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Anticoagulants and Thrombolytic

Anticoagulants and Thrombolytic. Intrinsic Pathway. Extrinsic Pathway. Tissue Injury. Blood Vessel Injury. Tissue Factor. XIIa. XII. Thromboplastin. XIa. XI. IXa. IX. VIIa. VII. Xa. X. X. Prothrombin. Thrombin. Factors affected By Heparin. Fribrin monomer. Fibrinogen.

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Anticoagulants and Thrombolytic

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  1. Anticoagulants and Thrombolytic

  2. Intrinsic Pathway Extrinsic Pathway Tissue Injury Blood Vessel Injury Tissue Factor XIIa XII Thromboplastin XIa XI IXa IX VIIa VII Xa X X Prothrombin Thrombin Factors affected By Heparin Fribrin monomer Fibrinogen Vit. K dependent Factors Affected by Oral Anticoagulants Fibrin polymer XIII

  3. Classes of Drugs • Prevent coagulation • Dissolve clots • Prevent bleeding and hemorrhage - Hemostatic • Overcome clotting deficiencies (replacement therapies)

  4. Classification A. Reduce the formation of fibrin clots. 1. INDIRECT THROMBIN INHIBITORS • UFH: Heparin • LMWH: Enoxaparin, dalteparin, tinzaparin • SYNTHETIC: Fondaparinux 2. DIRECT THROMBIN INHIBITORS • Parenteral: Hirudin, lepirudin • Oral: Ximelagatran, dabigatran 3. ORAL ANTICOAGULANT DRUGS • Coumarin anticoagulants • warfarin – dicumarol

  5. ANTICOAGULANT DRUGS (contd.) B. Lyse thrombi already formed • Streptokinase, Urokinase, Anistreplase • Tissue Plasminogen Activator: Alteplase, Reteplase, Tenecteplase C. Antiplatelet drugs • Aspirin, clopidogrel, ticlopidine • Platelet glycoprotein IIa/IIIb Receptor blockers • Others: dipyridamole, cilostazol

  6. Monitoring anticoagulant therapy • INR • Ratio of PT of patient • PT of normal person plasma INR = (patient PT/mean normal PT)ISI ISI= International sensitivity Index Relate measured prothrombin time to WHO reference standard thromboplastin ISI = 1

  7. Fibrinolytic drugs • Life saving drugs • Enhance degradation of clots • Activation of endogenous protease • Plasminogen (inactive form) is converted to Plasmin (active form) • Plasmin breaks down fibrin clots • Recently formed thrombus is easily lysed by these drugs. • Aged thrombi (72 hrs) are usually resistant.

  8. Fibrinolysis • Exogenously administered drugs • Streptokinase - synthesized by streptococci convert plasminogen to plasmin • Urokinase- human enzyme synthesized by kidney convert plasminogen to plasmin no immune response Plasmin is formed inside a thrombus , is protected from plasma antiplasmins , which allow it lyse the thrombus from within

  9. Alteplase: Tissue plasminogen activator (tPA) - genetically cloned • no immune reaction • EXPENSIVE • Activate plasminogen bound to fibrin Tenectreplase mutant form of t PA has longer half life Anistreplase (APSAC) Purified human plasminogen and bacterial streptokinase

  10. MECHANISMOF ACTION

  11. Clinical uses of fibrinolytic drugs • Pulmonary embolism with hemodynamic instability • Severe deep venous thrombosis • Ascending thromboplebitis • Acute myocardial infarction (streptokinase loading dose 250,000 units) • Acute ischemic stroke (Recombinant t PA)

  12. Adverse effects • Bleeding: • Fibrinolytic drugs may lyse both normal and pathologic thrombi. • Less effect is seen with t-PA (selectively activates plasminogen that is bound to fibrin) than streptokinase. • Bleeding can be controlled by Aminocaproic acid (inhibits plasminogen activation) • Hypersensitivity reaction: streptokinase • Arrhythmias: • Bradycardia, tachycardia • Free radicals generated after fibrinolysis.

