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EVALUATION OF THE BLEEDING PATIENT

EVALUATION OF THE BLEEDING PATIENT. HISTORY (inherited or acquired bleeding tendency?) Prior invasive procedures, dental extractions Family history Medications, alcohol PHYSICAL EXAM Mucosal/skin vs soft tissue bleeding? Bleeding from one or multiple sites?

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EVALUATION OF THE BLEEDING PATIENT

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  1. EVALUATION OF THE BLEEDING PATIENT HISTORY (inherited or acquired bleeding tendency?) • Prior invasive procedures, dental extractions • Family history • Medications, alcohol PHYSICAL EXAM • Mucosal/skin vs soft tissue bleeding? • Bleeding from one or multiple sites? • Mucosal hemangiomas, skin/joint laxity, etc

  2. Platelet defects and vessel disorders: immediate bleeding from skin and mucosal surfaces, petechiae

  3. Coagulation factor deficiency: delayed bleeding into soft tissues

  4. Bleeding confined to an operative site is usually due to a severed vessel

  5. Initial laboratory evaluation • Platelet count • PT/INR • aPTT • Fibrinogen • Platelet function screen

  6. Prothrombin time/INR Long PT/INR • Liver disease • Vitamin K deficiency • Warfarin or warfarin analogs (rat poison) • DIC • Inherited conditions rare • Won’t detect hemophilia, factor VIII inhibitor, heparin at therapeutic concentrations Magnitude of test abnormality usually proportional to clinical severity

  7. aPTT Long aPTT • Heparin (therapeutic or contaminant) • Hemophilia A or B • von Willebrand disease (low VIII – but PTT may be normal) • Factor XI deficiency • Factor VIII inhibitor • Contact factor deficiency (do not cause bleeding) • Lupus anticoagulant (does not cause bleeding) • Less sensitive than PT/INR to liver disease, DIC, warfarin Magnitude of test abnormality not necessarily proportional to clinical severity

  8. PFA-100 Platelet function screen • Replaces the bleeding time • Advantages • Ex vivo test (no skin incision) • Better standardized • Better sensitivity and specificity

  9. Sensitive to: Defective platelet adhesion in von Willebrand disease Platelet dysfunction due to many drugs Inherited platelet disorders Not useful in patients with moderate or severe Thrombocytopenia Rarely the only abnormal test in an acute bleeding disorder Platelet function screen

  10. Conditions that may cause bleeding with normal or near-normal screening tests • Mild hemophilia (factor level 20-30% of normal) • Von Willebrand disease • Factor XIII deficiency (very rare) • Fibrinolytic disorders • Vascular disorders (Ehlers-Danlos, amyloid, etc)

  11. ACUTE THROMBOCYTOPENIA

  12. ACUTE THROMBOCYTOPENIAImmune-mediated platelet consumption • ITP: Platelets < 10K common, but major bleeding unusual. Rarely develops during hospitalization • Drug-induced purpura: Platelets < 10K common, higher bleeding risk than ITP. Look for recent changes in drug regimen, quinine exposure • Heparin-induced thrombocytopenia: Up to 50% develop thrombosis. Usually not bleeding May occur after heparin d/c’d. Platelets rarely < 20 K. • Post-transfusion purpura: Recent blood transfusion, multiparous woman, sudden severe drop in platelet count (usually <10K).

  13. ACUTE THROMBOCYTOPENIAOther causes • TTP: Systemic signs and symptoms, high LDH, schistocytes on blood smear. Platelets may be < 10K. Rarely develops during hospitalization • HUS, other microangiopathies: Systemic signs and symptoms, renal failure, high LDH, schistocytes on blood smear. Platelets rarely <10K • DIC: Acute systemic illness, abnormal clotting times, platelets rarely <10K • Marrow failure: Other cell lines abnormal. Rarely presents with isolated severe thrombocytopenia

  14. ACUTE THROMBOCYTOPENIA

  15. * * * * * * DRUGS MOST LIKELY TO CAUSE THROMBOCYTOPENIA Hematology 2009;153

  16. ACUTE SEVERE THROMBOCYTOPENIA History • Recent transfusions, previous pregnancies (post-transfusion purpura) • Recent drug exposure • Neuro symptoms (TTP) • Fever, other systemic symptoms (DIC, TTP) • Autoimmune disease, CLL (ITP)

