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Bleeding & Clotting Disorders I

Bleeding & Clotting Disorders I. Richard E. Freeman MD 2013. Overview. The Players Factor Deficiencies causing bleeding Dissolving the Clot The Clinical Presentation Other Causes of Bleeding Hypercoagulability. Bleeding Bleeding Diathesis. Clotting Hemostasis Coagulation

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Bleeding & Clotting Disorders I

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  1. Bleeding & Clotting Disorders I Richard E. Freeman MD 2013

  2. Overview • The Players • Factor Deficiencies causing bleeding • Dissolving the Clot • The Clinical Presentation • Other Causes of Bleeding • Hypercoagulability

  3. Bleeding Bleeding Diathesis Clotting Hemostasis Coagulation Thrombophilia The Precarious Balance the anticoagulants vs. the procoagulants

  4. Hemostasis: • cessation of blood loss from a damaged vessel • Other Terms • bleeding disorders = bleeding diathesis = coagulopathies • diathesis [Gr. Diathenai – to predispose] : A constitutional predisposition to certain diseases or conditions

  5. Clots Stop Blood Flow

  6. Phases of Clot Formation • VASCULAR INJURY & SPASM constriction of injured blood vessel • injury releases tissue factors, platelets release serotonin (vasoconstrictor), and activates extrinsic pathway • PLATELET PLUG FORMATION collagen in vessel exposed by injury. von Willebrand factor (vWF) needed to bridge platelets and collagen. • Calcium (Ca 2+) needed

  7. Phases of Clot Formation • COAGULATION CASCADE INTRINSIC AND EXTRINSIC PATHWAYS formation of cross-linked fibrin polymer clot “fibrin clot” • DISSOLUTION OF CLOT

  8. vascular spasm

  9. collagen fibers platelet plug platelet plug formation

  10. fibrin clot formation

  11. The Players

  12. Complex Interactions • ALL OF THESE MUST FUNCTION NORMALLY for EFFECTIVE CLOT FORMATION and HEMOSTASIS • Vascular endothelial cells • Platelets • Clotting factor cascade • Blood flow & shear • Antifibrinolysis

  13. Blood Content & Hemostasis • Plasma – Unclotted liquid part of blood • 90% Water • 10% Dissolved and suspending particles • Organics: Proteins • albumin 53%-LIVER • globulins 43% • Antibodies-RE SYSTEM • Compliment & Kinin System (Inflamation) • Clotting Factors-LIVER AND ELSEWHERE • Fibrinogen 4% • Inorganics: salts • Blood Cells • RBCs – Erythrocytes • WBCs – Leukocytes • Platelets – Thrombocytes

  14. ENDOTHELIAL CELLS

  15. Three Layers of the Blood Vessel • Tunica intima:endothelial cells (EC) & subendothelium • Tunica media: • smooth muscles & extracellular matrix • Tunica adventitia:fibroblasts & cellular matrix(loose connective tissue)

  16. The Endothelial Cell (EC) • 1. Intact, healthy EC produces and is “teflon” coated with prostacyclin (PGI2) • – RESTING STATE • A vasodilator • Inhibits platelet adhesion • Acts in opposition to the platelet thromboxane A2 • 2. EC coated w/ heparin sulfate which activates anti-thrombin III in plasma & stops thrombosis • 3. Synthesis of Factor VIII – vonWillebrand factor • vWF synthesized in platelets & EC

  17. 3 • PLATELETS

  18. The Amazing Platelet • 1. Secrete procoagulants which promote clotting • 2. Secrete vasoconstrictors causing vascular spasm in injured blood vessels • 3. as they aggregate they undergo degranulation releasing: • serotonin (vasoconstrictor), • ADP (attractant)-calls for more platelets to help, • thromboxane A2 –(clot promoter) • 4. form temporary platelet plugs to stop bleeding • 5. dissolves blood clots that have outlasted their usefulness • 6. inflammation and remodeling

  19. Platelets

  20. Life of a Platelet • MEGAKARYOCYTE (“mama” cell) fragmentation in marrow • thrombopoietin (TPO) stimulates production produced in liver, bone marrow & kidney • 1/3 sequestered to the spleen • 2/3 into circulation (150-450,000 per microliter of blood). • LIFE SPAN 7 TO 10 DAYS • (RBCs 90-120 days, WBCs 1 day) • ASA (aspirin) thus effect lasts this long • irreversible acetylation of cyclooxygenase 1

