Characterization, Classification, and Treatment of von Willebrand Diseases: A Critical Appraisal of the Literature and Personal Experiences

Jan Jacques Michiels; Alain Gadisseur; Ulrich Budde; Zwi Berneman; Marc van der Planken; Wilfried Schroyens; Ann van de Velde; Huub van Vliet

doi:10.1055/s-2005-922230

Seminars in Thrombosis and Hemostasis, Table of Contents

Semin Thromb Hemost 2005; 31(5): 577-601
DOI: 10.1055/s-2005-922230

Characterization, Classification, and Treatment of von Willebrand Diseases: A Critical Appraisal of the Literature and Personal Experiences

Jan Jacques Michiels¹ ^, ⁵ , Alain Gadisseur¹ , Ulrich Budde³ , Zwi Berneman¹ , Marc van der Planken² , Wilfried Schroyens¹ , Ann van de Velde¹ , Huub van Vliet⁴

¹Hemostasis and Thrombosis Research; Department of Hematology, and Laboratory of Hematology and Hemostasis
²Department of Clinical Pathology, University Hospital Antwerp, Belgium
³Coagulation Laboratory, Hamburg, Germany
⁴Hemostasis Thrombosis Research, Erasmus University Medical Center, Rotterdam, The Netherlands
⁵Hemostasis and Thrombosis Research Science Center, Goodheart Institute, Rotterdam. The Netherlands

Abstract

ABSTRACT

Recessive type 3 von Willebrand disease (vWD) is a severe hemophilia-like bleeding disorder caused by homozygosity or double heterozygosity for two nonsense mutations (null alleles) and characterized by a strongly prolonged bleeding time (BT), absence of ristocetin-induced platelet aggregation (RIPA), absence of von Willebrand factor (vWF) protein, and prolonged activated partial thromboplastin time (APTT) due to factor VIII (FVIIIC): deficiency. Recessive severe type 1 vWD is caused by homozygosity or double heterozygosity for a missense mutation and differs from type 3 vWD by the detectable presence vWF:antigen (Ag) and FVIII:C levels between 0.09 and 0.40 U/mL. Carriers of one null allele or missense mutations are usually asymptomatic at vWF levels of 50% of normal. Mild recessive type 1 vWD may be due to a missense mutations, or one missense mutation plus blood group O. The so-called dominant type 1 vWD secretion defect and type 1 Vicenza are caused by a heterozygous missense mutation in the vWF gene that produces a mutant vWF protein having a dominant effect on the normal vWF protein produced by the normal vWF allele with regard to the defective processing, storage secretion, and/or proteolysis of vWF in endothelial cells and clearing from plasma consistent with a type 2 phenotype of vWD. Typical type 2 vWD patients, except 2N, show a defective vWF protein, decreased ratios for vWF:ristocetin cofactor [vWF:RCo]/vWF:Ag and vWF:collagen binding factor [vWF:CB]/vWF:Ag and prolonged BT. The BT is normal and FVIII:C levels clearly are lower than vWF:Ag in type 2N vWD. Multimeric analysis of vWF in plasma demonstrates that proteolysis of vWF is increased in type 2A and 2B vWD, with increased triplet structure of each band (not present in types 2M and 2U). Proteolysis of vWF is minimal in type 2C, 2D, and 2E variants that show aberrant multimeric structure of individual oligomers. vWD 2B differs from 2A by normal vWF in platelets, and increased RIPA. RIPA is normal in mild, decreased in moderate, and absent in severe type 2A vWD. RIPA is decreased or absent in 2M, 2U, 2C, and 2D; variable in 2E; and normal in 2N and dominant type 1. vWD 2M is usually mild and features decreased vWF:RCo and RIPA, and a normal or near-normal vWF multimeric pattern in a low-resolution agarose gel. vWD 2A-like or unclassifiable (2U) is distinct from 2A and 2B and typically features low vWF:RCo and RIPA with the relative lack of large vWF multimers. vWD type 2C is recessive; the dominant type 2D is rare. The response to desmopressin acetate (DDAVP) of vWF parameters is normal in pseudo-vWD and mild type 1. The responses to DDAVP of FVIII:C and vWF parameters in vWD 2M, Vincenza, 2E, and mild 2A, 2U, and 2N are transiently good for a variable number of hours to arrest mucocutaneous bleeding episodes or to prevent bleeding during minor surgery or trauma. However, the responses are not good enough to treat major bleedings or to prevent bleeding during major surgery or trauma. The response to DDAVP of vWF parameters is poor in recessive type 3, 1 and 2C, and dominant 2A, 2B, and 2U. Proper recommendations of FVIII/vWF concentrates using FVIII:C and vWF:RCo unit dosing for the prophylaxis and treatment of bleeding episodes in type 2 disease that is nonresponsive to DDAVP and in type 3 vWD are proposed.

