Clinical validity of dried blood spot assay for the measurement of functional C1 inhibitor in angioedema due to C1 inhibitor deficiency

Jonathan A. Bernstein MD , Jie Cheng PhD , Thomas Pisani MSc , Dan Sexton PhD , Rachel E. Whitaker PhD , Daniel Nova Estepan PharmD, RPh , Neil Inhaber MD
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Abstract

Background

Functional C1 inhibitor (fC1INH) is a key biomarker for the diagnosis of hereditary angioedema due to C1 inhibitor (C1INH) deficiency. A novel fC1INH assay from dried blood spot (DBS) reduces practical fC1INH testing limitations versus conventional fC1INH assays, but its sensitivity and specificity have not yet been characterized.

Objective

We sought to assess the sensitivity and specificity of fC1INH DBS assay and conventional fC1INH ELISA and chromogenic assay.

Methods

fC1INH DBS assay was performed in samples from 30 patients with previously diagnosed recurrent angioedema due to C1INH deficiency and from 100 healthy controls. Whole blood samples were spotted onto blotting paper and dried for 3 hours or longer, and then fC1INH from DBS was measured through its C1s protease inhibitory activity using liquid chromatography tandem mass spectrometry. fC1INH ELISA and chromogenic assays were performed by reanalyzing a subset of 29 patients and 50 healthy controls. Sensitivity and specificity were evaluated using a negative sample mean − 1.96 SD cutoff.

Results

fC1INH DBS assay had a sensitivity of 0.93, a specificity of 0.97, and area under the curve of the receiver-operating characteristic curve of 0.996 (95% CI, 0.989-1.000). In the subset, DBS and chromogenic assay had similar sensitivity (DBS, 1.00; chromogenic assay, 0.97) and specificity (DBS, 0.94; chromogenic assay, 1.00); ELISA sensitivity was lower (0.62) and specificity similar (1.00).

Conclusions

fC1INH DBS assay had similar sensitivity and specificity when contrasted with fC1INH chromogenic assay. Because of its easier sample collection and logistic benefits, fC1INH DBS assay may allow more accessible hereditary angioedema diagnostic testing, especially in underserved regions.
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干血斑点法测定C1抑制剂缺乏性血管性水肿患者功能性C1抑制剂含量的临床有效性
背景:功能性C1抑制剂(fC1INH)是诊断C1抑制剂(C1INH)缺乏引起的遗传性血管性水肿的关键生物标志物。与传统的fC1INH检测相比,一种新的干血斑(DBS) fC1INH检测方法减少了实际的fC1INH检测局限性,但其敏感性和特异性尚未表征。目的探讨fC1INH DBS法与传统的fC1INH ELISA和显色法的敏感性和特异性。方法对30例既往诊断为C1INH缺乏所致复发性血管性水肿患者和100例健康对照进行C1INH DBS检测。将全血样本在吸墨纸上斑点,干燥3小时或更长时间,然后用液相色谱串联质谱法测定DBS中的fC1INH的C1s蛋白酶抑制活性。通过对29名患者和50名健康对照进行再分析,进行fC1INH ELISA和显色分析。采用负样本均值- 1.96 SD截止值评估敏感性和特异性。结果fc1inh DBS法的灵敏度为0.93,特异性为0.97,受者-工作特征曲线下面积为0.996 (95% CI: 0.989 ~ 1.000)。在亚组中,DBS和显色法具有相似的敏感性(DBS, 1.00;显色试验,0.97)和特异性(DBS, 0.94;显色试验,1.00);ELISA检测灵敏度较低(0.62),特异度相近(1.00)。结论fC1INH DBS法与fC1INH显色法具有相似的敏感性和特异性。由于其更容易采集样本和物流优势,fC1INH DBS分析可能允许更容易获得的遗传性血管性水肿诊断测试,特别是在服务不足的地区。
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来源期刊
The journal of allergy and clinical immunology. Global
The journal of allergy and clinical immunology. Global Immunology, Allergology and Rheumatology
CiteScore
0.70
自引率
0.00%
发文量
0
审稿时长
92 days
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