  17. ACUTE SEVERE THROMBOCYTOPENIABlood smear • Platelet clumping (pseudothrombocytopenia) • RBC fragments/schistocytes (TTP, DIC) • Abnormal WBC (marrow dyscrasia) • Large platelets suggest rapid production

  18. ACUTE THROMBOCYTOPENIAFurther diagnostic testing Drug-dependent antibody panel Heparin antibody test HPA-1a antibody testing (post-transfusion purpura) D-dimer, INR, fibrin monomer (DIC) LDH, urinalysis, retic count (TTP) ADAMTS-13 activity (TTP) Marrow biopsy often unnecessary (for isolated thrombocytopenia) • ITP is diagnosis of exclusion • New onset thrombocytopenia in hospitalized patient is usually not due to ITP or TTP

  19. ACUTE THROMBOCYTOPENIATreatment

  20. www.ouhsc.edu/platelets

  21. HEMOPHILIA

  22. HEMOPHILIA • Inherited deficiency of factor VIII (hemophilia A) or factor IX (hemophilia B) • Sex-linked inheritance; almost all patients male • Most bleeding into joints, muscles; mucosal and CNS bleeding uncommon • Severity inversely proportional to factor level: < 1%: severe, bleeding after minimal injury 1-5%: moderate, bleeding after mild injury > 5%: mild, bleeding after significant trauma or surgery (may not be diagnosed until adulthood)

  23. HEMOPHILIATreatment of bleeding episodes • Unexplained pain in a hemophilia should be considered due to bleeding unless proven otherwise • External signs of bleeding may be absent • Treatment: factor replacement, pain control • Most adult patients self-administer factor • Test for inhibitor (antibody vs factor) if unexpectedly low response to factor replacement

  24. TREATMENT OF BLEEDS IN HEMOPHILIA • Administer appropriate clotting factor concentrate • 20-40 U/kg for minor bleeds, repeat daily for 2-3 days • 40-50 U/kg for major bleeds, repeat daily for 4-7 days • 50 U/kg q 12 hours for life-threatening bleeds • 1 U/kg should increase plasma level of factor by about 2% • Initial dose somewhat higher with factor IX concentrate (greater volume of distribution, but longer half-life)

  25. TREATMENT OF HEMOPHILIACS WITH INHIBITORS • Call a hematologist • Recombinant factor VIIa • High dose factor VIII (if low titer inhibitor) • Induce tolerance with daily factor infusion ± immunosuppression

  26. ACQUIRED FACTOR VIII DEFICIENCY • Autoantibody to factor VIII (most common autoimmune factor deficiency) • Most patients elderly • Often presents with severe soft tissue or mucosal bleeding (different bleeding pattern than inherited hemophilia) • Laboratory: prolonged aPTT not corrected by mixing with normal plasma, factor VIII activity typically < 10% • Bleeding risk not proportional to factor level • Normal INR and platelet count • Treatment: rVIIa, immunosuppression

  27. DISSEMINATED INTRAVASCULAR COAGULATION

  28. DISSEMINATED INTRAVASCULAR COAGULATION • Rapid formation & lysis of intravascular fibrin • Consumption of clotting factors, platelets, inhibitors • Life-threatening underlying disease • Bleeding due to uncontrolled fibrinolysis, thrombocytopenia, clotting factor consumption and tissue injury from underlying disease • Tissue injury/necrosis due to microvascular occlusion, hypotension, cytokine-mediated endothelial damage • Most deaths due to underlying disease

  29. PUPURA FULMINANS Pneumococcal sepsis in splenectomized patient NEJM 2001;344:1593

  30. DIAGNOSIS OF DIC • Underlying disease capable of causing DIC? • Evidence of accelerated clotting factor and platelet consumption, and increased fibrinolysis? If both present DIC is likely

  31. SCREENING FOR DIC • D-dimer (most sensitive) • PT/INR • Fibrinogen • CBC/platelet count • Fibrin monomer (most specific)

  32. TREAT UNDERLYING DISEASE! Clotting factor & inhibitor replacement for patients with significant bleeding: Fresh frozen plasma (goal INR ≤ 1.6) Cryoprecipitate (goal fibrinogen ≥ 100) Platelets (goal platelet count 50-75K) Pharmacologic inhibitors (selected pts with refractory bleeding) Heparin (low dose) Antifibrinolytics (Amicar, tranexamic acid) TREATMENT OF DIC