KEYWORDS

von Willebrand factor - von Willebrand disease - ristocetin cofactor activity - von Willebrand collagen binding activity - factor VIII:C - bleeding time - desmopressin acetate

Full Text

References

REFERENCES

1 Goodeve A, Peake I. A standard nomenclature for von Willebrand factor gene mutations and polymorphisms. Baillieres Clin Haematol. 2001; 14 235-240
2 Sadler J E. A revised classification of von Willebrand disease. Baillieres Clin Haematol. 1994; 71 520-525
3 Sadler J E, Mannucci P M, Berntorp E et al.. Impact, diagnosis and treatment of von Willebrand Disease. Thromb Haemost. 2000; 84 160-174
4 Zhang Z, Lindstedt M, Blombäck M, Anvret M. Effects of mutant von Willebrand factor gene in von Willebrand disease. Hum Genet. 1995; 96 388-394
5 Schneppenheim R, Krey S, Bergmann F et al.. Genetic heterogeneity of severe von Willebrand disease type III in the German population. Hum Genet. 1994; 94 640-652
6 Eikenboom J CJ. Congenital von Willebrand disease type 3: clinical manifestations, pathophysiology and molecular biology. Baillieres Clin Haematol. 2001; 14 365-379
7 Lak M, Peyvandi F, Mannucci P M. Clinical manifestations and complications of childbirth and replacement therapy in 385 Iranian patients with type 3 von Willebrand disease. Br J Haematol. 2000; 111 1236-1239
8 Eikenboom J CJ, Castaman G, Vos H L, Bertina R M, Rodeghiero F L. Characterisation of genetic defects in recessive type 1 and type 3 von Willebrand disease patients of Italian origin. Thromb Haemost. 1998; 79 709-717
9 Allen S, Abuzenadah A M, Hinks J et al.. A novel von Willebrand disease-causing mutation (Arg273Trp) in the von Willebrand factor propeptide that results in defective multimerisation and secretion. Blood. 2000; 96 560-568
10 Castaman G, Lattuada A, Mannucci P M, Rodeghiero F. Factor VIII:C increases after desmopressin in a subgroup of patients with autosomal recessive severe von Willebrand disease. Br J Haematol. 1995; 89 147-151
11 Castaman G, Eikenboom JCJ, Lattuada A, Manucci P M, Rodeghiero F. Heightened proteolysis of the von Willebrand factor subunit in patients with von Willebrand disease hemizygous or homozygous for the C2364F mutation. Br J Haematol. 2000; 108 188-190
12 Castaman G, Novella E, Castiglia E, Eikenboom JCJ, Rodeghiero F. A novel family with recessive von Willebrand disease due to compound heterozygosity for a splice site mutation and a missense mutation in the von Willebrand factor gene. Thromb Res. 2002; 105 135-138
13 Schneppenheim R, Budde U, Obser T et al.. Expression and characterization of von Willebrand factor dimerization defects in different types of von Willebrand disease. Blood. 2001; 97 2059-2066
14 Eikenboom J CJ, Reitsma P H, Peerlinck K JM, Briet E. Recessive inheritance of von Willebrand’s disease. Lancet. 1993; 341 982-986
15 Gill J C, Endres-Brooks J, Bauer P J, Marks W J, Montgomery J R. The effect of ABO bloodgroup on the diagnosis of von Willebrand dsease. Blood. 1987; 69 1691-1695
16 Sadler J E. Von Willebrand disease type 1: a diagnosis in search of a disease. Blood. 2003; 101 2089-2093
17 Sadler J E. New concepts in von Willebrand Disease. Annu Rev Med. 2005; 56 173-191
18 Coughlan T C, Blagg J L, Alulola M et al.. Null alleles are not a common cause of type 1 von Willebrand disease in the British population. Thromb Haemost. 1999; 82 1373-1375
19 O'Brien L A, James P D. Hemophilia Clinical Directors Canada . Lillicrap D. Founder von Willebrand factor haplotype associated with type 1 von Willebrand disease. Blood. 2003; 102 549-557
20 Bowen D. Type 1 von Willebrand disease: a possible novel mechanism. Blood Coagul Fibrinolysis. 2004; 14(suppl 1) S21-S23
