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Evolution and Utility of Antiplatelet Autoantibody Testing in Patients with Immune Thrombocytopenia

机译:免疫血小板减少症患者抗血小板自身抗体检测的进化与效用

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To this day, immune thrombocytopenia (HT) remains a clinical diagnosis made by exclusion of other causes for thrombocytopenia. Reliable detection of platelet autoantibodies would support the clinical diagnosis, but the lack of specificity and sensitivity of the available methods for platelet autoantibody testing limits their value in the diagnostic workup of thrombocytopenia. The introduction of methods for glycoprotein-specific autoantibody detection has improved the specificity of testing and is acceptable for ruling in ITP but not ruling it out as a diagnosis. The sensitivity of these assays varies widely, even between studies using comparable assays. A review of the relevant literature combined with our own laboratory's experience of testing large number of serum and platelet samples makes it clear that this variation can be explained by variations in the characteristics of the tests, including in the glycoprotein-specific monoclonal antibodies, the glycoproteins that are tested, the platelet numbers used in the assay and the cutoff levels for positive and negative results, as well as differences in the tested patient populations. In our opinion, further standardization and optimization of the direct autoantibody detection methods to increase sensitivity without compromising specificity seem possible but will still likely be insufficient to distinguish the often very weak specific autoantibody signals from background signals. Further developments of autoantibody detection methods will therefore be necessary to increase sensitivity to a level acceptable to provide laboratory confirmation of a diagnosis of ITP. (C) 2020 The Author(s). Published by Elsevier Inc.
机译:直到今天,免疫性血小板减少症(HT)仍然是排除血小板减少症的其他原因而做出的临床诊断。血小板自身抗体的可靠检测将支持临床诊断,但现有血小板自身抗体检测方法缺乏特异性和敏感性,限制了其在血小板减少症诊断检查中的价值。糖蛋白特异性自身抗体检测方法的引入提高了检测的特异性,可用于ITP的诊断,但不排除其作为诊断。这些分析的敏感性差异很大,甚至在使用类似分析的研究之间也是如此。通过对相关文献的回顾,结合我们实验室检测大量血清和血小板样本的经验,可以清楚地看出,这种变化可以通过检测特征的变化来解释,包括糖蛋白特异性单克隆抗体、被检测的糖蛋白、,分析中使用的血小板数量,阳性和阴性结果的临界值,以及受试患者群体的差异。我们认为,进一步标准化和优化直接自身抗体检测方法,以提高灵敏度而不损害特异性似乎是可能的,但仍可能不足以区分通常非常弱的特异性自身抗体信号和背景信号。因此,有必要进一步发展自身抗体检测方法,将灵敏度提高到可接受的水平,以提供ITP诊断的实验室确认。(C) 2020作者。爱思唯尔公司出版。

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