  33. THROMBOTIC THROMBOCYTOPENIC PURPURA (TTP)

  34. TTP • Microangiopathic hemolytic anemia • Thrombocytopenia • Organ dysfunction (CNS, renal, other) due to small vessel occlusion • Untreated mortality rate >90% • With treatment mortality < 20% • 1-2 cases/yr @ UWHC

  35. TTP • Caused by autoimmune destruction of ADAMTS-13 protease that modulates von Willebrand factor multimer size • Very large multimers clump platelets • Microthrombi damage RBC and block vessels

  36. TTP • Thrombocytopenia (may be severe) • Hemolytic anemia (high LDH, low haptoglobin, schistocytes in blood smear) • Organ dysfunction • Neurologic symptoms • Renal dysfunction (hematuria, proteinuria) • Cardiac (arrhythmia) • ADAMTS-13 activity low (usually <5%)

  37. TTP - DDX • Cancer (may be occult) • Pregnancy complications (HELLP, etc) • Hemolytic-uremic syndrome • Vasculitis (SLE, scleroderma) • HIV infection • DIC • Drugs (calcineurin inhibitors, mitomycin C, interferon)

  38. TTP • Urgent plasma exchange • Plasma infusion if PE not immediately available • Immunosuppression • Corticosteroids • Rituximab for patients with resistant, refractory or relapsed disease • Do not transfuse platelets unless there is lifethreatening bleeding

  39. BLOOD PRODUCTS AND DRUGS IN THE TREATMENT OF BLEEDING DISORDERS

  40. BLOOD COMPONENT TRANSFUSION TO TREAT OR PREVENT BLEEDING • Platelets: • Active bleeding: if platelet count < 50K • Prophylaxis: when platelets <10-20K • Patient having surgery: if platelets < 50-100K • FFP (active bleeding): • When INR > 1.6 • Cryoprecipitate (active bleeding): • Goal fibrinogen level 100

  41. DDAVP (Desmopressin) • Vasopressin analogue, stimulates VWF/factor VIII release from endothelium • Intravenous or intranasal administration • Increases plasma VWF/factor VIII levels for 18-24h, enhances platelet adhesion • Effective in • Type I VWD (usually not in type 2, never in type 3) • Mild hemophilia A • Platelet dysfunction (variably effective) • Side effects usually mild (HA, flushing, hyponatremia with repeated dosing)

  42. AMICAR(epsilon aminocaproic acid) • Antifibrinolytic: inhibits plasmin formation and binding to fibrin • Uses • Treating DIC with hyperfibrinolysis, or bleeding after thrombolytic drugs • Prophylaxis in severe thrombocytopenia • GI tract bleeding • Menorrhagia • Prophylaxis after dental extraction in hemophilia • Short half-life, needs frequent dosing (4-24 grams/d) • Oral or intravenous administration • Alternative: tranexamic acid (longer half-life)

  43. Recombinant Factor VIIa (rFVIIa) • Augments tissue factor-induced coagulation • FDA approved for treatment of Factor VIII inhibitor w/bleeding • Off-label use is common, efficacy unclear: • Other coagulation inhibitors (including drugs) w/bleeding • Emergency reversal of coagulopathy (eg, warfarin) in patients with lifethreatening bleeding • Potent procoagulant → risk of thrombosis • Very expensive!

  44. Prothrombin complex concentrate (PCC) • Mixture of vitamin K dependent procoagulant factors: II, IX, X ,VII • Used to rapidly correct warfarin effect (or severe vitamin K deficiency) in acutely bleeding patient or prior to urgent surgical procedure • Advantages vs FFP: • Less volume • No risk of TRALI, low risk of allergic rxn • Less risk of virus transmission

  45. VITAMIN K Indications: • Correction of vitamin K deficiency • Treatment of warfarin or superwarfarin overdose • Prophylaxis in patients at risk for vitamin K deficiency Oral or IV administration (unreliable absorption with subcutaneous injection)

  46. ANTICOAGULANT-RELATED BLEEDING

  47. 200 150 100 Bleeding events/100 patient-yr 50 0 <2 2.0-2.9 3-4.4 4.5-6.9 >7 INR BLEEDING RISK VS INR Lancet 1996; 348:423

  48. Treatment of warfarin-induced coagulopathy in the non-bleeding patientDentali et al, J Thrombos Haemost 2006;4:1853

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