Von Willebrand Diseases Clinical Trial
Official title:
Multicenter Retrospective Study From 5 Hemostasis Treatment Centers in Western France: Severe Hemorrhagic Treated Occurrences' Patterns and Global Substitutive COagulation Factors THerapy in the Inherited Von WILLebrand Disease
Von Willebrand disease (VWD) is the most common constitutional bleeding disorder in the
world, caused by missing or defective von Willebrand factor (VWF). In France, VWD affects
approximatively 7,000 patients.
There are many types of VWD. The severest forms are characterized by the occurrence of
extremely serious bleedings, requiring in-stays with clotting factors (CF) treatments in
specialized hospital units and/or an ambulatory substitutive therapy; both of them are highly
expensive.
In France, Hemostasis Treatment Centers (HTC) have the opportunity to record these kinds of
data in a database called NHEMO (Net-Hemostasis = care database for constitutional bleeding
disorders). Further ahead, the data can be coded, dumped into and extracted from the research
database BERHLINGO and analyzed.
The HOPSCOTcH-WILL study will be a retrospective, non-interventional, multicenter (national)
cohort study & will provide an overview of the real-life management of patients with VWD in
western France requiring a substitutive treatment with VWF, as well as a description of the
characteristics of their hemorrhagic events.
Model : Observationnal, real world evidence study. Time Horizon : 2015-2018. HTC (France):
Western University Hospitals (BERHLINGO network) = Nantes University Hospital (promotion),
Angers University Hospital, Brest University Hospital, Le Mans Regional Hospital & Rennes
University Hospital
von Willebrand Disease (vWD) represents the most common autosomal inherited bleeding
disorders with a prevalence up to 1%; nevertheless the clinical relevant patients represent
only 0.01% of the population.
vWD is caused by a deficiency and/or abnormality of von Willebrand factor (VWF), inhibiting a
satisfactory hemostasis. vWD is usually classified into three main types according to
quantitative (Types 1 and 3) or qualitative (Types 2A, 2B, 2M, 2N) deficiencies. Type 3
patients have the highest bleeding risk, type 2 patients are intermediate and type 1 patients
have the lowest bleeding risk. Beyond the typology, VWF levels, and therefore the hemorrhagic
exposition, are also notably influenced by physiological (age, exercise, pregnancy, gene
mutations) or pathological (inflammation and cancer) variables. Furthermore, blood group
plays a major role in plasma VWF levels; in fact they are 25%-35% lower in type-0 individuals
than in non-0. As a result, the clinical and biological identification of vWD can be
extremely challenging and may lead to a delay in the diagnosis.
In vWD, the clinical manifestations are essentially mucosal bleeding symptoms. Epistaxis,
menorrhagia, easy bruising, gingival bleeding are flagrant manifestations of the disease and,
despite the mostly small somatic impact in the majority of patients; they may significantly
affect the quality of life. Nevertheless, severe affected patients may face upper
consequences: gastrointestinal (GI) bleeding may be particularly frequent and difficult to
manage, and they are as well at high risk to develop major and life-threatening bleeds after
surgical procedures, even after minor ones such as tooth extraction.
To guarantee the best medical care management, VWD patients are followed in specialized rare
disease centers, both for the ambulatory follow-up and the hospitalizations & outpatient
aftercare. These hospital structures are the only ones authorized to prescribe and dispense
in- & outpatients' substitutive treatments.
Indeed, the optimal effective treatment of the disorder is the replacement of VWF by using
VWF concentrate obtained by fractionation of human plasma; in emergency, recombinant or
plasma-derived factor VIII (FVIII) can be added to the VWF. In case of history of inhibitors,
high dose of FVIII or by-passing agents can also be used. The current treatment for vWD
involves intravenous injections of VWF that are either given on demand in response to a
bleeding event or as a prophylactic therapy that is administered 2 to 4 times a week.
Numerous studies have shown the efficacy of prophylactic therapy in severe patients, but the
investigators lack data about surgery procedures and perioperative management. Moreover,
regardless of the small amounts of patients, those treatments remain quite costly and may
represent an economic burden for the Assurance Health System.
Due to the future availability of the first recombinant VWF, the investigators need a better
understanding of the current French practices. The lack of literature on the topic is
undeniably blatant and the few relevant papers concerned specific pd-VWF concentrates; no RWD
publication has been identified for the specific French cohort. The heterogeneity of VWD
concentrates brands and VWD types make the development of personalized care quite difficult
in this context and more information is needed, especially for the peri-operative treatment.
The economic evaluations usually focus on prophylaxis treatments or a specific concentrate,
neglecting a significant percentage of patients.
The objective of our 4-years retrospective study HOPSCOTcH-WILL is to provide an accurate and
detailed account of current vWD therapeutic management by collecting real-life data on
hemorrhagic treated events in 5 Western French HTC (Angers, Brest, Le Mans, Nantes & Rennes).
The data will be retrospectively recorded during 48 months from 2015 to 2018 for patients
followed in the 5 HTC involved in the study. A focus will be done on GI episodes and
surgeries which are the most at risk hemorrhagic events in vWD.
HOPSCOTcH-WILL could be considered as reliable photography of Western French HTC at a
particular time. Therefore, and especially with the launch of a new recombinant VWF, it is
particularly important to get a clear state-of-the-art and to assess the economic impact for
the French Health System.
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