Diagnostic Testing for Mild Hemophilia A in Patients with Discrepant One-Stage, Two-Stage, and Chromogenic Factor VIII:C Assays

Elizabeth M. Duncan; Susan E. Rodgers; Simon J. McRae

doi:10.1055/s-0033-1334863

Seminars in Thrombosis and Hemostasis, Table of Contents

Semin Thromb Hemost 2013; 39(03): 272-282
DOI: 10.1055/s-0033-1334863

Thieme Medical Publishers 333 Seventh Avenue, New York, NY 10001, USA.

Diagnostic Testing for Mild Hemophilia A in Patients with Discrepant One-Stage, Two-Stage, and Chromogenic Factor VIII:C Assays^[*]

Elizabeth M. Duncan

¹Haematology Division, IMVS Pathology, Adelaide, South Australia, Australia

,

Susan E. Rodgers

¹Haematology Division, IMVS Pathology, Adelaide, South Australia, Australia

,

Simon J. McRae

¹Haematology Division, IMVS Pathology, Adelaide, South Australia, Australia

› Author Affiliations

Abstract

In recent years, there has been greater awareness among hemostasis scientists and clinicians that factor VIII coagulant activity (FVIII:C) measured in certain patients with mild hemophilia A can show different results depending on the assay system. A subgroup of mild hemophilia families have a method-related discrepancy in FVIII:C results, whereby the one-stage clotting assay (FVIII:C-1) is significantly higher than the two-stage clotting assay (FVIII:C-2) or the chromogenic assay (FVIII:C-chr). To identify such patients, the routine laboratory can use automated procedures for the FVIII:C-chr to replace the complex, manual FVIII:C-2 method. Laboratories must employ appropriate quality management to ensure accurate and precise results, especially in the abnormal range. This discrepant phenotype of hemophilia A is seen in up to 40% of mild hemophilia A cases and represents a clinically significant bleeding disorder. A small proportion of these cases have FVIII:C-1 within the normal range and risk a missed diagnosis if the FVIII:C-chr is unavailable. Other patients may be mismanaged if FVIII:C-1 gives an overestimate of FVIII:C and their bleeding risk is consequently underestimated. Affected family members in the discrepant group of patients have a limited range of FVIII (F8) gene missense mutations, causing alterations of the structure of the A1, A2, or A3 domains of FVIII. Therefore, both FVIII:C-chr and F8 gene mutation analysis are recommended to confirm the diagnosis of mild hemophilia A and assist with decisions about the patient's phenotype.

