Rapid detection of IgG subclasses on DAT positive RBC membranes by flow cytometry (FC).

C Asmussen, K Gutensohn, D Wittkopf, P Kühnl
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引用次数: 0

Abstract

Unlabelled: Red blood cell (RBC)-bound IgG can cause hemolysis resulting, e.g. in severe cases of autoimmune hemolytic anemias (AIHA) or in hemolytic disease of the newborn (HDN). Serologic detection and differentiation of these antibodies are often difficult in cases of low antibody titers. We investigated 36 cases of poly- and monospecific IgG-positive DATs by flow cytometry. The RBC samples were washed, diluted, and incubated with monoclonal antibodies directed against IgG1, IgG2, IgG3, and IgG4, respectively. Analysis was performed on a flow cytometer. Nine cases were negative for all 4 IgG subclasses, 8 cases were positive for IgG2, 5 for IgG1, 5 for IgG3, and 3 for all four subclasses. In 6 patients we found combinations of 2 or 3 subclasses (2 for IgG1 and IgG2, 1 for IgG1 and IgG3, 1 for IgG3 and IgG4, 1 for IgG1, IgG2 and IgG4, 1 for IgG1, IgG3 and IgG4). Serological differentiation revealed specific anti-bodies only in 3 cases (anti-Lea, anti-Leb, anti-P1). The type of IgG subclass and the amount of RBC-bound IgG is relevant for the degree of in vivo RBC destruction. Flow cytometry provides a rapid, highly sensitive, cost efficient, and specific tool for IgG detection, including subgroups.

Conclusions: We therefore recommend flow cytometric analysis to be integrated into the serological decision process as an additional method for serological problem cases.

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流式细胞术(FC)快速检测DAT阳性红细胞膜上IgG亚类。
未标记:红细胞(RBC)结合的IgG可引起溶血,例如在自身免疫性溶血性贫血(AIHA)或新生儿溶血性疾病(HDN)的严重病例中。在低抗体滴度的情况下,这些抗体的血清学检测和分化往往是困难的。我们用流式细胞术研究了36例多特异性和单特异性igg阳性的dat。将红细胞样品洗涤、稀释,分别用针对IgG1、IgG2、IgG3和IgG4的单克隆抗体孵育。流式细胞仪进行分析。4种IgG亚型均阴性9例,IgG2阳性8例,IgG1阳性5例,IgG3阳性5例,4种亚型均阳性3例。在6例患者中,我们发现2或3个亚类的组合(2例为IgG1和IgG2, 1例为IgG1和IgG3, 1例为IgG3和IgG4, 1例为IgG1、IgG2和IgG4, 1例为IgG1、IgG3和IgG4)。血清学分化仅发现3例特异性抗体(抗lea、抗leb、抗p1)。IgG亚类的类型和与红细胞结合的IgG的数量与体内红细胞破坏的程度有关。流式细胞术提供了一种快速、高灵敏度、低成本和特异性的IgG检测工具,包括亚群。结论:因此,我们建议将流式细胞术分析作为血清学问题病例的附加方法整合到血清学决策过程中。
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