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NCT02460458 Clinical Trial

Type 3 Von Willebrand International Registries Inhibitor Prospective Study

Type 3 Von Willebrand's Disease Clinical Trial

3WINTERSIPSEXT

Official title:
Type 3 Von Willebrand International Registries Inhibitor Prospective Study

Clinical Trial Details — Status: Active, not recruiting

Administrative data
NCT number NCT02460458
Other study ID # ABB-11-01
Secondary ID
Status Active, not recruiting
Phase
First received
Last updated
Start date November 5, 2012
Est. completion date December 2022

Study information
Verified date March 2022
Source Fondazione Angelo Bianchi Bonomi
Contact n/a
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

International Registries and Prospective Study on Type 3 Von Willebrand's Disease (VWD3), aimed to assess number, types and risk factors for bleeding and the efficacy and safety of plasma-derived and/or recombinant Von Willebrand Factor (VWF) concentrates used to treat VWD patients.

Description:

Von Willebrand's Disease (VWD) is the most common inherited bleeding disorder, characterized by a quantitative and/or qualitative deficiency of Von Willebrand Factor (VWF), that plays a major role in early phases of hemostasis. Type 3 Von Willebrand's Disease (VWD3) is due to virtually complete deficiency of VWF and, for this reason, has been also described as "severe VWD". Recurrent Gastro-Intestinal Bleeds (GIB) is one of the most challenging complications encountered in the management of patients with VWD. The commonest cause is angiodysplasia (ANGDYS), but often no cause is identified due to the difficulty in making the diagnosis. In recent years, research from several laboratories has identified multiple roles for VWF in the control of vascular function. Globally, these findings provide the first possible explanation for the presence of ANGDYS in patients with VWD. These vascular malformations in the gastrointestinal (GI) tract are characterized by fragile, leaky mucosal vessels. Combined with the hemostatic dysfunction, these can lead to severe intractable bleeding including GIB. VWD3 is inherited as a recessive trait and heterozygous relatives have mild or no bleeding symptoms. Even if the prevalence of VWD3 is very low, the highest rate is found in Iran and the lowest in southern Europe. However, the actual prevalence of VWD3 is still unknown in most countries, due to the lack of retrospective or prospective studies. Although rare, VWD3 is of major interest because of its severe clinical presentation, the need for replacement therapy with plasma-derived and/or recombinant VWF concentrates and the risk of occurrence of anti-VWF inhibitors after the infusion of VWF concentrates, for which risk factors have not been systematically determined. The major objectives of the study are: to create an international network among European and Iranian Centers (ratio 1:1), the prospective enrollment of at least 250 VWD3 patients using a common database online, the collection of detailed information about previous bleedings and exposure to plasma-derived and/or recombinant VWF concentrates, the use of bleeding severity score of VWD3 calculated with a common questionnaire, the collection of plasma and DNA samples from all the identified VWD3 patients enrolled for centralized analyses, the confirmation of the local VWD3 diagnosis using centralized tests, Evaluation of VWF gene defects, VWF phenotype and risk of anti-VWF inhibitors through common methods, the evaluation of potential correlations between phenotypic results (including markers of angiogenesis) and GIB occurrence, the objective evaluation of severity of GIB in VWD3 patients, the assessment of frequency and sites of bleeding in VWD3 patients followed-up for 2 prospective observation periods (2 years each: 2017-2018 and 2020-2022), the efficacy assessment of the plasma-derived and/or recombinant VWF concentrates used to treat VWD3 (on demand versus prophylaxis) using the most objective criteria for efficacy during 2 prospective observation periods (2 years each: 2017-2018 and 2020-2022), the evaluation of the efficacy and safety of plasma-derived and/or recombinant VWF concentrates in the treatment of GIB during 2 prospective observation periods (2 years each: 2017-2018 and 2020-2022), in comparison to the use of anti-angiogenetic agents within the standard clinical setting. To these purposes, a cohort of at least 250 patients with diagnosis of VWD3 will be enrolled using homogenous and standardized criteria. The work planned to achieve the objectives of the project will be divided in three parts: - the first part deals with standardized criteria for enrolment and collection of retrospective clinical and laboratory data, to be confirmed by centralized laboratories; - the second part involves a further characterization of clinical and laboratory parameters, collected in the retrospective phase, including prevalence of anti-VWF inhibitors, advanced laboratory tests to further identify VWD3, mutations analyses of the VWF gene; - the third part of the study is divided in two parts: a first prospective observation and a second prospective observation. The third part for the first time deals with the prospective clinical observation in a large cohort of VWD3 patients all previously well characterized by an international panel of experts.

