首页> 外文期刊>Journal of thrombosis and haemostasis: JTH >A novel flow-based assay reveals discrepancies in ADAMTS- 13 inhibitor assessment as compared with a conventional clinical static assay
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A novel flow-based assay reveals discrepancies in ADAMTS- 13 inhibitor assessment as compared with a conventional clinical static assay

机译:一种新颖的基于流量的分析方法与传统的临床静态分析方法相比揭示了ADAMTS-13抑制剂评估的差异

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Background: Several static Bethesda-type assays are routinely used to determine ADAMTS-13-neutralizing autoantibodies in acquired thrombotic thrombocytopenic purpura (TTP), but the inhibitory activity of these antibodies has not been thoroughly evaluated under the more physiologic condition of flow. Objectives: We investigated whether ADAMTS-13 inhibitor assessment with the FRETS-VWF73 assay is predictive for evaluation under flow. Methods: Anti-ADAMTS-13 autoantibodies were purified from patients with acquired TTP by chromatography involving an ADAMTS-13 affinity matrix and/or protein G. ADAMTS-13 activity was measured with the FRETS-VWF73 assay and a novel flow assay determining the ADAMTS-13-mediated decrease in platelet aggregate surface coverage, caused by perfusion of a suspension containing platelets, erythrocytes and von Willebrand factor (VWF) over a surface coated with extracellular matrix components. The neutralizing activities of ADAMTS-13 inhibitors were compared under static conditions and under flow by use of the two assays. Results: The suitability of the flow-based ADAMTS-13 activity assay for quantification of ADAMTS-13 inhibitors could be demonstrated by reversibility of the ADAMTS-13-dependent decrease in surface coverage upon addition of goat ADAMTS- 13 antiserum. Testing the neutralizing activity of purified autoantibodies from six patients in the flow assay according to their FRETS-VWF73-based inhibitor titers gave rise to vastly different inhibitory effects, indicating a discrepancy in inhibitor assessment between static and flow conditions. Conclusions: Anti-ADAMTS-13 autoantibodies may show inhibitory properties in vivo that are not consistent with the ADAMTS-13 inhibitor levels determined in routine static assays, possibly because certain epitopes are selectively exposed under shear. Consequently, the course of disease and treatment efficacy may vary among TTP patients, despite common inhibitor titers.
机译:背景:常规使用几种静态贝塞斯达型测定法来测定获得性血栓性血小板减少性紫癜(TTP)中的ADAMTS-13中和性自身抗体,但尚未在更生理的流动条件下彻底评估这些抗体的抑制活性。目的:我们调查了使用FRETS-VWF73测定的ADAMTS-13抑制剂评估是否可预测流量下的评估。方法:通过ADAMTS-13亲和基质和/或蛋白G的色谱法,从获得性TTP患者中纯化抗ADAMTS-13自身抗体。用FRETS-VWF73测定法和新型流动测定法测定ADAMTS来测定ADAMTS-13活性-13介导的血小板聚集体表面覆盖率的降低是由于在覆盖有细胞外基质成分的表面上灌注了含有血小板,红细胞和von Willebrand因子(VWF)的悬浮液引起的。通过使用两种测定法,在静态条件下和流动条件下比较了ADAMTS-13抑制剂的中和活性。结果:通过添加山羊ADAMTS-13抗血清后表面覆盖的ADAMTS-13依赖性降低的可逆性,可以证明基于流的ADAMTS-13活性测定对定量ADAMTS-13抑制剂的适用性。根据基于FRETS-VWF73的抑制剂效价在流量分析中测试来自六名患者的纯化自身抗体的中和活性,产生了截然不同的抑制作用,表明静态和流动条件之间的抑制剂评估存在差异。结论:抗ADAMTS-13自身抗体可能在体内表现出与常规静态测定中确定的ADAMTS-13抑制剂水平不一致的抑制特性,这可能是由于某些表位在剪切作用下选择性暴露所致。因此,尽管有常见的抑制剂效价,但TTP患者的病程和治疗效果可能有所不同。

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