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LC-MS/MS 定量分析 1 型发作性睡病患者低丰度血清糖蛋白衍生的 HILIC 富集-β-糖肽

LC-MS/MS Quantitation of HILIC-Enriched -glycopeptides Derived from Low-Abundance Serum Glycoproteins in Patients with Narcolepsy Type 1.

机构信息

Department of Chemistry and Biochemistry, Texas Tech University, Lubbock, TX 79409, USA.

Department of biochemistry and molecular genetics, Faculty of Biochemistry and Molecular Genetics, American University of Beirut, Beirut 11072020, Lebanon.

出版信息

Biomolecules. 2023 Oct 28;13(11):1589. doi: 10.3390/biom13111589.

Abstract

Glycoproteomic analysis is always challenging because of low abundance and complex site-specific heterogeneity. Glycoproteins are involved in various biological processes such as cell signaling, adhesion, and cell-cell communication and may serve as potential biomarkers when analyzing different diseases. Here, we investigate glycoproteins in narcolepsy type 1 (NT1) disease, a form of narcolepsy characterized by cataplexy-the sudden onset of muscle paralysis that is typically triggered by intense emotions. In this study, 27 human blood serum samples were analyzed, 16 from NT1 patients and 11 from healthy individuals serving as controls. We quantified hydrophilic interaction liquid chromatography (HILIC)-enriched glycopeptides from low-abundance serum samples of controls and NT1 patients via LC-MS/MS. Twenty-eight unique -glycopeptides showed significant changes between the two studied groups. The sialylated -glycopeptide structures LPTQNITFQTESSVAEQEAEFQSPK HexNAc, Hex, Neu5Ac (derived from the ITIH4 protein) and the structure IVLDPSGSMNIYLVLDGSDSIGASNFTGAK HexNAc, Hex, Fuc (derived from the CFB protein), with values of 0.008 and 0.01, respectively, were elevated in NT1 samples compared with controls. In addition, the -glycopeptide protein sources Ceruloplasmin, Complement factor B, and ITH4 were observed to play an important role in the complement activation and acute-phase response signaling pathways. This may explain the possible association between the biomarkers and pathophysiological effects.

摘要

糖蛋白质组学分析一直具有挑战性,因为其丰度低且存在复杂的位点特异性异质性。糖蛋白参与多种生物过程,如细胞信号转导、黏附和细胞间通讯,在分析不同疾病时可能作为潜在的生物标志物。在这里,我们研究了 1 型发作性睡病(NT1)疾病中的糖蛋白,这是一种以猝倒为特征的发作性睡病 - 肌肉突然瘫痪,通常由强烈的情绪引发。在这项研究中,分析了 27 个人类血清样本,其中 16 个来自 NT1 患者,11 个来自健康个体作为对照。我们通过 LC-MS/MS 定量分析了来自对照和 NT1 患者低丰度血清样本的亲水相互作用液相色谱(HILIC)富集糖肽。在两个研究组之间,有 28 个独特的糖肽结构发生了显著变化。唾液酸化的糖肽结构 LPTQNITFQTESSVAEQEAEFQSPK HexNAc、Hex、Neu5Ac(来自 ITIH4 蛋白)和结构 IVLDPSGSMNIYLVLDGSDSIGASNFTGAK HexNAc、Hex、Fuc(来自 CFB 蛋白),其 值分别为 0.008 和 0.01,在 NT1 样本中比对照样本升高。此外,糖肽蛋白来源 Ceruloplasmin、Complement factor B 和 ITH4 被观察到在补体激活和急性期反应信号通路中发挥重要作用。这可能解释了生物标志物与病理生理效应之间的可能关联。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b1f3/10669497/ee3ddf939b32/biomolecules-13-01589-g001.jpg

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