Abstract
BackgroundVon Willebrand disease (VWD) is not uncommon in Taiwan. In type 2 or type 3 VWD hemorrhagic symptoms are severer and laboratory data relatively more distinctive. De novo mutation and somatic mosaicism of type 2 VWD gene were rarely reported. Therefore clinical, laboratory and genetic studies of only type 2A, 2B and 2M VWD will be presented and issues of de novo mutation and somatic mosaicism will be explored.MethodsFifty-four patients belonging to 23 unrelated families from all around the country in whom type 2 VWD exclusive of type 2N has been diagnosed not only by clinical and routine laboratory studies but also by genetic confirmation during 1990–2015 were investigated. A novel technique named amplification refractory mutation system-quantitative polymerase chain reaction (ARMS-qPCR) was used to confirm the presence of somatic mosaicism. Informed consent was obtained for study.Results De novo mutation was identified in 4 families among 15 families (26.7 %) in whom family members including parents were available for examination. All their parents were free from bleeding symptoms and had no similar mutation as their respective affected daughter.An interesting example of somatic mosaicism of VWF gene mutation was found in a large family with type 2A VWD. The father carrying a mutated VWF gene, p.Arg1597Trp, transmitted this mutation to his 3 daughters, 1 son, 3 granddaughters and 2 grandsons. However, the father had normal laboratory findings and experienced no abnormal bleeding, while his offspring who inherited the mutation showed abnormal laboratory findings compatible with type 2A VWD and had history of abnormal bleedings. ARMS-qPCR revealed that the father had only 25.5 % mutant in his blood cells and 31.1 % mutant in his oral mucosal cells, while all his offspring had about 49 % mutant in their blood cells.Conclusion De novo mutation of type 2 VWD gene was identified in 4 out of 15 families (26.7 %) examined. Since only one child was affected in each family, germline mosaicism was not likely. A somatic mosaicism of type 2A VWD gene was documented in a big family by a newly in-house developed technique ARMS-qPCR.
Highlights
Von Willebrand disease (VWD) is not uncommon in Taiwan
Eleven different previously reported mutations of the von Willebrand factor (VWF) gene based on the ISTH-SSC VWF database, as accessed in June 2016, was identified in the 16 index patients with type 2 VWD including 6 mutations from 8 type 2A VWD patients: p.Arg1374His, p.Ser1506Leu, p.Cys1272Gly, p.Arg1597Trp, p.Cys1272Arg and p.Ile16 28Thr; 3 mutations from 5 type 2B VWD patients: p.Arg1306Trp, p.Val1316Met and p.Arg1308Cys; and 2 mutations from 3 type 2M VWD patients: p.Arg1374Cys and p.Arg1315Cys
Six different novel mutations of the VWF gene according to the ISTH-SSC VWF database was identified in the 7 index patients with type 2 VWD including 3 mutations from 3 type 2A VWD patients: p.Leu1696del, p.Glu1519del and p.Ala1500Val; and 3 mutations from 4 type 2M VWD patients: c.53121 ~ −2del AG, p.Leu1276Arg and c.3538 + 1G → C
Summary
In type 2 or type 3 VWD hemorrhagic symptoms are severer and laboratory data relatively more distinctive. Clinical, laboratory and genetic studies of only type 2A, 2B and 2M VWD will be presented and issues of de novo mutation and somatic mosaicism will be explored. Willebrand disease (VWD) is a genetically and clinically heterogeneous inherited hemorrhagic disorder caused by a deficiency or dysfunction of von Willebrand factor (VWF). In type 2 and type 3 VWD, hemorrhagic symptoms are severer and laboratory data relatively more distinctive, which lead to diagnose the patient [3, 4]. Laboratory and genetic studies of only type 2 VWD exclusive of type 2N seen in Taiwan were investigated, which demonstrated a not-souncommon occurrence of de novo mutation. In this study we cited an interesting example from a big family suffered from type 2A VWD, in which somatic mosaicism of the VWF gene mutation will be presented
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