Recruitment information / eligibility
Status Active, not recruiting
Enrollment 265
Est. completion date December 2022
Est. primary completion date October 2022
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria: - Male and female of any age, including infants, children, adolescent and adults - Informed Consent obtained (parents should sign for patients < 18 y.o.) - Previous Diagnosis of VWD3 (VWF Antigen: undetectable or <5 U/dL) - Detailed information on inherited pattern, history of bleeding, previous exposure to blood products - Availability of plasma and DNA samples Exclusion Criteria: • VWD3 patients who may not be available for follow-up

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
Von Willebrand Factor
Replacement therapy with plasma-derived and/or recombinant VWF concentrates on-demand or under prophylaxis therapeutic scheme.

Locations
Country Name City State
Finland Helsinki University Central Hospital, Department Internal Medicine, Coagulation Disorders, at Haematology and Laboratory Services Helsinki
France Institut d'Hématologie - Hôpital Cardiologique - University of Lille - Haematology Department Lille Cedex
France Centre Régional de Traitement de l'Hémophilie - Laboratoire d'Hématologie Nantes Cedex 1
Germany University Clinic Bonn - Institute of Experimental Haematology & Transfusion Medicine Bonn
Germany University Children's Hospital - Department of Pediatric Hematology and Oncology Hamburg
Germany Department of Haematology, Haemostasis, Oncology and Stem Cell Transplantation - Hannover Medical School - Haemophilia Care Centre Hannover
Hungary St. Istvan & St. Laszlo Hospital of Budapest - Hematology and Stem Cell Transplantation Budapest
Iran, Islamic Republic of Ahvaz Jundishpur University of Medical Sciences - Research Center for Thalassemia & Hemoglobinopathy - Division of Hematology & Oncology Ahvaz
Iran, Islamic Republic of Seid-ol-Shohada Hospital - Hemophilia Center - Esfahan University of Medical Science Esfahan
Iran, Islamic Republic of Hemophilia- Thalassaemia Center of Mashhad (Sarvar Clinic) - Mashad University of Medical Science Mashhad
Iran, Islamic Republic of Nemazee Hospital Hemophilia Center - Shiraz University of Medical Science Shiraz
Iran, Islamic Republic of Iranian Hemophilia Comprehensive Treatment Centre - Iranian Hemophilia Society Tehran
Iran, Islamic Republic of Mofid Comprehensive Care Centre for Children with Hemophilia - Shahid Beheshti University of Medical Science Tehran
Iran, Islamic Republic of Thrombosis Hemostasis Research Center - Vali-Asr Hospital - Emam Khmeini Complex Hospital - Tehran University of Medical Science Tehran
Italy Azienda Ospedaliera Policlinico Consorziale di Bari - Unità Operativa Semplice di Emostasi e Trombosi Bari
Italy Azienda Ospedaliera Universitaria Careggi - Agenzia per l'Emofilia - Centro di Riferimento Coagulopatie Congenite Firenze
Italy Centro Emofilia e Trombosi - Fondazione Angelo Bianchi Bonomi - IRCCS Ospedale Ca' Granda - Dip. di Medicina Interna - Università degli Studi di Milano Milano
Italy Dipartimento di Biotecnologie Cellulari ed Ematologia - Università "Sapienza" di Roma - Policlinico Umberto I Roma
Italy Dipartimento di Terapie Cellulari ed Ematologia - Centro Malattie Emorragiche e Trombotiche - Ospedale San Bortolo Vicenza
Netherlands Leiden University Medical Center - Department of Hematology - Hemostasis and Thrombosis Center Leiden
Netherlands Erasmus Medical Center - Department of Hematology Rotterdam
Spain Complejo Hospitalario Universitario de A Coruña - Servicio de Hematología y Hemoterapia A Coruña
Spain Hospital Universitari General Vall d'Hebron - Unidad de Hemofilia Barcelona
Sweden Lund University - Centre for Thrombosis and Haemostasis - Skane University Hospital Malmö
United Kingdom Central Manchester University Hospital NHS Foundation Trust - Manchester Royal Infirmary - Manchester Royal Eye Hospital Manchester

Sponsors (2)
Lead Sponsor Collaborator
Fondazione Angelo Bianchi Bonomi Sintesi Research Srl

