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We thank Shetty et al. ,[1][1] for their comments about the relationship between the type of mutation and clinical phenotype in hemophilia. As clearly mentioned in our manuscript,[2][2] the higher prevalence of missense mutations in hemophilia B compared to hemophilia A could be one of the most

haematologica

The higher prevalence of missense mutations in hemophilia B compared to hemophilia A could be important in determining a milder clinical phenotype in patients with severe hemophilia B