strategy for enrichment and mass spectrometry-based characterization of glycoproteins following GALNT3 gene knockdown (KD) in A2780s EOC cells. A total of 589 differentially expressed glycoproteins were identified upon GALNT3 KD. Most identified proteins were involved in mechanisms of cellular metabolic functions, post-translational modifications, and some have been reported to be implicated in EOC etiology.The GALNT3-dependent glycoproteins identified by this metabolic labeling approach support the oncogenic role of GALNT3 in EOC dissemination and may be pursued as novel EOC biomarkers and/or therapeutic targets. Biological significance: Knowledge of the O-glycoproteome has been relatively elusive, and the functions of the individual polypeptide GalNAc-Ts have been poorly characterized. Alterations in GalNAc-Ts expression were shown to provide huge variability in the O-glycoproteome in various pathologies, including cancer. The application of a chemical biology approach for the metabolic labeling and subsequent characterization of O-glycoproteins in EOC using the Ac4GalNAz metabolite has provided a strategy allowing for proteomic discovery of GalNAc-Ts specific functions. Our study supports an essential role of one of the GalNAc-Ts — GALNT3, in EOC dissemination, including its implication in modulating PTMs and EOC metabolism. Our approach validates the use of the applied metabolic strategy to identify important functions of GalNAc-Ts in normal and pathological conditions.
机译:上皮性卵巢癌(EOC)是一种导致西方世界女性死亡人数高于所有其他妇科恶性肿瘤的疾病。迫切需要新的治疗靶点并更好地了解EOC的启动和进展。我们先前已经确定,多肽N-乙酰半乳糖胺基转移酶3(GALNT3)基因是GalNAc-转移酶(GalNAc-Ts)基因家族的成员,在高级别浆液性EOC肿瘤中甲基化程度低且过表达,而低恶性潜能EOC肿瘤和正常的卵巢组织。该数据还暗示了GALNT3在异常EOC糖基化中的作用,可能与疾病进展有关。为了评估由GALNT3表达调节引起的EOC中的差异糖基化,我们使用了代谢标记策略对A2780s EOC细胞中GALNT3基因敲低(KD)后糖蛋白的富集和基于质谱的表征。 GALNT3 KD鉴定出总共589个差异表达的糖蛋白。大多数鉴定出的蛋白质参与细胞代谢功能,翻译后修饰的机制,并且据报道与EOC病因有关。通过这种代谢标记方法鉴定出的GALNT3依赖性糖蛋白支持GALNT3在EOC传播和扩散中的致癌作用。可以作为新的EOC生物标记和/或治疗靶标进行研究。生物学意义:对O-糖蛋白组学的了解相对较难,并且单个多肽GalNAc-Ts的功能表征较差。研究表明,GalNAc-Ts表达的变化可在包括癌症在内的各种病理中为O-糖蛋白组提供巨大的变异性。使用Ac4GalNAz代谢物对EOC中O-糖蛋白进行代谢标记和随后表征的化学生物学方法的应用提供了一种允许蛋白质组学发现GalNAc-Ts特定功能的策略。我们的研究支持GalNAc-T之一GALNT3在EOC传播中的重要作用,包括其在调节PTM和EOC代谢中的作用。我们的方法验证了在正常和病理条件下使用应用的代谢策略来识别GalNAc-Ts的重要功能。

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