Countries where clinical trial is conducted

Finland,  France,  Germany,  Hungary,  Iran, Islamic Republic of,  Italy,  Netherlands,  Spain,  Sweden,  United Kingdom, 

References & Publications (128)

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Castaman G, Eikenboom JC, Lattuada A, Mannucci PM, Rodeghiero F. Heightened proteolysis of the von Willebrand factor subunit in patients with von Willebrand disease hemizygous or homozygous for the C2362F mutation. Br J Haematol. 2000 Jan;108(1):188-90. — View Citation

Castaman G, Federici AB, Tosetto A, La Marca S, Stufano F, Mannucci PM, Rodeghiero F. Different bleeding risk in type 2A and 2M von Willebrand disease: a 2-year prospective study in 107 patients. J Thromb Haemost. 2012 Apr;10(4):632-8. doi: 10.1111/j.1538-7836.2012.04661.x. — View Citation

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Cattaneo M, Federici AB, Lecchi A, Agati B, Lombardi R, Stabile F, Bucciarelli P. Evaluation of the PFA-100 system in the diagnosis and therapeutic monitoring of patients with von Willebrand disease. Thromb Haemost. 1999 Jul;82(1):35-9. — View Citation

Cattaneo M, Moia M, Delle Valle P, Castellana P, Mannucci PM. DDAVP shortens the prolonged bleeding times of patients with severe von Willebrand disease treated with cryoprecipitate. Evidence for a mechanism of action independent of released von Willebrand factor. Blood. 1989 Nov 1;74(6):1972-5. — View Citation

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Federici AB, Barillari G, Zanon E, Mazzucconi MG, Musso R, Targhetta R, Mannucci PM. Efficacy and safety of highly purified, doubly virus-inactivated VWF/FVIII concentrates in inherited von Willebrand's disease: results of an Italian cohort study on 120 patients characterized by bleeding severity score. Haemophilia. 2010 Jan;16(1):101-10. doi: 10.1111/j.1365-2516.2009.02088.x. Epub 2009 Oct 6. — View Citation

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Federici AB, Mannucci PM, Castaman G, Baronciani L, Bucciarelli P, Canciani MT, Pecci A, Lenting PJ, De Groot PG. Clinical and molecular predictors of thrombocytopenia and risk of bleeding in patients with von Willebrand disease type 2B: a cohort study of 67 patients. Blood. 2009 Jan 15;113(3):526-34. doi: 10.1182/blood-2008-04-152280. Epub 2008 Sep 19. — View Citation

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Goudemand J, Scharrer I, Berntorp E, Lee CA, Borel-Derlon A, Stieltjes N, Caron C, Scherrmann JM, Bridey F, Tellier Z, Federici AB, Mannucci PM. Pharmacokinetic studies on Wilfactin, a von Willebrand factor concentrate with a low factor VIII content treated with three virus-inactivation/removal methods. J Thromb Haemost. 2005 Oct;3(10):2219-27. — View Citation

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Gupta PK, Saxena R, Adamtziki E, Budde U, Oyen F, Obser T, Schneppenheim R. Genetic defects in von Willebrand disease type 3 in Indian and Greek patients. Blood Cells Mol Dis. 2008 Sep-Oct;41(2):219-22. doi: 10.1016/j.bcmd.2008.03.004. Epub 2008 May 16. — View Citation

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* Note: There are 128 references in allClick here to view all references

