The clinical presentation of a severe factor deficiency is sponta

The clinical presentation of a severe factor deficiency is spontaneous

bleeding or excessive bleeding following minor trauma in otherwise healthy infants. ICH may be the presenting symptom. Facial purpura following birth is usually associated with severe platelet dysfunction or thrombocytopenia. Oral mucous membrane bleeding is common for thrombocytopenic infants; however, gum bleeding and epistaxis hardly ever present in neonates. Joint haemarthroses, typical for severe factor deficiencies, rarely occur before ambulation. Persistent oozing from the umbilical stump is typical for infants click here with defective fibrinogen production or function and FXIII deficiency. The correct diagnostic assays and appropriate management vary according to the underlying basic disorder. Most forms of von Willebrand’s disease (VWD) cannot be diagnosed in newborns, as physiological concentrations of VWF and the proportion of high molecular weight multimers of VWF are increased [10]. Thus, type 3 VWD (the severe form, complete factor deficiency) can be diagnosed in neonates, whereas the diagnoses of mild or qualitative deficiencies (type 1 or 2 VWD,

respectively) are troublesome and require repeated testing for confirmation in later infancy. Severe FXI deficiency, a genetic disorder that prevails among Ashkenazi Jews, can present in newborns following haemostatic challenges, such as circumcision [35]. As physiological FXI levels may be low after birth, infants with borderline FXI levels EPZ-6438 solubility dmso should be retested prior to any elective surgical procedures, for

treatment of bleeding episodes, or during surgery and treated accordingly, if required. Severe homozygous FVII deficiency (plasma levels <0.03 units mL−1) can present with ICH following birth (r). Milder deficiencies are usually diagnosed at older ages, as a result of lower boundaries of the vitamin K-dependant FVII at birth as well as more selleck kinase inhibitor subtle bleeding manifestations. Deficiencies of factor XII, prekalikrein and high molecular weight kininogen are of no clinical significance in newborns. Rare autosomal recessive homozygous severe FV deficiency (diagnosed by plasma concentrations <0.1 units mL−1) as well as homozygous severe FII or FX deficiencies (plasma concentrations lower than 0.2 and 0.1 units mL−1, respectively) can cause haemorrhagic symptoms. The exact prevalence of these disorders is unknown. All infants suffering these disorders demonstrate abnormal coagulation screening tests, with prolonged PT and PTT. Whereas FV deficiency is easily diagnosed in neonates, FII or FX (both vitamin K-dependant factors) borderline-low levels may overlap with neonatal physiological levels, making the diagnosis difficult.

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