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Glycosylation of Human Plasma Clusterin Yields a Novel Candidate Biomarker of Alzheimer's Disease

机译:人血浆簇蛋白的糖基化产生阿尔茨海默氏病的新型候选生物标志物

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Specific glycosylated peptides of clusterin are found associated with hippocampal atrophy. The glycosylation of clusterin from human plasma was comprehensively analyzed and characterized using mass spectrometry (MS)-based glycoproteomics analysis. All six known N-glycosylation sites are covered, three in the alpha subunit (alpha 64N, alpha 81N and alpha 123N) and three in the beta subunit (beta 64N, beta 127N, and beta 147N). More detailed structural characterization of clusterin glycopeptides was also performed, demonstrating the presence of glycosylated peptides and their corresponding glycans. Using liquid chromatography-tandem mass spectrometry (LC-MS/MS), we have determined the differences in the glycoforms associated at each of the different glycosylation sites in plasma clusterin obtained from subjects of low hippocampal atrophy (n = 13) and high hippocampal atrophy (n = 14). In our pilot study, the beta 64N site shows the most significant regulations between clinical groups. Eight beta 64N glycoforms are significantly reduced in patients with high atrophy compared with those with low atrophy, which demonstrates the utility of clusterin isoforms as diagnostic and prognostic Alzheimers disease (AD) markers. These results provide a novel and robust workflow suitable for rapid verification of specific clusterin glycoforms with utility as AD biomarkers.
机译:发现簇蛋白的特定糖基化肽与海马萎缩有关。使用基于质谱(MS)的糖蛋白组学分析对人血浆中簇蛋白的糖基化进行了全面分析和表征。覆盖了所有六个已知的N-糖基化位点,三个位于α亚基(alpha 64N,alpha 81N和alpha 123N)和三个位于β亚基(beta 64N,beta 127N和beta 147N)。还对簇蛋白糖肽进行了更详细的结构表征,证明了糖基化肽及其相应聚糖的存在。使用液相色谱-串联质谱(LC-MS / MS),我们确定了血浆簇蛋白中每个不同糖基化位点的相关糖型的差异,这些血浆簇蛋白来自低海马萎缩症(n = 13)和高海马萎缩症患者(n = 14)。在我们的初步研究中,β64N位点显示了临床组之间最重要的规定。与萎缩程度低的患者相比,萎缩程度高的患者中有八种β64N糖型显着减少,这表明簇蛋白同工型可作为诊断和预后阿尔茨海默氏病(AD)标记物。这些结果提供了一种新颖而强大的工作流程,适用于快速验证具有AD生物标志物作用的特定簇蛋白糖型。

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