Diagnosis of factor VIII deficiency

Verbruggen, Bert; Meijer, Piet; Nováková, I.R.O.

doi:10.1111/j.1365-2516.2008.01715.x

Cited by 41 publications

(45 citation statements)

References 32 publications

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“…The results of this study showed that the variation between laboratories is higher when FVIII activity levels are lower, both in the OSA and CSA. These results are consistent with the results by Verbruggen et al in 2008, who also showed a J‐shaped relationship between FVIII activity levels and CV, for FVIII results predominantly from the OSA. In their study, the CV increased strongly below 0.20 IU/mL with a maximal CV between 30% and 40%.…”

Section: Discussionsupporting

confidence: 93%

“…In the ECAT surveys, many different lot numbers were used by the different laboratories, and therefore, we do not expect that typical properties of a single lot will be able to influence the results from the ECAT surveys. Finally, previous studies have shown that some activators (STA Cephascreen [Stago] and Actin FS [Siemens]) are not optimal in diagnosing severe haemophilia A patients which may also have influenced the FVIII activity levels found in this study …”

Section: Discussionmentioning

confidence: 75%

“…The use of varying products may partially explain the between‐laboratory variation in FVIII results. However, it is still unclear what the precise impact is of varying in reagents and equipment on the variability of FVIII activity measurements . A possible explanation may be that particular companies provide the majority of products applied for the haemostatic testing which is standard in haemophilia.…”

Section: Introductionmentioning

confidence: 99%

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Analytical variation in factor VIII one‐stage and chromogenic assays: Experiences from the ECAT external quality assessment programme

Moort

Meijer²,

Priem‐Visser

et al. 2018

Haemophilia

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BackgroundBoth one‐stage (OSA) and chromogenic substrate assays (CSA) are used to measure factor VIII (FVIII) activity. Factors explaining analytical variation in FVIII activity levels are still to be completely elucidated.AimThe aim of this study was to investigate and quantify the analytical variation in OSA and CSA.MethodsFactors determining analytical variation were studied in sixteen lyophilized plasma samples (FVIII activity <0.01‐1.94 IU/mL) and distributed by the ECAT surveys. To elucidate the causes of OSA variation, we exchanged deficient plasma between three company set‐ups.ResultsOn average, 206 (range 164‐230) laboratories used the OSA to measure FVIII activity and 30 (range 12‐51) used CSA. The coefficient of variation of OSA and CSA increased with lower FVIII levels (FVIII <0.05 IU/mL). This resulted in misclassification of a severe haemophilia A sample into a moderate or mild haemophilia A sample in 4/30 (13.3%) of CSA measurements, while this was 37/139 (26.6%) for OSA. OSA measurements performed with reagents and equipment from Werfen showed slightly lower FVIII activity (0.93, IQR 0.88‐0.98 IU/mL) compared to measurements with Stago (1.07, IQR 1.02‐1.14 IU/mL) and Siemens (1.03, IQR 0.97‐1.07 IU/mL). Part of this difference is explained by the value of the calibrator. For CSA, the measured FVIII levels were similar using the different kits.ConclusionsIn the lower range (<0.05 IU/mL), analytical variation of FVIII measurements is high in both OSA and CSA measurements. The variation in FVIII activity levels was partly explained by specific manufacturers. Further standardization of FVIII measurements and understanding of analytical variation is required.

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Section: Discussionsupporting

confidence: 93%

Section: Discussionmentioning

confidence: 75%

Section: Introductionmentioning

confidence: 99%

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Analytical variation in factor VIII one‐stage and chromogenic assays: Experiences from the ECAT external quality assessment programme

Moort

Meijer²,

Priem‐Visser

et al. 2018

Haemophilia

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“…Haemophilia A diagnosis is usually done considering family and/or personal history of bleeding and the presence of an isolated prolonged activated partial thromboplastin time (aPTT) justified by reduced or absent FVIII:C in patient's plasma. Based on the residual FVIII:C, haemophilia A is defined as severe (FVIII:C < 1 IU/dL), moderate (FVIII:C 1‐5 IU/dL) or mild (FVIII:C 6‐40 IU/dL) . Usually age at diagnosis and bleeding frequency are inversely related to the residual FVIII:C levels.…”