21 Bowen D, Collins P W, Lester W et al.. The prevalence of the cysteine 1584 variant of von Willebrand factor is increased in type 1 von Willebrand disease: co-segregation with increased susceptibility to 13 proteolysis but not clinical phenotype. Br J Haematol. 2005; 128 830-836
22 Michiels J J, Van De Velde A, Van Vliet H HDM, Van Der Planken M, Schroyens W, Berneman Z N. Response of von Willebrand factor parameters to desmopressin in patients with type 1 and type 2 congenital von Willebrand disease: diagnostic and therapeutic implications. Semin Thromb Hemost. 2002; 28 111-131
23 Eikenboom J CJ, Castaman G, Kamphuisen P W, Rosendaal F R, Bertina R M. The factor VIII/von Willebrand factor ratio discriminates between reduced synthesis and increased clearance of von Willebrand factor. Thromb Haemost. 2002; 87 252
24 Eikenboom J CJ, Matsushita T, Reitsma P H et al.. Dominant type 1 von Willebrand disease caused by mutated cysteine residues in the D3 domain of von Willebrand factor. Blood. 1996; 88 2433-2441
25 Bodo I, Katsumi A, Tuley E A, Eikenboom J CJ, Dong Z, Sadler J E. Type 1 von Willebrand disease mutation Cys1149Arg causes intracellular retention and degradation of heterodimers: a possible general mechanism for dominant mutations of oligomeric proteins. Blood. 2001; 98 2973-2978
26 Castaman G, Eikenboom J CJ, Missiaglia E, Rodeghiero F. Autosomal dominant type 1 von Willebrand disease due to G3639T mutation (C1130) in exon 26 of von Willebrand gene: description of five Italian families and evidence for a founder effect. Br J Haematol. 2000; 108 876-879
27 Tjernberg P, Vos H L, Castaman G, Bertina R M, Eikenboom J CJ. Dimerization and multimerization defects of von Willebrand factor due to mutated cysteine residues. J Thromb Haemost. 2004; 2 257-265
28 Casana P, Martinez F, Haya S, Espinos C. Association of the 3467C > T mutation (T1156M) in the von Willebrand’s factor gene with dominant type 1 von Willebrand’s disease. Ann Hematol. 2001; 80 381-383
29 Federici A B, De Groot P hG, Moia M, Ijssedijk M JW, Sixma J J, Mannucci P M. Type 1 von Willebrand disease, subtype ‘platelet low’: decreased platelet adhesion can be explained by low synthesis of von Willebrand factor in endothelial cells. Br J Haematol. 1993; 83 88-93
30 Nitu-Whalley I C, Ridell A, Lee C et al.. Identification of type 2 von Willebrand disease in previously diagnosed type 1 patients: a reappraisal using phenotypes, genotypes and molecular modelling. Thromb Haemost. 2000; 84 998-1004
31 Mannucci P M, Lombardi R, Castaman G et al.. Von Willebrand disease “Vicenza” with larger-than-normal (Supranormal) von Willebrand factor multimers. Blood. 1988; 71 65-70
32 Casonato A, Pontara E, Sartorelo F et al.. Reduced von Willebrand factor survival in type Vicenza von Willebrand disease. Blood. 2002; 99 180-184
33 Cattaneo M, Federici A B, Lecchi A et al.. Evaluation of the PFA-1000 system in the diagnosis and therapeutic monitoring of patients with von Willebrand disease. Thromb Haemost. 1999; 82 35-39
34 Schneppenheim R, Federici A, Budde U et al.. von Willebrand disease type 2M “Vicenza” in Italian and German patients: identification of the first candidate mutation (G3864A; R1205H) in 8 families. Thromb Haemost. 2000; 82 136-140
35 Michiels J J, Berneman Z, Gadisseur A et al.. Characterization of recessive severe type 1 and 3 von Willebrand disease (VWD), asymptomatic heterozygous carriers versus bloodgroup O related von Willebrand factor deficiency and dominant type 1 VWD. Clin Applied Thromb Hemost. 2005; , (in press)