Keywords

factor VIII - hemophilia A - discrepant - assay methods

Full Text

References

References
1 Preston FE, Kitchen S, Jennings I, Woods TA, Makris M. SSC/ISTH classification of hemophilia A: can hemophilia center laboratories achieve the new criteria?. J Thromb Haemost 2004; 2 (2) 271-274
2 Kitchen S, Hayward C, Negrier C, Dargaud Y. New developments in laboratory diagnosis and monitoring. Haemophilia 2010; 16 (Suppl. 05) 61-66
3 Mackie I, Cooper P, Lawrie A, Kitchen S, Gray E, Laffan M. British Committee for Standards in Haematology. Guidelines on the laboratory aspects of assays used in haemostasis and thrombosis. Int J Lab Hematol 2013; 35 (1) 1-13
4 Parquet-Gernez A, Mazurier C, Goudemand M. Functional and immunological assays of FVIII in 133 haemophiliacs—characterization of a subgroup of patients with mild haemophilia A and discrepancy in 1- and 2-stage assays. Thromb Haemost 1988; 59 (2) 202-206
5 Duncan EM, Duncan BM, Tunbridge LJ, Lloyd JV. Familial discrepancy between the one-stage and two-stage factor VIII methods in a subgroup of patients with haemophilia A. Br J Haematol 1994; 87 (4) 846-848
6 Rudzki Z, Duncan EM, Casey GJ, Neumann M, Favaloro EJ, Lloyd JV. Mutations in a subgroup of patients with mild haemophilia A and a familial discrepancy between the one-stage and two-stage factor VIII:C methods. Br J Haematol 1996; 94 (2) 400-406
7 Mazurier C, Gaucher C, Jorieux S, Parquet-Gernez A. Mutations in the FVIII gene in seven families with mild haemophilia A. Br J Haematol 1997; 96 (2) 426-427
8 Keeling DM, Sukhu K, Kemball-Cook G, Waseem N, Bagnall R, Lloyd JV. Diagnostic importance of the two-stage factor VIII:C assay demonstrated by a case of mild haemophilia associated with His1954—> Leu substitution in the factor VIII A3 domain. Br J Haematol 1999; 105 (4) 1123-1126
9 Pipe SW, Eickhorst AN, McKinley SH, Saenko EL, Kaufman RJ. Mild hemophilia A caused by increased rate of factor VIII A2 subunit dissociation: evidence for nonproteolytic inactivation of factor VIIIa in vivo. Blood 1999; 93 (1) 176-183
10 Pipe SW, Saenko EL, Eickhorst AN, Kemball-Cook G, Kaufman RJ. Hemophilia A mutations associated with 1-stage/2-stage activity discrepancy disrupt protein-protein interactions within the triplicated A domains of thrombin-activated factor VIIIa. Blood 2001; 97 (3) 685-691
11 Lyall H, Hill M, Westby J, Grimley C, Dolan G. Tyr346—> Cys mutation results in factor VIII:C assay discrepancy and a normal bleeding phenotype - is this mild haemophilia A?. Haemophilia 2008; 14 (1) 78-80
12 Lippi G, Franchini M, Favaloro EJ. One-stage clotting versus chromogenic assays for assessing recombinant factor VIII: two faces of a haemostasis coin. Blood Coagul Fibrinolysis 2009; 20 (1) 1-3
13 Denson KWE, Biggs R. Laboratory diagnosis - tests of clotting function and their standardization. In: Biggs R, , ed. Human Blood Coagulation, Haemostasis and Thrombosis. Oxford: Blackwell Scientific Publications; 1976: 310-364
14 Hathaway WE, Christian MJ, Jacobson LJ. Variant mild haemophilia. Discrepancy in one stage and two stage factor VIII assays. Thromb Haemost 1983; (Suppl. 50) 357 (abstract 1123)
15 Schwaab R, Oldenburg J, Kemball-Cook G , et al. Assay discrepancy in mild haemophilia A due to a factor VIII missense mutation (Asn694Ile) in a large Danish family. Br J Haematol 2000; 109 (3) 523-528
16 Hill M, Deam S, Gordon B, Dolan G. Mutation analysis in 51 patients with haemophilia A: report of 10 novel mutations and correlations between genotype and clinical phenotype. Haemophilia 2005; 11 (2) 133-141
17 Lucía JF, Aguilar C, Dobon M , et al. Discrepant factor VIII activity in a family with mild haemophilia A and 531 mutation using various FVIII assays and APTT reagents. Haemophilia 2005; 11 (5) 561-564
18 Cid AR, Calabuig M, Cortina V , et al. One-stage and chromogenic FVIII:C assay discrepancy in mild haemophilia A and the relationship with the mutation and bleeding phenotype. Haemophilia 2008; 14 (5) 1049-1054
19 Poulsen AL, Pedersen LH, Hvas AM, Poulsen LH, Thykjaer H, Ingerslev J. Assay discrepancy in mild haemophilia A: entire population study in a National Haemophilia Centre. Haemophilia 2009; 15 (1) 285-289
20 Kemball-Cook G. Haemophilia A Database (also known as HAMSTERs). Available at: www.hadb.org.uk . Accessed August 2012
