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Total cellular glycomics allows characterizing cells and streamlining the discovery process for cellular biomarkers

机译:总细胞糖组学可以表征细胞并简化细胞生物标志物的发现过程

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摘要

Although many of the frequently used pluripotency biomarkers are glycoconjugates, a glycoconjugate-based exploration of novel cellular biomarkers has proven difficult due to technical difficulties. This study reports a unique approach for the systematic overview of all major classes of oligosaccharides in the cellular glycome. The proposed method enabled mass spectrometry–based structurally intensive analyses, both qualitatively and quantitatively, of cellular N- and O-linked glycans derived from glycoproteins, glycosaminoglycans, and glycosphingolipids, as well as free oligosaccharides of human embryonic stem cells (hESCs), induced pluripotent stem cells (hiPSCs), and various human cells derived from normal and carcinoma cells. Cellular total glycomes were found to be highly cell specific, demonstrating their utility as unique cellular descriptors. Structures of glycans of all classes specifically observed in hESCs and hiPSCs tended to be immature in general, suggesting the presence of stem cell–specific glycosylation spectra. The current analysis revealed the high similarity of the total cellular glycome between hESCs and hiPSCs, although it was suggested that hESCs are more homogeneous than hiPSCs from a glycomic standpoint. Notably, this study enabled a priori identification of known pluripotency biomarkers such as SSEA-3, -4, and -5 and Tra-1–60/81, as well as a panel of glycans specifically expressed by hESCs and hiPSCs.
机译:尽管许多常用的多能生物标记物是糖缀合物,但是由于技术上的困难,已证明基于糖缀合物的新型细胞生物标记物的探索是困难的。这项研究报告了一种独特的方法,用于系统概述细胞糖蜜中所有主要类别的寡糖。拟议的方法能够基于质谱进行定性和定量的结构密集分析,包括从糖蛋白,糖胺聚糖和糖鞘脂以及人类胚胎干细胞(hESCs)诱导的游离寡糖衍生而来的细胞N-和O-连接的聚糖多能干细胞(hiPSC),以及源自正常细胞和癌细胞的各种人类细胞。发现细胞总糖原具有高度的细胞特异性,证明了其作为独特的细胞描述符的效用。通常在hESCs和hiPSCs中观察到的所有类别的聚糖结构一般都不太成熟,这表明存在干细胞特异性糖基化光谱。目前的分析显示,hESC和hiPSC之间的总细胞糖原高度相似,尽管从糖类学的观点来看,hESC比hiPSC更均匀。值得注意的是,这项研究能够事先鉴定出已知的多能生物标记物,例如SSEA-3,-4和-5和Tra-1-60 / 81,以及一组由hESC和hiPSC特异性表达的聚糖。

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