36 De Wit T R, Van Mourik J A. Biosynthesis, processing and secretion of von Willebrand factor: biological implications. Baillieres Clin Haematol. 2001; 14 241-255
37 Ruggeri Z M. Structure of von Willebrand factor and itsfunction in platelet adhesion and thrombus formation. Baillieres Clin Haematol. 2001; 14 257-279
38 Zimmerman ThS, Dent JA, Ruggeri ZM, Nannini LH. Subunit composition of plasma von Willebrand factor. J Clin Invest. 1986; 77 947-951
39 Schneppenheim R, Budde U, Ruggeri Z M. A molecular approach to the classfication of von Willebrand disease. Baillieres Clin Haematol. 2001; 14 281-298
40 Budde U, Scheneppenheim R. Phenotypic and genotypic diagnosis of von Willebrand disease: a 2004 update. Semin Hematol. 2005; 42 15-28
41 Nichols W, Ginsburg D. von Willebrand disease. Medicine. 1997; 76 1-20
42 Meyer D, Fressinaud E, Gaucher C et al.. Gene defects in 150 unrelated French cases with type 2 von Willebrand disease: from the patient to the gene. Thromb Haemost. 1997; 78 451-456
43 Meyer D, Fressinaud E, Hilbert L, Ribba A-S, Lavergne J-M, Mazurier C. Type 2 von Willebrand disease causing defective vonWillebrand factor-dependent platelet function. Baillieres Clin Haematol. 2001; 14 349-364
44 Castaman G, Federici A B, Rodeghiero F, Mannucci P M. von Willebrand's disease in the year 2003: towards the complete indentification of gene defects for correct diagnosis and treatment. Haematologica. 2003; 88 94-108
45 Lyons S E, Bruck M E, Bowie EJW, Ginsburg D. Impaired intracellular transport by a subset of type IIA von Willebrand disease mutations. J Biol Chem. 1992; 267 4424-4430
46 Batlle J, Lopez-Fernandez M F, Campos M et al.. The heterogeneity of type IIA von Willebrand's disease. Blood. 1986; 68 1207-1212
47 Batlle J, Lassieri J, Villamor A F et al.. Proteolytic processing of von Willebrand factor subunit: heterogeneity in type IIA von Willebrand disease. Ann Hematol. 1994; 68 111-115
48 Howard M A, Salem H H, Thomas K B et al.. Variant von Willebrand's disease type B-revisited. Blood. 1982; 60 1420-1428
49 Rabinowitz I, Tuley E A, Mancuso D J et al.. von Willebrand disease type B: a missense mutation selectively abolishes ristocetine-induced von Willebrand binding to platelet glycoprotein Ib. Proc Natl Acad Sci USA. 1992; 89 9846-9849
50 Firkin B, Firkin F, Stott L. von Willebrand's disease type B: a newly defined bleeding diathesis. Aust N Z J Med. 1973; 3 225-229
51 Mannucci P M, Lombardi R, Bader R et al.. Heterogeneity of type I von Willebrand disease: evidence for a subgroup with abnormal von Willebrand factor. Blood. 1985; 66 796-802
52 Federici A B, Canciani M T, Forza I, Cozzi G. Ristocetin cofactor and collagen binding activities normalized to antigen levels for a rapid diagnosis of type 2 von Willebrand disease. Thromb Haemost. 2000; 84 1127-1128
53 Mancusco D J, Kroner P A, Christopherson P M, Vokac E A, Gill J C, Montgomery R R. Type 2M:Milwaukee-1 von Willebrand disease with an in-frame deletion in the Cys509-Cys695 loop of the von Willebrand factor A1 domain causes deficient binding of von Willebrand to platelets. Blood. 1996; 88 2559-2568
54 Hillery C A, Mabcusco D J, Sadler J E et al.. Type 2M von Willebrand disease: F606I and I662F mutations in the glycoprotein Ib binding domain selectively impair ristocetin-but not botrocetin-mediated binding of von Willebrand factor to platelets. Blood. 1998; 91 1572-1581
55 Hilbert L, Jenkins P V, Gaucher G et al.. Type 2M vWD resulting from a lysine deletion within a four lysine residue repeat in the A1 loop of von Willebrand factor. Thromb Haemost. 2000; 84 188-194
