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Proteomic analysis of platelet N-glycoproteins in PMM2-CDG patients

机译:PMM2-CDG患者血小板N-糖蛋白的蛋白质组学分析

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摘要

PMM2-CDG, the most frequent congenital disorder of N-glycosylation, is an autosomal recessive disease with a multisystem presentation. PMM2-CDG patients show an increased risk for thrombosis, which might be in part due to spontaneous platelet aggregations as previously described. A potential hypoglycosylation of platelet proteins in these patients might explain this increased reactivity, as removal of sialic acid from platelets, particularly of GPIbα, leads to enhance platelet aggregation and clearance from the circulation. This study is the first one that has evaluated the glycosylation status of platelet proteins in 6 PMM2-CDG patients using different approaches including immunoblot, RCA 120 lectin binding to platelets and expression of different membrane platelet N-glycoproteins by flow cytometry, as well as by platelet N-glycoproteome analysis. RCA120 lectin binding to the platelet membrane of PMM2-CDG patients showed evidence for decreased sialic acid content. However, immunoblot and flow cytometric analysis of different platelet N-glycoproteins, together with the more sensitive 2D-DIGE analysis, suggest that platelet N-glycoproteins, including GPIbα, seem to be neither quantitatively nor qualitatively significantly affected. The increased binding of RCA120 lectin could be explained by the abnormal glycosylation of hepatic proteins being attached to the platelets. Conclusions: This is the first study that has evaluated the platelet N-glycoproteome. Our findings suggest that platelet proteins are not significantly affected in PMM2-CDG patients. Further studies are still warranted to unravel the mechanism(s) that increase(s) the risk of thrombosis in these patients.
机译:PMM2-CDG是最常见的先天性N-糖基化疾病,是一种常染色体隐性遗传疾病,具有多系统表现。 PMM2-CDG患者显示血栓形成的风险增加,这可能部分是由于先前所述的自发性血小板聚集。这些患者中血小板蛋白潜在的低糖基化可能解释了这种增加的反应性,因为从血小板,特别是GPIbα中除去唾液酸会导致血小板聚集和从循环中清除。这项研究是第一个使用不同方法评估6名PMM2-CDG患者血小板蛋白糖基化状态的方法,包括免疫印迹,RCA 120凝集素与血小板结合以及通过流式细胞术以及通过流式细胞仪检测不同膜血小板N-糖蛋白的表达。血小板N-糖蛋白分析。 RCA120凝集素与PMM2-CDG患者的血小板膜结合显示出唾液酸含量降低的证据。但是,对不同血小板N-糖蛋白的免疫印迹和流式细胞仪分析以及更敏感的2D-DIGE分析表明,血小板N-糖蛋白(包括GPIbα)似乎没有受到定量或质量上的显着影响。 RCA120凝集素结合的增加可以通过附着在血小板上的肝蛋白的异常糖基化来解释。结论:这是评估血小板N-糖蛋白组的第一项研究。我们的发现表明,在PMM2-CDG患者中血小板蛋白未受到明显影响。仍然有必要进行进一步的研究,以阐明增加这些患者血栓形成风险的机制。

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