Section: Introductionmentioning

confidence: 99%

Evaluation of an automated chromogenic assay for Factor VIII clotting activity measurement in patients affected by haemophilia A

et al. 2019

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Introduction The original one‐stage clotting assay is still the most widely used method to measure Factor VIII clotting activity (FVIII:C) in patients with haemophilia A (HA), although the use of chromogenic assays is increasing significantly. Aim Evaluation of the analytical performance and diagnostic accuracy of BIOPHEN™ FVIII:C (HYPHEN BioMed, Neuville‐sur‐Oise, France) assay on Sysmex CS‐2400 (Sysmex, Kobe, Japan) analyser. Methods Sixty patients with haemophilia A (HA; any severity) and 120 healthy Italian subjects were included. All the assays were performed on citrate platelet‐poor plasmas stored at −80°C. Chromogenic BIOPHEN™ FVIII:C was compared with the one‐stage assay using Actin FS and Factor VIII deficient plasma (Siemens Healthcare Diagnostics, Marburg, Germany) on Sysmex CS‐2400 and with another chromogenic automated assay (COAMATIC™ Factor VIII, CHROMOGENIX on ACL TOP analyzer; Instrumentation Laboratory, Milan, Italy). Results Intra‐assay and inter‐assay coefficient of variation were <6%. Linearity was good up to 1/128 dilution (r = 0.99); mean recovery was 91.7% and limit of detection was 0.2%. BIOPHEN™ FVIII:C assay showed a good correlation and diagnostic agreement with the chromogenic COAMATIC™ assay: the Spearmen's Rank correlation coefficient was 0.98 and the inter‐rate agreement K Cohen coefficient was 0.61. The K coefficient was 0.91 when BIOPHEN™ FVIII:C was compared with the historical classification of the patients, demonstrating an optimal diagnostic accuracy in HA. Conclusions BIOPHEN™ FVIII:C showed good analytical performance and diagnostic accuracy and could be considered suitable for the introduction in routine analytical panel of coagulation for the diagnosis of HA patients.

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“…The APTT reagent is also the test base for one-stage factor assays and the variable responsiveness is also propagated to these assays. The importance of choosing the correct APTT reagents for FVIII:C and FIX:C activity assays was recently shown by two investigations that illustrate how the diagnostic value can differ between reagents [14,15]. The laboratory phenotype known as discrepant mild haemophilia A is another example where the APTT-based onestage FVIII:C assay may be poorly correlated to the bleeding phenotype.…”

Section: Abstract: Pre-analytical Variables Aptt Coagulation Analysesmentioning

confidence: 99%

Considerations in the laboratory assessment of haemostasis

2010

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Summary. This review outlines a number of key issues when performing laboratory testing of homeostasis. The effect pre-analytical variables have on the reliability and consistency of screening tests is often forgotten due to a lack of understanding and awareness. This can be improved through educating healthcare professionals who are involved in taking blood for assessment. Recent advances in coagulation testing have not enabled laboratories to replace the Prothrombin Time (PT) and Activated Partial Thromboplastin Time (APTT) screening tests with more advanced assays and they continue to play an important role with the advantage of being easily automated. However, there are many analysers on the market, each with varying sensitivity to coagulation defects and it is important to keep this in mind when interpreting results.

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Diagnosis of factor VIII deficiency

Cited by 41 publications

References 32 publications

Analytical variation in factor VIII one‐stage and chromogenic assays: Experiences from the ECAT external quality assessment programme

Analytical variation in factor VIII one‐stage and chromogenic assays: Experiences from the ECAT external quality assessment programme

Evaluation of an automated chromogenic assay for Factor VIII clotting activity measurement in patients affected by haemophilia A

Considerations in the laboratory assessment of haemostasis

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