  21. Cell Lines

  22. Platelet-Chemistry • ACTIN-MYOSIN • Contraction – pulls clot together • SURFACE: GP IIb/IIIa glycoprotein • Important in adhesion and aggregation • DENSE GRANULE: • Calcium, ADP, Serotonin • ALPHA-GRANULE: • Growth factor, fibrinogen, Factor V, vonWillebrand factor (vWF), fibronectin, beta-thromboglobulin, heparin antagonist (PF4), thrombospondin

  23. PLATELET

  24. PLATELETS-FOUR MAJOR FUNCTIONS • 1. ADHESION ACTIVATION • 2. AGGREGATION • 3. SECRETION • 4. PROCOAGULANT ACTIVATION

  25. 1. ADHESION ACTIVATION: • platelet on subendothelial matrix (surface) • glycoprotein IIb/IIIa surface receptor binds vWF in subendo matrix

  26. 2. AGGREGATION: • cohesion of platelets • fibrinogen binds activated glycoprotein IIb/IIIa receptor • Inhibited by • abciximab IV (ReoproR), tirofiban (AggrastatR), eptifibatide (IntegrelinR) all IV; used in angioplasty; often used along with aspirin and heparin* • ADP-receptor involved in GP IIb/IIIa-fibrinogen interaction and possibly also the vWF site • Inhibited by • clopidogrel (PlavixR), ticlopidine (TicilidR) inhibit; both given PO* *all treat and prevent arterial thrombosis

  27. 3. SECRETION: • release of plt. granule proteins • ADP, serotonin, adhesive protein (fibronectin, others), Factor V, thromboxane A2 • many growth factors (smooth muscle etc) • may be involved in restenosis post PTCA

  28. 4. PROCOAGULANT ACTIVITY: • enhancement of thrombin generation • assembly of the clotting cascade on the platelet surface

  29. 4 1 2 3

  30. GP-IIb/IIIa Receptor

  31. CLOTTING FACTOR CASCADE

  32. Coagulation: thecommon pathway • THE OBJECTIVE • is to convert the plasma protein fibrinogen into fibrin, a sticky protein that adheres to the walls of a vessel and also traps additional platelets and RBCs like a spider’s web Factor X

  33. Fibrin Polymerization-

  34. Coagulation Cascade • TWO reaction pathways (roads) • INTRINSIC PATHWAYuses only clotting factors found inside the blood itself (plasma, platelets) 3- 6 seconds • EXTRINSIC PATHWAY initiated by clotting factors released in damaged vessels (tissue factor or thromboplastin) and perivascular tissues-15 seconds • Roman numerals indicate the order discovered, however some numbers are not used: • Factor IV is Ca++; Factor VI is activated Factor V

  35. Extrinsic Pathway Coagulation Cascade Pathways Intrinsic Pathway Common Pathway EXtrinsic = In Tissue INtrinsic = In Blood Common = Yields fibrin CLOT

  36. THE INTRINSIC PATHWAY- the reaction amplification cascade

  37. Table 18.9

  38. PROCOAGULANT “CLOTTING FACTORS” Synthesis • ALL synthesized in the LIVERexcept • von Willebrand Factor in megakaryocytes and endothelial cells • vWF is involved in • PLATELET ACTIVATION • Maintaining normal factor VIII levels

  39. Vitamin K • Vitamin K-dependent procoagulants • II (Prothrombin), VII, IX, X • Vitamin K-dependent anticoagulants • Warfarin-dicoumarol (COUMADIN) • Vit K antagonist • Inhibits Vit K epoxide reductase • (recycles oxidized Vit K – after K has been used in carboxylation of clotting factor production)

  40. “THE REGULATORS” • PROTEIN C & S • ANTITHROMBIN • TISSUE FACTOR PATHWAY INHIBITOR • PLASMINOGEN->PLASMA • PROSTACYCLIN ( PGI2)

  41. PROTEIN C & PROTEIN S Protein C & Protein S • ACTION: inactivates Factor Va and VIIIa • “Natural anticoagulant” – keeps system in balance • Protein C: • vitamin K-dependent serine protease enzyme • Thrombomodulin (on endothelial cell surfaces) and Thrombin stimulate Protein C and when activated by Protein S- inactivates Factor V • .see flow diagram

  42. thrombin + thrombomodulin on endothelium turns off clotting cascade by activating Protein C. Protein C w/ Protein S (a cofactor) turn off various Factors

  43. Protein C & S deficiency • Spontaneous Thrombosis/thromboemboli • Suspect in young person with DVT/Stroke with significant risk factors • Most will be need Lifelong Anticoagulant therapy

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