Coagulation Disorders Corrina Mc Mahon
Laboratory investigations PT: VII, X, V APTT; XII, XI, IX, VIII TT; Fibrinogen D dimers; fibrin breakdown
Case 1 4 yr old boy URTI 2 weeks ago Sudden onset bruising/petechiae PH: Nil FH: Nil Physical examination:
Investigations FBC: Hb 11g/dl; WCC 8x10^/l; Platelets <10x10^9/l PT 14 sec ; APTT 33 sec; Fibrinogen 2.0g/l Treatment options: Nil; IVIg; Steroids Outcome: 90% recovery; 10% chronic
Congenital Thrombocytopenia Dysfunctional platelets Bernard Soulier Grey platelet syndrome Wiskott-Aldrich syndrome Normal Platelet function May-Hegglin TAR
Case 2 Newborn infant Intracranial Haemorrhage No dysmorphic features 1st child No liver/spleen palpable FBC Hb 18.5g/dl WCC 10 x x 109/l /l Platelets 10 x 109/l /l Coagulation screen PT 15 sec. (13-16) APTT 41 sec (28-36)
Differential diagnosis Infection DIC Immune Thrombocytopenia Alloimmune Isoimmune Congenital Thrombocytopenia TAR syndrome Wiscott Aldrich Syndrome Von Willebrands disease Type 2B A-V malformations
Alloimmune Thrombocytopenia Incidence 1:1000-5000 births IgG antibodies HPA1a 80% HPA5b 15% 50% occur in 1st pregnancy Bleeding can be in utero or after birth Treatment Platelets IVIg ?Steroids
Isoimmune Thrombocytopenia Maternal anti-platelet IgG Placental Passage Thrombocytopenia nadir ~5days post-partum History & examination of mother Treatment IvIg ± steroids
Disseminated Intravascular Coagulopathy Infection Symptoms and Signs Petechiae Bruising Bleeding Laboratory results Anaemia Thrombocytopenia ↑PT/ ↑APTT/↓Fibrinogen/ ↑d dimers
Haemophila Inherited Bleeding Disorder Factor VIII/FIX deficiency X-Linked Inheritance Carrier XX may have low levels Spontaneous mutation
Inheritance of Haemophilia
Life Expectancy In Haemophilia
Bleeding problems in Haemophilia Factor Level Type of Bleed <1% Spontaneous/severe 2%-5% Mild trauma/ occasionally spontaneous >5% Trauma/Surgery
Intracranial Bleeds At Birth Injury Admission Factor Concentrate Scanning Observation Neurosurgery
Forearm Bleed
Joint bleed Synovial inflammation and hyperaemia Synovial overgrowth and Bone resorption Further Bleed Joint Destruction
Joint Bleeding
Chronic Joint Bleeding
The role of prophylaxis in the prevention of joint injury Lofqvist, Nilsson et al ( Journal Int. Medicine May 1997): 34 patients aged 7-22yrs. Age at commencement of prophylaxis - 1-4.5yrs. 79% had no joint problems and the rest had no deterioration in joint abnormalities. Liesner,Khair, Hann, ( BJH Mar 1996) 27 children aged 1.3-15.9yrs. No. of bleeds/yr pre-prophylaxis-14.5 and post - 1.5. 20 children had evidence of arthropathy which improved on prophylaxis.
Prophylaxis The Irish Data (1992-1997) Bleeds/yr, pre-prophylaxis, 9.5-106 (mean 38) Bleeds/yr, post-prophylaxis, 0-9 (mean 3.5) Development of inhibitors, 2 - low level (<1Bu) and transient (< 1 year)
Prophylaxis Factor VIII T½ = 8 hours Frequency – three times/week Dose – 20-40iu/kg Factor IX T½ = 18 hours Frequency – twice/week Dose – 50iu/kg
Dose Adjustment Growth Break through bleeds
Management of Acute Bleeds Rest Factor Concentrate FVIII; 35-50iu/kg FIX; 70-100% (7-10iu/ml) Wt x desired rise x 1.25 Continuous infusion FVIII 50iu/kg bolus; infusion 4iu/kg/hr FIX 100% bolus; infusion 6-8iu/kg/hr
Mild Factor VIII Deficiency DDAVP 0.3mcg/kg/30 min Antifibrinolytic therapy
Haemophilia The problems Bleeding Destructive arthropathy Addiction Infection Inhibitors
Inhibitors Anti-FVIII Antibodies - IgG Incidence: 10-20% High responding or lowlevel/transient Familial incidence (x6) Majority <10yrs Occur within first 25 treatment days Bleeding
Management of Inhibitors Acute Bleeding episodes FVIIa Immune Tolerance High Dose 200-300iu/kg/d x 1-3 yrs Cyclophosphamide/FVIII/IVIg 50iu/kg/d x 1->12m 25iu/kg/d x 1->12m
Von Willebrands Disease Autosomal Inheritance Abnormal VWF S/S: easy bruising, mucosal bleeds, heavy periods Treatment: antifibrinolytic agents DDAVP Plasma derived factor (Fanhdi) Lab Investigations FVIIIc VWF:Ag VWF:RCF Bleeding time VWF Multimers