Quantification of C1 inhibitor activity using a chromogenic automated assay: analytical and clinical performances.

IF 3.8 2区医学 Q1 MEDICAL LABORATORY TECHNOLOGY

Clinical chemistry and laboratory medicine Pub Date : 2024-06-12 DOI:10.1515/cclm-2024-0024

Yves Renaudineau, Laurent Sailler, Bénédicte Puissant-Lubrano

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引用次数: 0

Abstract

Objectives: The quantification of functional C1 inhibitor activity (fC1-INH) is an important tool to diagnose bradykinin-mediated angioedema (AE), whether hereditary or acquired. For that an accurate assay is necessary, therefore we evaluated the analytical performances of a fC1-INH chromogenic assay (Berichrom^®, Siemens) performed utilizing an Optilite turbidimeter (Binding Site).

Methods: fC1-INH was quantified by means of the chromogenic assay Berichrom^®. Internal quality controls were used to determine the precision of the assay. Stability under various storage and matrix conditions, uncertainty, linearity, interference (of hemolysis, lipemia, and icterus), agreement with the manual Technochrom^® assay, and diagnostic performances were further evaluated on samples from patients and healthy donors.

Results: The fC1-INH Berichrom^® assay presented good performances regarding intra- and inter-assay precision (CV: 1.3-4.5 % and 3.0-6.0 %, respectively), expanded uncertainty (5.5 % at normal level and 12.5 % at the clinical threshold) and linearity (rho²>0.99: range 7-130 % activity). Addition of interfering substances (hemoglobin <16 g/L, intralipid^® <12 g/L, and bilirubin <1 g/L) did not affect fC1-INH quantification. fC1-INH activity from healthy donors remained stable in citrate whole blood until 4 days at room temperature, and 7 days when plasma was collected. Agreement between the automated Berichrom^® assay and the manual Technochrom^® assay (n=47) was excellent as obtained with both quantitative (Deming regression and Bland-Altman difference plot) and qualitative (Kappa index=1) analyses. Finally, the diagnostic performance of the quantification of fC1-INH for AE evaluated on 81 patients revealed a sensitivity of 100 %, a specificity of 97.2 %, a positive predictive value of 83.3 % and a negative predictive value of 100 %.

Conclusions: The automated fC1-INH Berichrom^® assay showed good performance, both at the analytical and diagnostic/clinical levels that allowed its usage in a clinical laboratory for C1-INH-dependent bradykinin-mediated AE research in combination with quantitative C1-INH and C4 determinations.

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使用发色性自动测定法定量分析 C1 抑制剂活性：分析和临床表现。

目的：功能性 C1 抑制剂活性（fC1-INH）的量化是诊断缓激肽介导的血管性水肿（AE）的重要工具，无论是遗传性还是获得性血管性水肿。因此，我们评估了利用 Optilite 浊度仪（Binding Site）进行的 fC1-INH 色原测定（Berichrom®，西门子）的分析性能。内部质量控制用于确定测定的精确度。对患者和健康供体样本在不同储存和基质条件下的稳定性、不确定性、线性度、干扰（溶血、脂血和黄疸）、与手工 Technochrom® 检测法的一致性以及诊断性能进行了进一步评估：结果：fC1-INH Berichrom® 检测法在检测内和检测间精密度（CV：分别为 1.3-4.5 % 和 3.0-6.0 %）、扩大不确定性（正常水平为 5.5 %，临床阈值为 12.5 %）和线性度（rho2>0.99：活性范围为 7-130 %）方面表现良好。根据定量（戴明回归图和布兰德-阿尔特曼差异图）和定性（Kappa 指数=1）分析，加入干扰物质（血红蛋白 ® ® 检测法和手动 Technochrom® 检测法（n=47））后的结果非常好。最后，在对 81 名患者的 AE 诊断性能进行评估后发现，fC1-INH 定量的敏感性为 100%，特异性为 97.2%，阳性预测值为 83.3%，阴性预测值为 100%：自动 fC1-INH Berichrom® 检测法在分析和诊断/临床层面都表现出良好的性能，可用于临床实验室结合定量 C1-INH 和 C4 检测进行 C1-INH 依赖性缓激肽介导的 AE 研究。

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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来源期刊

Clinical chemistry and laboratory medicine 医学-医学实验技术

CiteScore

11.30

自引率

16.20%

发文量

306

审稿时长

3 months

期刊介绍： Clinical Chemistry and Laboratory Medicine (CCLM) publishes articles on novel teaching and training methods applicable to laboratory medicine. CCLM welcomes contributions on the progress in fundamental and applied research and cutting-edge clinical laboratory medicine. It is one of the leading journals in the field, with an impact factor over 3. CCLM is issued monthly, and it is published in print and electronically. CCLM is the official journal of the European Federation of Clinical Chemistry and Laboratory Medicine (EFLM) and publishes regularly EFLM recommendations and news. CCLM is the official journal of the National Societies from Austria (ÖGLMKC); Belgium (RBSLM); Germany (DGKL); Hungary (MLDT); Ireland (ACBI); Italy (SIBioC); Portugal (SPML); and Slovenia (SZKK); and it is affiliated to AACB (Australia) and SFBC (France). Topics: - clinical biochemistry - clinical genomics and molecular biology - clinical haematology and coagulation - clinical immunology and autoimmunity - clinical microbiology - drug monitoring and analysis - evaluation of diagnostic biomarkers - disease-oriented topics (cardiovascular disease, cancer diagnostics, diabetes) - new reagents, instrumentation and technologies - new methodologies - reference materials and methods - reference values and decision limits - quality and safety in laboratory medicine - translational laboratory medicine - clinical metrology Follow @cclm_degruyter on Twitter!

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