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Glycosylation pattern of anti-platelet IgG is stable during pregnancy and predicts clinical outcome in alloimmune thrombocytopenia

机译:抗血小板IgG的糖基化模式在怀孕期间稳定,并预测同种免疫性血小板减少症的临床结局

摘要

Fetal or neonatal alloimmune thrombocytopenia (FNAIT) is a potentially life-threatening disease where fetal platelets are destroyed by maternal anti-platelet IgG alloantibodies. The clinical outcome varies from asymptomatic, to petechiae or intracranial haemorrhage, but no marker has shown reliable correlation with severity, making screening for FNAIT impractical and highly inefficient. We recently found IgG Fc-glycosylation towards platelet and red blood cell antigens to be skewed towards decreased fucosylation, increased galactosylation and sialylation. The lowered core-fucosylation increases the affinity of the pathogenic antibodies to FcγRIIIa and FcγRIIIb, and hence platelet destruction. Here we analysed the N-linked glycans of human platelet antigen (HPA)-1a specific IgG1 with mass spectrometry in large series of FNAIT cases (n = 166) including longitudinal samples (n = 26). Besides a significant decrease in Fc-fucosylation after the first pregnancy (P = 0·0124), Fc-glycosylation levels remained stable during and after pregnancy and in subsequent pregnancies. Multiple logistic regression analysis identified anti-HPA-1a -fucosylation (P = 0·006) combined with galactosylation (P = 0·021) and antibody level (P = 0·038) correlated with bleeding severity, making these parameters a feasible marker in screening for severe cases of FNAIT
机译:胎儿或新生儿同种免疫血小板减少症(FNAIT)是一种潜在的威胁生命的疾病,其中胎儿血小板被母体抗血小板IgG同种抗体破坏。临床结果从无症状到瘀点或颅内出血不等,但没有标志物显示出与严重程度相关的可靠信息,因此筛查FNAIT不切实际且效率很低。我们最近发现,针对血小板和红细胞抗原的IgG Fc-糖基化倾向于降低岩藻糖基化,增加半乳糖基化和唾液酸化。降低的核心岩藻糖基化增加了病原性抗体对FcγRIIIa和FcγRIIIb的亲和力,并因此破坏了血小板。在这里,我们使用质谱分析了包括纵向样本(n = 26)在内的大批FNAIT病例(n = 166)中人血小板抗原(HPA)-1a特异性IgG1的N-连接聚糖。除了第一次怀孕后Fc岩藻糖基化显着下降(P = 0·0124)外,在怀孕期间和之后以及随后的怀孕中,Fc糖基化水平保持稳定。多重logistic回归分析确定抗HPA-1a岩藻糖基化(P = 0·006)结合半乳糖基化(P = 0·021)和抗体水平(P = 0·038)与出血严重程度相关,这些参数成为可行的标记筛查FNAIT严重病例

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