56 Michiels J J, Berneman Z, Gadisseur A et al.. Classification and characterization of type 2A, 2B, 2C, 2E, 2D, 2M, 2N and 2U (unclassifiable) von Willebrand diseases. Clin Appl Thromb Hemost. 2005; , (in press)
57 Lethagen S, Frick K, Isaksson C, Kristoffersson A-C, Holmberg L. Revised classification and treatment of von Willebrand disease. Thromb Haemost. 1998; 80 199-200
58 Hoyer L W, Rizza C R, Tuddenham G D, Carta C A, Armitage H, Rotblatt F. von Willebrand factor multimer patterns in von Willebrand's disease. Br J Haematol. 1983; 55 493-507
59 Castaman G, Eikenboom J CJ, Rodeghiero F, Briet E, Reitsma PH. A novel candidate mutation (Arg⁶¹¹ → His) in type I ‘platelet discordant' von Willebrand disease with desopressine-induced thrombocytopenia. Br J Haematol. 1995; 89 656-658
60 Hilbert L, Gaucher C, Mazurier C. Identification of two mutations (Arg611Cys and Arg611His) in the A1 loop of von Willebrand factor (VWF) responsible for type 2 von Willebrand disease with decreased platelet-dependent function of VWF. Blood. 1995; 86 1010-1018
61 Nishikubo T, Christophe O, Lavergne J-M et al.. Abnormal proteolytic processing of von Willebrand factor Arg611Cys and Arg611His. Thromb Haemost. 1997; 77 174-182
62 Ribba A N, Hilbert L, Lavergne J M et al.. The Arg552Cys (R552C) mutation within the A1 loop of von Willebrand factor (VWF) induces abnormal folding with loss-of-function resulting in 2A-like phenotype of von Willebrand disease. Study of ten patients and of mutated recombinant VWF. Blood. 2001; 97 952-959
63 Ruggeri Z M, Nilsson I M, Lombardi R, Holmberg L, Zimmerman TS. Aberrant multimeric structure of von Willebrand factor in a new variant of von Willebrand's disease (type IIC). J Clin Invest. 1982; 70 1124-1127
64 Holmberg L, Karpman D, Isakson C, Kristofferson A C, Lethagen S, Schneppenheim R. Ins405AsnPro mutation in the von Willebrand factor propeptide in recessive type 2A (IIC) von Willebrand's disease. Thromb Haemost. 1998; 79 718-722
65 Mazurier C, Manucci P M, Parquet-Gernez A, Goudemand M, Meyer D. Investigation of a case of subtype IIC von Willebrand disease: characterisation of the variability of this subtype. Am J Hematol. 1986; 22 301-311
66 Gaucher C, Diéval J, Mazurier C. Characterization of von Willebrand factor gene defects in two unrelated patients with type IIC von Willebrand disease. Blood. 1994; 84 1024-1030
67 Batlle J, Lopez-Fernandez M F, Lasiera J et al.. von Willebrand disease type IIC with different abnormalities of von Willebrand factor in the same sibship. Am J Hematol. 1986; 21 177-188
68 Batlle J, Lopez Gernandez M F, Fernandez Villamor A, Lopez Berges C, Zimmerman TS. Multimeric pattern discrepancy between platelet and plasma von Willebrand factor in type IIC von Willebrand disease. Am J Hematol. 1986; 22 87-88
69 Schneppenheim R, Thomas K B, Krey S et al.. Identification of a candidate missense mutation in a family with von Willebrand disease type IIC. Hum Genet. 1995; 95 681-686
70 Mannucci P M, Lombardi R, Pareti F I, Solinas S, Mazzucconi M G, Mariani G. A variant of von Willebrand's disease characterized by recessive inheritance and missing triplet structure of von Willebrand factor multimers. Blood. 1983; 62 1000-1005
71 Kinoshita S, Harrison J, Lazerson J, Abildgaard CF. A new variant of dominant type II von Willebrand's disease with aberrant multimeric pattern of factor VIII-related antigen (type IID). Blood. 1984; 63 1369-1371
72 Schneppenheim R, Brassard J, Krey S et al.. Defective dimerization of von Willebrand factor subunits due to a Cys → Arg mutation in type IID von Willebrand disease. Proc Natl Acad Sci USA. 1996; 93 3581-3586