21 Rodgers SE, Duncan EM, Barbulescu DM, Quinn DM, Lloyd JV. In vitro kinetics of factor VIII activity in patients with mild haemophilia A and a discrepancy between one-stage and two-stage factor VIII assay results. Br J Haematol 2007; 136 (1) 138-145
22 Rodgers SE, Duncan EM, Sobieraj-Teague M, Lloyd JV. Evaluation of three automated chromogenic FVIII kits for the diagnosis of mild discrepant haemophilia A. Int J Lab Hematol 2009; 31 (2) 180-188
23 Favaloro EJ, Soltani S, McDonald J, Grezchnik E, Easton L. Cross-laboratory audit of normal reference ranges and assessment of ABO blood group, gender and age on detected levels of plasma coagulation factors. Blood Coagul Fibrinolysis 2005; 16 (8) 597-605
24 Bonar R, Favaloro EJ, Adcock DM. Quality in coagulation and haemostasis testing. Biochem Med (Zagreb) 2010; 20 (2) 184-199
25 Cunningham MT, Brandt JT, Chandler WL , et al. Quality assurance in hemostasis: the perspective from the College of American Pathologists proficiency testing program. Semin Thromb Hemost 2007; 33 (3) 250-258
26 Verbruggen B, Meijer P, Novákova I, Van Heerde W. Diagnosis of factor VIII deficiency. Haemophilia 2008; 14 (Suppl. 03) 76-82
27 Westgard JO. What's the idea behind statistical quality control?. In: Basic QC Practices. 3rd ed. Madison, WI: Westgard QC Inc; 2010: 15-26
28 Westgard JO. How is the imprecision of a method determined?. In: Basic Method Validation. 2nd ed. Madison, WI: Westgard QC Inc; 2003: 101-110
29 National Pathology Accreditation Advisory Council (NPAAC). Requirements for the estimation of measurement uncertainty (2007 edition). Available at: www.health.gov.au/npaac . Accessed September 2012
30 Sobas F, Mazliak L, Bellisario A , et al. Determining the adequate number of internal quality control levels: the example of coagulation factor VIII assay. Blood Coagul Fibrinolysis 2008; 19 (5) 433-437
31 Sobas F, Benattar N, Bellisario A , et al. Impact of quality control matrix effect: application to the calculation of uncertainty of measurement in one-stage clotting factor VIII assay. Blood Coagul Fibrinolysis 2010; 21 (5) 498-501
32 Kleinveld HA, Andersson NE, van Voorthuizen H, den Hartog J, de Groot PG. Determination of coagulation factor VIII activity by a chromogenic substrate method on STA, an automated coagulation analyzer. Scand J Clin Lab Invest 1999; 59 (5) 335-341
33 Denson KWE, Wilkins T. Semi-automation of the two-stage factor VIII assay. Clin Lab Haematol 1980; 2: 311-316
34 Barrowcliffe TW. Comparisons of one-stage and two-stage assays of factor VIII:C. Scand J Haematol Suppl 1984; 41 (Suppl. 41) 39-54
35 Mainwaring CJ, Evans J, Chana J, Lewis H. Normalization of factor VIII levels in a patient with mild haemophilia A during a 35-year period. Haemophilia 2006; 12 (6) 668-671
36 Gilmore R, Harmon S, Gannon C, Byrne M, O'Donnell JS, Jenkins PV. Thrombin generation in haemophilia A patients with mutations causing factor VIII assay discrepancy. Haemophilia 2010; 16 (4) 671-674
37 Trossaërt M, Regnault V, Sigaud M, Boisseau P, Fressinaud E, Lecompte T. Mild hemophilia A with factor VIII assay discrepancy: using thrombin generation assay to assess the bleeding phenotype. J Thromb Haemost 2008; 6 (3) 486-493
38 Bowyer AE, Goodeve A, Liesner R, Mumford AD, Kitchen S, Makris M. p.Tyr365Cys change in factor VIII: haemophilia A, but not as we know it. Br J Haematol 2011; 154 (5) 618-625
39 Beltrán-Miranda CP, Khan A, Jaloma-Cruz AR, Laffan MA. Thrombin generation and phenotypic correlation in haemophilia A. Haemophilia 2005; 11 (4) 326-334
40 Lippi G, Salvagno GL, Montagnana M, Lima-Oliveira G, Guidi GC, Favaloro EJ. Quality standards for sample collection in coagulation testing. Semin Thromb Hemost 2012; 38 (6) 565-575
41 Rodgers SE, Lerda NV, Favaloro EJ , et al. Identification of von Willebrand disease type 2N (Normandy) in Australia: a cross-laboratory investigation using different methods. Am J Clin Pathol 2002; 118 (2) 269-276

Diagnostic Testing for Mild Hemophilia A in Patients with Discrepant One-Stage, Two-Stage, and Chromogenic Factor VIII:C Assays[*]

Diagnostic Testing for Mild Hemophilia A in Patients with Discrepant One-Stage, Two-Stage, and Chromogenic Factor VIII:C Assays^[*]