Details

Autor(en) / Beteiligte

• Pérez‐Rodríguez, Almudena
• Batlle, Javier
• Pinto, Joana Costa
• Corrales, Irene
• Borràs, Nina
• Garcia‐Martínez, Iris
• Cid, Ana Rosa
• Bonanad, Santiago
• Parra, Rafael
• Mingot‐Castellano, María Eva
• Navarro, Nira
• Altisent, Carmen
• Pérez‐Montes, Rocío
• Moretó, Ana
• Herrero, Sonia
• Soto, Inmaculada
• Mosteirín, Nuria Fernández
• Jiménez‐Yuste, Víctor
• Jacob, Aurora de Andrés
• Fontanes, Emilia
• Mateo, José
• Quismondo, Nerea Castro
• Batlle, Fernando
• Vidal, Francisco
• López‐Fernández, María Fernanda

Titel

Type 2N VWD: Conclusions from the Spanish PCM‐EVW‐ES project

Ist Teil von

• Haemophilia : the official journal of the World Federation of Hemophilia, 2021-11, Vol.27 (6), p.1007-1021

Ort / Verlag

England: Wiley Subscription Services, Inc

Erscheinungsjahr

2021

Link zum Volltext

Quelle

MEDLINE

Beschreibungen/Notizen

• Introduction Type 2N von Willebrand disease (VWD) is characterized by a decreased affinity of von Willebrand factor (VWF) for factor VIII (FVIII). Abnormal binding of FVIII to VWF (VWF:FVIIIB), results in low FVIII plasma levels, which can lead to a misdiagnosis of mild haemophilia A. Accurate diagnosis of type 2N VWD is essential for appropriate genetic counselling and therapy. This disease can be distinguished from haemophilia A by in vitro assays (measurement VWF:FVIIIB activity) and/or genetic analysis. Aim To identify the current challenges in the diagnosis and treatment of this type of VWD and provide an in‐depth description of the phenotypes and mutations identified. Results Twenty‐eight patients had at least one type 2N mutation, and 13 of these had a type 2N mutation combined with other variations. Three type 2N mutations were detected: p.Arg816Trp, p.Arg854Gln, and p.Arg763Ser. Two of these are the most frequently described mutations worldwide. This mutational spectrum differs from the broad spectrum seen in neighbouring France, where at least eight distinct 2N mutations have been found. In the PCM‐EVW‐ES cohort, 11 asymptomatic type 2N carriers with borderline FVIII plasma levels would probably have been excluded if the evaluation had been based on clinical and laboratory data only. Likewise, three patients with a severe phenotype would have been classified as homozygous for a 2N mutation if only the phenotype study had been performed. Conclusion The high detection yield and affordability of next‐generation sequencing support the use of this technology as a first‐line diagnostic tool in this setting.