73 Schneppenheim R, Budde U, Obser T et al.. Expression and characterization of von Willebrand factor dimerization defects in different types of von Willebrand disease. Blood. 2001; 97 2059-2066
74 Baillod P, Gaucher C, Affolter B, Mazurier C, Pflugshaupt R. New variant of type II von Willebrand's disease with structural abnormality of plasma von Willebrand factor in a patient with very mild bleeding history. Am J Hematol. 1995; 49 21-28
75 Gaucher C, Parquet A, Baillod P, Hanss M, Mazurier C. Mutations in the D3 domain of von Willebrand factor are identified in patients classified as 1 or 2A von Willebrand disease. Thromb Haemost. 1997; (suppl) 388 , (abst OC-1583)
76 Castaman G, Rodeghiero F, Lattuada A, Mannucci P M. A new variant of von Willebrand disease (type II I) with a normal degree of proteolytic cleavage of von Willebrand factor. Thromb Res. 1992; 65 343-351
77 Ledford M, Rabinowitz I, Sadler J E, Kent J W, Civantos F. New variant of von Willebrand disease type II with markedly increased levels of von Willebrand antigen and dominant mode of inheritance: von Willebrand disease type IIC Miami. Blood. 1993; 82 169-175
78 Mannucci P M, Lombardi R, Federici A B, Dent J A, Zimmerman TS, Ruggeri ZM. A new variant of type II von Willebrand disease with aberrant multimeric structure of plasma but not platelet von Willebrand factor (type IIF). Blood. 1986; 68 269-274
79 Gralnick H R, Williams S B, McKeown L P, Maisonneuve P, Jeneau C, Sultan Y. A variant of type II von Willebrand disease with an abnormal triplet structure and discordant effects of protease inhibitors on plasma and platelet von Willebrand factor structure. Am J Hematol. 1987; 24 259-266
80 Federici A B, Manuccio P M, Lombardi R et al.. Type II H von Willebrand disease: new structural abnormality of plasma and platelet von Willebrand factor in a patients with prolonged bleeding time and borderline levels of ristocetin cofactor activity. Am J Hematol. 1989; 32 287-293
81 Mazurier C. von Willebrand disease masquerading as haemophilia A. Thromb Haemost. 1992; 67 391-396
82 Mazurier C, Goudemand J, Hilbert L, Caron C, Fressinaud E, Meyer D. Type 2N von Willebrand disease: clinical manifestations, pathophysiology. Laboratory diagnosis and molecular biology. Baillieres Clin Haematol. 2001; 14 337-347
83 Schneppenheim R, Budde U, Krey S et al.. Results of a screening for von Willebrand disease type 2N in patients with suspected haemophilia A or von Willebrand disease type 1. Thromb Haemost. 1996; 76 598-602
84 Mazurier C, Gaucher C, Joriuex S, Goudemand M. Biological effect of desmopressin in eight patients with type 2N (‘Normandy’) von Willebrand disease. Br J Haematol. 1994; 88 849-854
85 Federici A B, Mazurier C, Berntorp E et al.. Biologic response to desmopressin in patients with severe type 1 and type 2 von Willebrand disease: results of a multicenter European study. Blood. 2004; 103 2032-2038
86 Mannucci P M, Moia M, Rebulla P, Altieri D, Monteaguda J, Castillo R. Correction of the bleeding time in treated patients with severe von Willebrand disease is not solely dependent on the normal multimeric structure of plasma von Willebrand factor. Am J Hematol. 1987; 25 55-65
87 Castillo R, Monteaguda J, Escolar G, Ordinas A, Magallon M, Villar J M. Hemostatic effect of normal platelet transfusion in severe von Willebrand disease patients. Blood. 1991; 77 1901-1905
88 Mannucci P M. Recommended protocol for the study of ex vivo biological effects of virus-inactivated plasma concentrates with von Willebrand disease. Thromb Haemost. 1992; 68 84-88
89 Mannucci P M, Tenconi P M, Castaman G, Rodeghiero R. Comparison of four virus-inactivated plasma concentrates for treatment of severe von Willebrand disease: a cross-over randomized trial. Blood. 1992; 79 3130-3137
