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Inherited Coagulation Disorders

Inherited Coagulation Disorders. Dr Galila Zaher Consultant Hematologist KAUH. BLOOD CLOTTING. Blood clotting interactions Plasma protein clotting factors Platelets Vascular endothelium. Hemostasis. Hemostasis. Subendothelial matrix. Subendothelial matrix.

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Inherited Coagulation Disorders

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  1. Inherited Coagulation Disorders Dr Galila Zaher Consultant Hematologist KAUH

  2. BLOOD CLOTTING Blood clotting interactions Plasma protein clotting factors Platelets Vascular endothelium

  3. Hemostasis Hemostasis Subendothelial matrix Subendothelial matrix Hemostatic plug Hemostatic plug Endothelial cell Endothelial cell WBC WBC WBC WBC Fibrin RBC Platelets Fibrin RBC Platelets

  4. COAGULOPATHIES Bleeding Thrombosis Clotting factors Natural anticoagulant platelets

  5. Clot formation Platelet activation Primary hemostasis No &count (immediate) Fibrin generation plasma clotting Secondary hemostasis factors (delayed)

  6. ADP Aggregation Aggregation Aggregation GpIIb/IIIa GpIIb/IIIa GpIIb/IIIa GpIIb/IIIa GpIIb/IIIa GpIIb/IIIa Adrenaline Adhesion Adhesion vWF Endothelium Exposed Collagen Platelet Activation Pathways (1) COLLAGEN THROMBIN ADP GpIIb/IIIa Platelet GpIb Adrenaline Adhesion

  7. Clotting factor production Liver: source of plasma clotting factors except VWF Factor VIII: produced by liver & endothelium VWF: endothelial cells & megakaryocytes Vitamin K dependent clotting factors are: II, VII, IX, X

  8. COAGULATION PATHWAYS Intrinsic & extrinsic pathways “conclude” in the common pathway Intrinsic pathway clotting factors Extrinsic pathway clotting factors Common pathway clotting factors

  9. NORMAL COAGULATION PATHWAYS Intrinsic pathway clotting factors Factor XII Factor IX Factor VIII Factor XI Extrinsic pathway clotting factors Tissue factor (TF)* Factor VII Common pathway clotting factors Factor X Factor V Factor II Prothrombin Factor I Fibrinogen

  10. Extrinsic pathway VII + TF ----->VIIa/TF v IXase (“crossover”) Xase (minor) Intrinsic pathway XII ---> XIIa v XI---------XIa • v • IX --------> IXa • + VIII • v • X----------------------> Xa [Common pathway] • v • Xa + V • prothrombin -------------> thrombin • v • fibrinogen--------------> fibrin

  11. Fibrin XIIIa Cross-linked fibrin

  12. Deficiencies of: • Factor XII • High molecular weight kininogen • Prekallikrein • - Do NOT produce bleeding diatheses

  13. COAGULATION TESTS • Platelet tests <150,000 thrombocytopenia >400,000 thrombocytosis • Tests of clotting factors

  14. Platelet tests Test Comment Platelet count Part of routine CBC, normal count: 150,000 - 400,000/uL Mean platelet volume MPV Some analyzers provide MPV measurement; in healthy individuals, MPV varies inversely with platelet count Platelet aggregation Not routine tests, and secretion tests used only in special circumstances

  15. Tests of clotting factors

  16. Hemophilia A = Factor VIII deficiency • B = Factor IX deficiency • Affects one in 6000 males • A is 5 X > B • Mild > 5 % normal amount of factor • Moderate 2 - 5 %, severe < 2 % • Levels remain stable throughout life

  17. Inheritance • Both HA & HB are X linked • Only men can have the disease • Women are carriers

  18. Clinical presentation • < 2 years: joint bleeds Rare Only bruising or mouth bleeds are seen Head injuries are a major concern • > 2 years joint and muscle bleeds become more common

  19. Clotting factor deficiencies

  20. Laboratory Diagnosis • Isolated prolongation of APTT • Microcytic hypochromic anemia • Normal platelets count • Mixing studies :corrected.

  21. When to treat • All joint bleeds: Pain, swelling ,warmth or loss of movement . • Muscle bleeds that cause severe pain or are in a dangerous location • Bruises usually don’t need treatment • When in doubt .