Outcome
Type Measure Description Time frame Safety issue
Primary Centralized Factor VIII (FVIII) Procoagulant Activity (FVIII:C) Laboratory Test for Type 3 Von Willebrand's Disease (VWD3) Diagnosis Measurement of the Factor VIII (FVIII) Procoagulant Activity (FVIII:C) in the blood through one-stage clotting test. Only patients with FVIII:C less or equal to 5 IU/dL were considered for the analysis. 12 months (confirmatory phase)
Primary Centralized Von Willebrand Factor Antigen (VWF:Ag) Laboratory Test for Type 3 Von Willebrand's Disease (VWD3) Diagnosis Measurement of the amount of Von Willebrand Factor (VWF) protein in the blood through Von Willebrand Factor Antigen (VWF:Ag) test. Only patients with VWF:Ag less or equal to 5 IU/dL were considered for the analysis. 12 months (confirmatory phase)
Primary Centralized Factor VIII (FVIII) Amidolytic Activity (FVIII:Am) Laboratory Test for Type 3 Von Willebrand's Disease (VWD3) Diagnosis Measurement of Factor VIII (FVIII) Amidolytic Activity (FVIII:Am) in the blood through chromogenic test. Only patients with FVIII:Am less or equal to 5 IU/dL were considered for the analysis. 12 months (confirmatory phase)
Primary Centralized Factor VIII (FVIII) Antigen (FVIII:Ag) Laboratory Test for Type 3 Von Willebrand's Disease (VWD3) Diagnosis Measurement of the amount of Factor VIII (FVIII) protein in the blood through FVIII:Ag test. Only patients with FVIII:Ag less or equal to 5 IU/dL were considered for the analysis. 12 months (confirmatory phase)
Primary Centralized Von Willebrand Factor (VWF) Multimer Analysis for Type 3 Von Willebrand's Disease (VWD3) Diagnosis Multimer analysis of Von Willebrand Factor (VWF) was carried out by electrophoresis of blood samples collected by investigational sites. The number of patients belonging of each multimer profile group (1 - Homozygotes / 2 - Only Protomers / 3 - 2-4 Bands) was calculated. The qualitative evaluation of VWF multimers is part of the diagnostic process of VWD3. 12 months (confirmatory phase)
Primary Centralized Von Willebrand Factor (VWF) Propeptide Laboratory Test for Type 3 Von Willebrand's Disease (VWD3) Diagnosis Measurement of Von Willebrand Factor (VWF) Propeptide levels in the blood through VWF Propeptide test. 12 months (confirmatory phase)
Primary Centralized Molecular Type 3 Von Willebrand's Disease (VWD3) Diagnosis Through DNA Analysis Evaluation of the presence of Von Willebrand Factor (VWF) gene defects (confirmation or screening for the first time). 12 months (confirmatory phase)
Primary Record of Bleeding Episodes Bleeding: severity, start date, stop date; Treatment: Product name, start date, stop date, Total IU, Total of Exposure Days (ED). 24 months (first prospective phase) + 24 months (second prospective phase)
Primary Adverse Events Record of all adverse events occurred during the prospective phase of the study. 24 months (first prospective phase) + 24 months (second prospective phase)
Primary Type of Von Willebrand Factor / Factor VIII (VWF/FVIII)-Containing Concentrates in Use Record of any Von Willebrand Factor / Factor VIII (VWF/FVIII)-containing concentrates used and currently in use, including the current schedule type of treatment. 24 months (first prospective phase) + 24 months (second prospective phase)
Secondary Patients Experiencing Allergic Reactions During Use of Von Willebrand Factor (VWF)-Containing Concentrates Record of any allergic and anaphylactic reactions occurred in the past due to the use of any Von Willebrand Factor (VWF) concentrate and the date of onset. 24 months (retrospective phase)
Secondary Number of Participants With Previous Use of Blood Products Record of any product used during the retrospective phase (collected type of blood products/Von Willebrand Factor (VWF) concentrate, year of first exposure, units used). 24 months (retrospective phase)
Secondary Number of Patients With Available Local Laboratory Test for Anti-Von Willebrand Factor (Anti-VWF) Antibodies Evaluation of the titre of Anti-Von Willebrand Factor (anti-VWF) Antibodies through Bethesda Test. 24 months (retrospective phase)
Secondary Local Laboratory Tests for Type 3 Von Willebrand's Disease (VWD3) Diagnosis (Composite) Number of patients for who the following tests have been performed:
Hemoglobin (mmol/L), Hemagglutination Titer (HT) (%), Mean Corpuscular Volume (MVC) (fl), Leucocytes (E9/L), Neutrophils (%), Basophils (%), Eosinophils (%), Lymphocytes (%), Platelet Count (E9/L), Mean Platelet Volume (MPV) (fl), Prothrombin Time (sec), Partial Thromboplastin Time (PTT) (sec), Partial Thromboplastin Time Mix 50:50 (PTT mix 50:50) (sec), Ferritin (ug/l), Bleeding Time (min:sec), Closure Time (sec), Collagen/ADP (sec), Collagen/Epinephrine (sec); Factor VIII Procoagulant Activity (FVIII:C) (IU/mL), Von Willebrand Factor Ristocetin Cofactor (VWF:RCo) (IU/mL), Won Willebrand Factor Antigen (VWF:Ag) (IU/mL).		 24 months (retrospective phase)