癌症患者尿液中酸性游离 N-聚糖水平升高,包括多触角和岩藻糖基化结构。

Increased levels of acidic free-N-glycans, including multi-antennary and fucosylated structures, in the urine of cancer patients.

机构信息

Department of Molecular Biology, Osaka International Cancer Institute, Chuo-ku, Osaka, Japan.

Graduate School of Science and Technology, Niigata University, Nishi-ku, Niigata, Japan.

出版信息

PLoS One. 2022 Apr 12;17(4):e0266927. doi: 10.1371/journal.pone.0266927. eCollection 2022.

Abstract

We recently reported increased levels of urinary free-glycans in some cancer patients. Here, we focused on cancer related alterations in the levels of high molecular weight free-glycans. The rationale for this study was that branching, elongation, fucosylation and sialylation, which lead to increases in the molecular weight of glycans, are known to be up-regulated in cancer. Urine samples from patients with gastric cancer, pancreatic cancer, cholangiocarcinoma and colorectal cancer and normal controls were analyzed. The extracted free-glycans were fluorescently labeled with 2-aminopyridine and analyzed by multi-step liquid chromatography. Comparison of the glycan profiles revealed increased levels of glycans in some cancer patients. Structural analysis of the glycans was carried out by performing chromatography and mass spectrometry together with enzymatic or chemical treatments. To compare glycan levels between samples with high sensitivity and selectivity, simultaneous measurements by reversed-phase liquid chromatography-selected ion monitoring of mass spectrometry were also performed. As a result, three lactose-core glycans and 78 free-N-glycans (one phosphorylated oligomannose-type, four sialylated hybrid-type and 73 bi-, tri- and tetra-antennary complex-type structures) were identified. Among them, glycans with α1,3-fucosylation ((+/- sialyl) Lewis X), triply α2,6-sialylated tri-antennary structures and/or a (Man3)GlcNAc1-core displayed elevated levels in cancer patients. However, simple α2,3-sialylation and α1,6-core-fucosylation did not appear to contribute to the observed increase in the level of glycans. Interestingly, one tri-antennary free-N-glycan that showed remarkable elevation in some cancer patients contained a unique Glcβ1-4GlcNAc-core instead of the common GlcNAc2-core at the reducing end. This study provides further insights into free-glycans as potential tumor markers and their processing pathways in cancer.

摘要

我们最近报道了一些癌症患者尿液中游离糖链水平升高。在这里,我们重点研究了高分子量游离糖链水平与癌症相关的变化。这项研究的依据是,分支、延伸、岩藻糖基化和唾液酸化会导致糖链分子量增加,这些过程在癌症中被证实是上调的。我们分析了胃癌、胰腺癌、胆管癌和结直肠癌患者和正常对照者的尿液样本。提取的游离糖链用 2-氨基吡啶荧光标记,然后通过多步液相色谱分析。糖谱分析比较显示,一些癌症患者的糖链水平升高。通过与酶或化学处理一起进行色谱和质谱分析,对糖链结构进行了分析。为了比较样品中糖链水平的敏感性和选择性,还同时进行了反相液相色谱-选择离子监测质谱分析。结果鉴定出三种乳糖核心糖链和 78 种游离 N-糖链(一种磷酸化寡甘露糖型、四种唾液酸化杂合型和 73 种双、三、四天线复杂型结构)。其中,具有α1,3-岩藻糖基化((+/-唾液酸)Lewis X)、三α2,6-唾液酸化三天线结构和/或(Man3)GlcNAc1 核心的糖链在癌症患者中水平升高。然而,简单的α2,3-唾液酸化和α1,6-核心岩藻糖基化似乎并没有导致糖链水平的升高。有趣的是,一些癌症患者中一种显著升高的三天线游离 N-糖链在还原端含有独特的 Glcβ1-4GlcNAc 核心,而不是常见的 GlcNAc2 核心。这项研究为游离糖链作为潜在肿瘤标志物及其在癌症中的加工途径提供了进一步的认识。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7d52/9004742/851b327ef847/pone.0266927.g001.jpg

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