  22. Treatment • Keep weight off of joint • Ice pack • Factor replacement - the sooner the better • Amicar or tranexamic acid : mouth bleed • CVL s :Frequent bleeds or factor given on a regular basis • Port-a-catheters

  23. Dose & Duration • 1 IU/kg of factor VIII increases the level by 2% • 1 IU/kg of factor IX increases the level by 1% • Every 12 hours the level decreases by half

  24. Prophylaxis • To prevent bleeds • Started after developing a target joint • Usually it is administered 3/week • Stepwise approach: Initially 1/week, increasing to 2-3/week if needed • Goal is to prevent long-term joint damage

  25. Team Approach • We all work together Child and parents Doctor and nurses Physiotherapy Social work • Everyone has an essential role • The aim is to get life to be as normal as possible

  26. Factor VIII Replacement • Mechanism of action : activate FX • Mode of administration : IV • Monitoring : no predict the effectiveness of treatment • Indications :HA & HB • Severe surgical bleeding • Factor VII deficiency

  27. Factor VIII • Derived from pooled human plasma • Derived from pig (porcine) plasma • Recombinate products

  28. Porcine factor VIII • Hyate:C • Apparently no pig viruses present • Can replace human Factor VIII in clotting cascade • Minimal cross reactivity with AHF antibodies • Minimal von Willebrand factor present

  29. von Willebrand Factor (V W F) • VWF bridges platelets to collagen exposure from blood vessel injury • VWF contributes to primary hemostasis • Factor VIII circulates bound to VWF . • VWD: clinically similar to platelet disorders • Most common inherited bleeding disorder

  30. VWD • Inherited as a dominant or recessive . • Most common congenital bleeding disorder • Affecting 1-3% of the population. • Personal and family bleeding history. • Highly heterogeneous • Ranging from asymptomatic to a life threatening bleeding. • The most common bleeding symptoms ever were epistaxis, bruising • Menorrhagia is one of the most important and frequent complications in women

  31. Platelet disorders

  32. DIAGNOSIS • The condition is caused by a quantitative or qualitative deficiency of vWF. • Prolonged bleeding time (BT) & activated partial thromboplastin time (APTT) • iron deficiency anemia . • type 1 vWD

  33. Managment • The aim of treatment is to correct the dual defect of hemostasis ( low VIII:C & prolonged bleeding time). • DDAVP is the treatment of choice for the mild forms of type 1 and 2 VWD • Unresponsive to DDAVP, plasma virally inactivated concentrates of factor VIII • Tranexamic acid

  34. Increased PT Deficient, function or inhibition : Liver disease production/ vit K malabsorption vit. K antagonists warfarin (blocks carboxylation) Heparin the PTT is a more sensitive test FDPs inhibits coagulation lupus anticoagulant PTT is a better test (LA)

  35. Increased PTT Heparin unfractionated heparin inhibits Xa and IIa vit K antagonists PT is a more sensitive fibrin/fibrinogen inhibits coagulation degradation products lupus anticoagulant PTT is a better than PT

  36. TT increased • Congenital disorders afibrinogenemia homozygous def. hypofibrinogenemia heterozygous def. dysfibrinogenemia dysfunctional fibrinogen • Acquired disorders hypofibrinogenemia liver disease, (disseminated intravascular coagulation), thrombolytic therapy dysfibrinogenemia liver disease, hepatic malignancy Fibrin degradation inhibits coagulation products Heparin inactivates IIa

  37. Fibrinogen level hypofibrinogenemia) Liver disease decreased production Consumption disseminated intravascular coagulation (DIC) Thrombolytic therapy Congenital def. afibrinogenemia: homo. def. hypofibrinogenemia: hetero.

  38. Fibrinogen assay

  39. Problem solving PT PTT TT Incr. NL NL _____________ NL Incr. NL _____________ Incr. Incr. NL _____________ Incr. Incr. Incr. _____________

  40. Actions of thrombin Intrinsic pathway XII ---> XIIa Extrinsic pathway VII + TF ----->VIIa/TF v IXase (“crossover”) Xase (minor) v XI---------XIa • v • IX --------> IXa • + VIII • v • X----------------------> Xa [Common pathway] • v • Xa + V • prothrombin -------------> thrombin • v • fibrinogen--------------> fibrin ---> VIIIa ---> Va v XIII ---> XIIIav cross-linked fibrin

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