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首页> 外文期刊>Biochimica et biophysica acta: BBA: International journal of biochemistry, biophysics and molecular biololgy. Proteins and Proteomics >Simultaneous characterization of SNPs and N-glycans from multiple glycosylation sites of intact beta-2-glycoprotein-1 (B2GP1) by ESI-qTOF-MS
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Simultaneous characterization of SNPs and N-glycans from multiple glycosylation sites of intact beta-2-glycoprotein-1 (B2GP1) by ESI-qTOF-MS

机译:ESI-QTOF-MS的完整β-2-糖蛋白-1(B2GP1)多糖基化位点同时表征SNP和N-聚糖

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摘要

The highly glycosylated beta-2-glycoprotein-1 (B2GP1), also called apolipoprotein H, is a 50 kDa human plasma protein with four or five N-glycosylation sites. Glycosylation of B2GP1 can impact auto antibody recognition leading to the development of antiphospholipid syndrome (APS), which can result in miscarriages or thrombosis. Next to its glycosylation different genetic variants are known to increase the risk of suffering from APS. Here we show that ESI-q/TOF-MS of intact B2GP1 can be used to analyze genetic variants and glycosylation simultaneously. After enrichment of B2GP1 from 16 different plasma samples and subsequent ESI-MS measurement of the intact protein, we detected five different SNPs in our samples either homozygous or heterozygous. The dominant glycan composition shows four biantennary, fully sialylated glycan structures, with a relative proportion of about 30%. We also detected compositions with one or two triantennary glycan structures in lower amounts and fucosylated species with one or two fucosyl residues. Two of our samples showed an unreported partially occupied fifth glycosylation site presumably arising from the presence of SNP variant 588N. Our method allows a fast determination of genetic variants and glycan compositions of human B2GP1 to be potentially used as diagnostic marker.
机译:高糖基化的β-2-糖蛋白-1(B2GP1)也称为载脂蛋白H,是50kDa人血浆蛋白,具有四个或五种N-糖基化位点。 B2GP1的糖基化会影响自动抗体识别,导致抗磷脂综合征(APS)的发育,这可能导致流产或血栓形成。众所周知,糖基化旁边,已知不同的遗传变异,以增加患有AP的风险。在这里,我们表明完整B2GP1的ESI-Q / TOF-MS可用于同时分析遗传变体和糖基化。在从16种不同的血浆样品中富集B2GP1和随后的完整蛋白质的测量后,我们在样品中检测到纯合或杂合的五种不同的SNP。优势聚糖组合物显示出四个双烯烃,完全唾液酸化的聚糖结构,相对比例约为30%。我们还以较低量和岩藻糖基化物种的一种或两种三合一甘油结构检测组合物,其中岩藻糖基化物质具有一个或两个岩藻糖基残基。我们的样品中的两个表现,从SNP变异588N的存在可能产生的未报告的部分占据第五基化位点。我们的方法允许遗传变异体和人B2GP1的聚糖的组合物的快速确定要被潜在地用来作为诊断标志物。

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