C3:CH50 ratio as a proposed composite marker for eculizumab monitoring in atypical hemolytic uremic syndrome: Preliminary results

Journal of Immunoassay and Immunochemistry Pub Date : 2017-03-04 DOI:10.1080/15321819.2016.1234485

K. Kerboua, F. Haiba, D. Batouche

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引用次数: 4

Abstract

ABSTRACT Treatment of atypical hemolytic uremic syndrome (aHUS) by the complement C5 inhibitor eculizumab (Soliris®) is highly effective but unfortunately, associated with an economic pressure on the health care systems even in high incomes countries. Despite spacing infusions having been proposed as the unique solution to minimize this economic impact, no reliable laboratory assays are available to tailor such therapy optimization. We aimed to propose and evaluate a complement composite marker for eculizumab efficacy monitoring in aHUS. We have retrospectively analyzed complement profiles data of eight aHUS patients under eculizumab from the International Registry of HUS/Thrombotic Thrombocytopenia Purpura, and calculated a novel marker “C3:CH50 ratio” by dividing C3 value by CH50 one for each sample during induction and maintenance periods. The results significance was compared to the currently used biomarkers for eculizumab tailoring. In contrast to the current biomarkers used for eculizumab efficacy monitoring like CH50 and soluble or deposit membrane attack complexes, “C3:CH50 ratio” seems to be the most interesting one since its value at pre-eculizumab dosage equaled 0.92 ± 0.2 while the post-eculizumab one increased significantly to reach 24.54 ± 10.7; P < 0.001. Furthermore, this ratio correlated negatively with platelets count (r = −0.722, P = 0.018) while no correlation was found within the thrombotic microangiopathy (TMA) biomarkers and complement blockade for the other parameters that change in pre and post-eculizumab therapy. As far as we know, this is the first study that suggests a post-eculizumab parameter correlating simultaneously with drug’s activity (complement inhibition) and disease activity (platelets counts). Nonetheless, the limited number of patients enrolled in this study should be considered in larger studies to guide eculizumab optimization by indicating the time when subsequent withdrawal or infusion spacing is allowed or recommended.

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C3:CH50比值作为eculizumab监测非典型溶血性尿毒症综合征的复合标记物:初步结果

补体C5抑制剂eculizumab (Soliris®)治疗非典型溶血性尿毒症综合征(aHUS)非常有效，但不幸的是，即使在高收入国家，也与卫生保健系统的经济压力相关。尽管间隔输注被认为是减少这种经济影响的唯一解决方案，但目前还没有可靠的实验室分析方法来定制这种疗法的优化。我们的目的是提出并评估一种补体复合标记物，用于监测eculizumab在aHUS中的疗效。我们回顾性分析了来自国际溶血性尿毒综合征/血栓性血小板减少性紫癜登记处的8例eculizumab下的aHUS患者的补体谱数据，并通过在诱导和维持期间将每个样本的C3值除以CH50，计算出一个新的标记物“C3:CH50比率”。结果的意义与目前用于eculizumab裁剪的生物标志物进行了比较。与目前用于eculizumab疗效监测的生物标志物(如CH50和可溶性或沉积膜攻击复合物)相比，“C3:CH50比值”似乎是最有趣的，因为在eculizumab给药前其值为0.92±0.2，而eculizumab给药后其值显著增加，达到24.54±10.7;P < 0.001。此外，该比值与血小板计数呈负相关(r = - 0.722, P = 0.018)，而血栓性微血管病变(TMA)生物标志物和补体阻断在eculizumab治疗前后的其他参数变化中未发现相关性。据我们所知，这是第一个表明eculizumab后参数与药物活性(补体抑制)和疾病活性(血小板计数)同时相关的研究。尽管如此，在更大规模的研究中，应该考虑纳入本研究的有限患者数量，通过指示允许或推荐后续停药或输液间隔的时间来指导eculizumab优化。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Journal of Immunoassay and Immunochemistry

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