Wienzek-Lischka Sandra, König Inke R, Papenkort Eva-Maria, Hackstein Holger, Santoso Sentot, Sachs Ulrich J, Bein Gregor
Institute for Clinical Immunology and Transfusion Medicine, Justus-Liebig-University, Giessen, Germany.
German Center for Fetomaternal Incompatibility (DZFI), University Hospital Giessen and Marburg, Giessen, Germany.
Transfusion. 2017 Mar;57(3):533-540. doi: 10.1111/trf.13950. Epub 2016 Dec 26.
Most cases of fetal and neonatal alloimmune thrombocytopenia (FNAIT) are caused by maternal alloantibodies against human platelet antigen-1a (HPA-1a). Alloimmunization mainly occurs in HPA-1a-negative mothers who are carriers of the HLA-DRB301:01 allele. Recently, it has been reported that the combined presence of HLA-DRB301:01 and HLA-DRB4*01:01P was associated with severity of FNAIT. We tested this hypothesis by analyzing a large cohort of cases and controls.
In total, 101 mothers with a history of FNAIT caused by anti-HPA-1a were investigated. HLA-DRB1, -DRB3, -DRB4, and -DRB5 genotypes were determined by Luminex technology. Haplotype frequencies were compared between cases and 100 controls. The platelet (PLT) counts of neonates and the incidence of intracranial hemorrhage (ICH) were compared between subgroups defined by genotype.
Of the HPA-1a-immunized mothers, 98% (99/101) carried at least one copy of HLA-DRB301:01. Carriage of HLA-DRB301:01 was significantly associated with immune response to HPA-1a (odds ratio, 92.3; 95% confidence interval, 26.9-317.1; p = 1.34 × 10 ). No association between HLA-DRB301:01 and HLA-DRB401:01P alone or in combination with the PLT count of the newborns or the incidence of ICH was detected.
In contrast to HLA-DRB401:01P, the inheritance of HLA-DRB301:01 is strongly associated with the propensity for mounting a humoral immune response against fetal HPA-1a antigen. Neither a homozygous nor a compound heterozygous gene dose predicts the severity of the disease. Testing for the presence of HLA-DRB3*01:01 might be very useful in counseling women at risk of FNAIT due to anti-HPA-1a.
大多数胎儿及新生儿同种免疫性血小板减少症(FNAIT)病例是由母体针对人血小板抗原-1a(HPA-1a)的同种抗体引起的。同种免疫主要发生在携带HLA-DRB301:01等位基因的HPA-1a阴性母亲中。最近,有报道称HLA-DRB301:01和HLA-DRB4*01:01P共同存在与FNAIT的严重程度相关。我们通过分析大量病例和对照来验证这一假设。
总共调查了101名有抗HPA-1a导致的FNAIT病史的母亲。通过Luminex技术确定HLA-DRB1、-DRB3、-DRB4和-DRB5基因型。比较病例组和100名对照组的单倍型频率。比较由基因型定义的亚组之间新生儿的血小板(PLT)计数和颅内出血(ICH)的发生率。
在HPA-1a免疫的母亲中,98%(99/101)携带至少一份HLA-DRB301:01。携带HLA-DRB301:01与对HPA-1a的免疫反应显著相关(优势比,92.3;95%置信区间,26.9 - 317.1;p = 1.34×10 )。未检测到HLA-DRB301:01单独或与HLA-DRB401:01P联合与新生儿PLT计数或ICH发生率之间存在关联。
与HLA-DRB401:01P不同,HLA-DRB301:01的遗传与针对胎儿HPA-1a抗原产生体液免疫反应的倾向密切相关。纯合子或复合杂合子基因剂量均不能预测疾病的严重程度。检测HLA-DRB3*01:01的存在对于为因抗HPA-1a而有FNAIT风险的女性提供咨询可能非常有用。