90 Lethagen S, Berntorp E, Nilsson IM. Pharmacokinetics and hemostatic effect of different factor VIII-von Willebrand factor concentrates in von Willebrand's disease type III. Ann Hematol. 1992; 65 253-259
91 Menache D, Aronson D L, Darr F, Montgomery RR. The Cooperative Study Group . Pharmacokinetics of von Willebrand factor and factor VIIIC in patients with severe von Willebrand disease (type 3): estimation of the rate of factor VIIIC synthesis. Br J Haematol. 1996; 94 740-745
92 Ver Elst K, Van Vliet H HDM, Kappers-Klunne M C, Leebeek F WG. In vitro studies, pharmacokinetic studies and clinical use of a high purity double virus inactivated FVIII/VWF concentrate (Immunate) in the treatment of von Willebrand disease. Thromb Haemost. 2004; 92 67-74
93 Auerswald G, Eberspächer B, Engl W et al.. Successful treatment of patients with von Willebrand disease using a high-purity double-virus inactivated factor VIII/von Willebrand factor concentrate (Immunate). Semin Thromb Hemost. 2002; 28 203-213
94 Mannucci P M, Chediak J, Bymes W et al.. Treatment of von Willebrand disease with high-purity factor VIII/von Willebrand factor concentrate: a prospective, multicenter study. Blood. 2002; 99 450-456
95 Michiels J J, Berneman Z N, Van Der Planken M, Schroyens W, Budde U, Van Vliet HHDM. Bleeding prophylaxis for major surgery in patients with type 2 von Willebrand disease with an intermediate purity factor VIII-von Willebrand factor concentrate (Haemate-P). Blood Coagul Fibrinolysis. 2004; 15 323-330
96 Mannucci P M, Federici A B. Management of inherited von Willebrand disease. Baillieres Clin Haematol. 2001; 14 455-462
97 Mannucci P M. Treatment of von Willebrand's Disease. N Engl J Med. 2004; 351 683-694
98 Rodeghiero F, Castaman G. Treatment of von Willebrand disease. Semin Hematol. 2005; 42 29-35
99 Pasi K J, Collins P W, Keeling D M et al.. Management of von Willebrand disease: a guideline from the UK Haemophilia Centre Doctor's Organization. Haemophilia. 2004; 10 218-231
100 Gill J C, Ewenstein B M, Thompson A R, Mueller-Veltens G, Schwartz B A. The Humate-P Study Group. Successful treatment of urgent bleeding in von Willebrand disease with factor VIII/VWF concentrate (VWF:RCo) to measure potency and to guide therapy. Haemophilia. 2003; 9 688-695
101 Thompson A R, Gill J C, Ewenstein B M, Mueller-Veltens G, Schwartz BA. Successful treatment for patients with von Willebrand disease undergoing urgent surgery using factor VIII/VWF concentrate (Humate-P). Haemophilia. 2004; 10 42-51
102 Goudemand J, Mazurier C, Marey A et al.. Clinical and biological evaluation in von Willebrand's disease of a von Willebrand factor concentrate with low factor VIII activity. Br J Haematol. 1992; 80 214-221
103 Menache D, Aronson D L, Darr F, Montgomery RR. The Cooperative Study Group. Pharmacokinetics of von Willebrand factor and factor VIIIC in patients with severe von Willebrand disease (type 3): estimation of the rate of factor VIII synthesis. Br J Haematol. 1996; 94 740-745
104 Menache D, Aronson D L. New treatments of von Willebrand disease: plasma derived von Willebrand factor concentrates. Thromb Haemost. 1997; 78 566-570
105 Goudemand J, Negrier C, Ounmnoughene N, Sultan Y. Clinical management of patients with von Willebrand's disease with a VHP VWF concentrate: the French experience. Haemophilia. 1998; 4(suppl 3) 48-52

Jan Jacques MichielsM.D. Ph.D.

Goodheart Institute and Foundation, Hemostasis Thrombosis Science Center

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