Clinical Review

Von Willebrand Disease: Approach to Diagnosis and Management


 

References

Introduction

von Willebrand disease (VWD) is an inherited bleeding disorder caused by deficient or defective plasma von Willebrand factor (VWF). VWF is an adhesive multimeric plasma glycoprotein that performs 2 major functions in hemostasis: it mediates platelet adhesion to injured subendothelium via glycoprotein 1bα (GPIbα), and it binds and stabilizes factor VIII (FVIII) in circulation, protecting it from proteolytic degradation by enzymes. The current VWD classification recognizes 3 types (Table 1).1

In order to understand the role of the numerous laboratory investigations as well as the classification of VWD, it is important to review the structure and function of the VWF subunit. Bleeding symptoms, including mucocutaneous bleeding and excessive bleeding after surgery or trauma, reflect the defect in primary hemostasis. Treatment focuses on increasing VWF levels with desmopressin (1-deamino-8-D-arginine vasopressin, DDAVP) or clotting factor concentrates containing both VWF and FVIII (VWF/FVIII concentrate). Nonspecific treatment options include antifibrinolytic agents (tranexamic acid) and hormone therapy (oral contraceptive pill).

Prevalence

VWD is the most common inherited bleeding disorder. However, because VWF levels are highly variable and disease severity ranges from mild bleeding symptoms to severe or life-threatening bleeds, the reported prevalence of VWD depends on the diagnostic definition used. Two large epidemiologic studies have reported prevalence rates of approximately 1%.2,3 In these studies, healthy school-aged children were screened and diagnosed with VWD based on low VWF activity, measured as ristocetin cofactor, and a personal and family history of bleeding symptoms. At the other extreme, when considering patients whose bleeding symptoms are sufficiently severe to warrant referral to specialized centers, the reported prevalence of VWD ranges from 20 to 113 per million.4 These studies likely over- and underestimate clinically significant VWD. More recent studies suggest that the prevalence of VWD in individuals whose bleeding symptoms are significant enough to present to a primary care physician is approximately 0.1%.5 This figure is likely a more accurate estimate of the true prevalence of symptomatic VWD.

Although VWD is autosomally inherited, females are more likely to present with bleeding symptoms and be diagnosed because of increased exposure to bleeding challenges, such as menorrhagia and childbirth. VWD does not show any geographic or ethnic predilection, but there is an increased prevalence of the recessive forms, such as type 2N and type 3 VWD, in areas with high rates of consanguinity.

VWF Protein Structure and Function

The VWF gene is located on chromosome 12 at p13.3 and spans 178 kb comprising 52 exons.6 The expression of the VWF gene is tightly restricted to endothelial cells, platelets, and megakaryocytes, where VWF is stored in Weibel-Palade bodies and α-granules. VWF is a large multimeric glycoprotein with several important functional domains (Figure).

Extensive post-translational modifications, mediated by domains D3 and CK as well as the VWF propeptide, result in disulfide-linked multimers that can be greater than 20,000 kDa, while the VWF subunit is approximately 250 kDa. The high-molecular-weight (HMW) multimers are most effective in mediating platelet adhesion to the site of vascular injury; therefore, appropriate multimer formation is integral to VWF’s function. VWF is either secreted from local endothelial cells or recruited from the circulation to the site of endothelial injury, where it adheres to exposed collagen, predominately via the collagen-binding site in the A3 domain. Once immobilized, VWF is subjected to the high shear rates of the arterial circulation and undergoes a conformational change that exposes the platelet GPIbα binding site within the A1 domain.7 The high-affinity, rapid and reversible interaction between VWF and GPIbα tethers platelets to the endothelium where they roll until they are immobilized by integrin-mediated binding, which has slower binding kinetics. The RGD (Arg-Gly-Asp) sequence within the C4 domain also contributes to platelet adhesion by interacting with GPIIb-IIIa of activated platelets.8 ADAMTS13 (a disintegrin and metalloproteinase with a thrombospondin type 1 motif, member 13) is a plasma protease that cleaves circulating VWF in the A2 domain when VWF multimers unfold in response to sufficient shear, exposing the cleavage site within the A2 domain.9 VWF’s second role in hemostasis is fulfilled by the D’ and D3 domains, which bind and protect FVIII from proteolytic degradation, thereby prolonging its half-life. In the absence of VWF, FVIII has a half-life of approximately 2 hours, in contrast to a normal half-life of 12 to 20 hours when bound to VWF.4

Classification, Pathophysiology, and Genetics

The International Society of Thrombosis and Hemostasis (ISTH) classification of VWD was updated in 2006 (Table 1).1 It incorporates important aspects of clinical phenotype, pathophysiological mechanisms, and treatment considerations. The 3 categories are: type 1, which is a partial quantitative deficiency; type 2 with 4 subtypes (2A, 2B, 2M, and 2N), which is a qualitative defect; and type 3, which is a virtual absence of VWF. Although the diagnosis and categorization of VWD can be achieved with widely available laboratory testing, further subcategorization among type 2 VWD subtypes may require referral to a specialized laboratory. The current ISTH classification intentionally does not incorporate genotypic data. In type 2 or type 3 VWD disease, VWF mutations are identified in more than 90% of cases and are completely penetrant, whereas mutations are identified in only approximately 65% of type 1 VWD cases and have been associated with incomplete penetrance and variable expressivity.10 These studies suggest that type 1 VWD is an oligogenic disease with mutations in genes regulating secretion or clearance contributing to a VWD phenotype.

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