We have retrospectively evaluated the predictive markers of peri-

We have retrospectively evaluated the predictive markers of peri-operative major haemorrhages in a large single-centre population (n = 2455) of patients with VWF:RCo <50 IU dL−1 and type 1 VWD, possible type TSA HDAC supplier 1 and type 2 VWD. Diagnostic criteria for type 1 and possible type1 (VWF:RCo 15–30 IU dL−1 and 31–49 IU dL−1, respectively),

VWF:RCo/VWF:Ag ratio >0.6 and type 2 with VWF:RCo/VWF:Ag <0.6 were used. For each patient, the severity of each symptom was summarized using the BS system ranging from 0 to 3 [38], according to ISTH recommendations [39], and taking into account the most severe episode for each symptom [40]. The BS was considered useful for the identification of a significant bleeding history (≥5 in females and ≥3 in males) for the diagnosis of type 1 VWD. This approach can also be useful in all VWD types [41,42]. Patient characteristics of group A (without surgical bleeding) and

group VX-809 concentration B (with surgical bleeding) are shown in Table 2. Major surgical bleeding appeared in 26% of all type1 patients (32.6% type1 and 24.8% possible type1) and 54.9% of type 2. Considering surgeries, major haemorrhage was observed in 17.8% of all type1 and 50% of type 2 (Table 3). No significant differences were observed in family history, blood group, age, gender, BS, the number of bleeding sites (Table 1) and laboratory parameters (Table 4), between groups A and B. FVIII levels were not useful as predictors of postoperative bleeding. In possible type 1, group B, a higher frequency of bleeding after MCE tooth extraction (Table 5) and a higher BS in females were found. Postpartum bleeding was the most frequent symptom in type 2 VWD, although not significant. Caesarean section and adeno-tonsillectomy showed the highest frequency of major haemorrhage. Personal bleeding history, especially bleeding after tooth extraction in type 1 VWD [43], and postpartum haemorrhage in type 2 and the type of surgery appear to be predictive markers of major postoperative

haemorrhage. The relative risk (RR) between type 1 and 2 was as expected. Possible type 1 VWD patients showed similar risk of peri-operative major bleeding compared with type 1, again emphasizing the superiority of symptoms over laboratory parameters. Neither the family history nor laboratory parameters could anticipate surgical bleeding. The authors stated that they had no interests which might be perceived as posing a conflict or bias. “
“Although it has been suggested that switching of factor VIII (FVIII) products may increase inhibitor formation this is disputed. Half of UK patients changed rFVIII brands because of national contracting in 2010, presenting an opportunity to compare inhibitor incidence of switchers with non-switchers.

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