Thromb Haemost 1998; 79(04): 872-875
DOI: 10.1055/s-0037-1615080
Scientific and Standardization Committee Communication
Schattauer GmbH

A Detailed Comparison of the Performance of the Standard versus the Nijmegen Modification of the Bethesda Assay in Detecting Factor VIII:C Inhibitors in the Haemophilia A Population of Canada

Alan R. Giles
1   From the AHCDC Factor VIII Inhibitor Reference Laboratory Kingston General Hospital, Kingston, Ontario, Canada
2   From the Association of Hemophilia Centre Directors of Canada (AHCDC), Toronto, ON, Canada
,
Bert Verbruggen
3   From the Central Laboratory for Hematology of Academic Hospital St. Radboud, Nijmegen, The Netherlands
,
Georges E. Rivard
2   From the Association of Hemophilia Centre Directors of Canada (AHCDC), Toronto, ON, Canada
,
Jerome Teitel
2   From the Association of Hemophilia Centre Directors of Canada (AHCDC), Toronto, ON, Canada
,
Irwin Walker
2   From the Association of Hemophilia Centre Directors of Canada (AHCDC), Toronto, ON, Canada
,
Association of Hemophilia Centre Directors of Canada, Factor VIII/IX Subcommittee of Scientific and Standardization Committee of International Society on Thrombosis and Haemostasis › Author Affiliations
Further Information

Publication History





Publication Date:
07 December 2017 (online)

Summary

The Bethesda assay is widely used to monitor the development and progress of Factor VIII:C inhibitors. Factor VIII stability in the substrate plasma (normal pool) is compromised by pH shift and reduction in protein concentration. Preliminary study, by Verbruggen and colleagues (8), suggested a reduction in spuriously positive assay results may result from buffering the normal pool plasma substrate with imidazole to pH 7.4 and substituting Factor VIII deficient plasma for imidazole buffer in the control incubation mix. These laboratory findings have now been confirmed by the performance of both the standard and the modified Bethesda assays in parallel on 877 patient samples screened during the Factor VIII:C Inhibitor Surveillance Program instituted following the conversion of all Canadian haemophilia A patients to recombinant Factor VIII. Although this study does not address the question of the clinical significance of spurious positive assays, these laboratory findings do support the conclusions of Verbruggen and the modified assay has recently been endorsed by the Factor VIII/IX Subcommittee of the SSC.

* Association of Hemophilia Clinic Directors of Canada (AHCDC): Gerry Growe, Man-Chiu Poon, John Wu, Robert Card, Kaiser Ali, Sara Israels, Morel Rubinger, Jordan Herst, Kulwant Gill, Martin Inwood, Patricia J. McCusker, Irwin Walker, Mohan Pai, Bernadette Garvey, Jerome Teitel, Victor Blanchette, Alan Giles, David Lillicrap, Mariana Silva, Jeanne Drouin, Koon-Hung Luke, Mason Bond, Michele David, Georges Rivard, Jean St-Louis, Mariette Lepine-Martin, Christine Demers, Francois Jobin, Marie- Frances Scully, Sean Dolan, Sheldon Rubin, Dorothy Barnard, Sue Robinson, Elizabeth Ross, Lawrence Jardine


 
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