  13. Contraindications Absolute • Prior intracranial hemorrhage • Known structural cerebral vascular lesion • Known malignant intracranial neoplasm • Ischemic stroke within 3 months • Suspected aortic dissection • Active bleeding or bleeding diathesis

  14. Relative • Uncontrolled hypertension • Major surgery within 3 weeks • Recent internal bleeding • For streptokinase prior allergic reaction • Pregnancy • Active peptic ulcer • Current use of warfarin

  15. Antifibrinolytics • Drugs which inhibit plasminogen activation and dissolution of clot • 1- Epsilon amino-caproic acid (EACA) • 2- Tranexaemic acid Indications • Overdose of streptokinase • To prevent recurrence of subarachnoid and G.I hemorhage • Abruptio placentae, PPH and menorhagia

  16. ANTIPLATELET DRUGS • THROMBOXANE A2 INHIBITORS • Aspirin • ADP RECEPTOR INHIBITORS • Ticlopidine • Clopidogrel • Prasugrel • GLYCOPROTEIN IIB/IIA INHIBITORS • Abciximab • Eptifibatide • PHOSPHODIESTERASE INHIBITORS • Cilostazol

  17. Platelet aggregation & sites of drug action Vascular Endothelium         Collagen vWF Granules GP Ib GP Ia Aspirin . . . ... Platelet .. .. TXA2 ADP 5-HT … … .. .. . … … GP IIb/IIIa … … … Abciximab Clopidogrel Ticlopidine Fibrinogen GP IIb/IIIa  GP GP

  18. ASPIRIN Mechanism & Pharmacological effects • Aspirin and most other NSAIDs inhibit the synthesis of prostaglandins: • Decrease endothelial synthesis of PGI2 (prostacyclin) • Decrease thromoboxane A2 production in platelets by inhibiting cyclooxygenase type I and type 2 • Irreversible inhibition of cyclooxygenase and platelet aggregation for the life of the platelet • It may cause bleeding, especially in the GI, and hypoprothrombinemic effect (high doses)

  19. THERAPEUTIC USES OF ASPIRIN • Dose of aspirin 75-325 mg • Prophylactic for transient cerebral ischemia • Reduce the incidence of recurrent MI • Decrease mortality in postmyocardial infarction patients

  20. TICLOPIDINE/CLOPIDOGREL Mechanisms and Pharmacological effects: • Inhibits adenosine diphosphate (ADP)-induced expression of platelet glycoprotein receptors & reduces fibrinogen binding and platelet aggregation. • Can be used in patients who are unresponsive to aspirin to prevent thrombotic stroke.

  21. Clinical use • Prevent thrombosis in patients undergoing placement of a coronary stent • Ticlopidine Prevention of stroke in patients with a history of transient ischemic attack (TIA) or thrombotic stroke Adverse effects: Nausea, dyspepsia and diarrhea, thrombotic thrombocytopenic purpura

  22. Clopidogrel • Unstable angina or non-ST elevation acute myocardial infarction in combination with aspirin • Neutropenia- Less with clopidogrel • Clopidogrel is preferred over ticlopidine

  23. GLYCOPROTEIN IIB/IIA INHIBITORSABCIXIMAB • Chimeric (human-murine) monoclonal antibody • binds to platelet glycoprotein IIb/IIIa receptors and prevents binding by fibrinogen • used solely for the prevention of thrombosis in patients undergoing coronary angioplasty • Parenteral administration

  24. DIPYRIDAMOLE (vasodilator) • Inhibits platelets adhesion to damaged blood vessels •  dosage  increase in platelets cAMP formation and  platelet Ca++ which inhibits platelets aggregation • Used in combination with aspirin to prevent cerebrovascular ischemia

  25. Drugs used in bleeding disorders • Vitamin K (oral and parenteral forms) K1 and K2 newborns, vit k deficiency in patients with poor diet, parenteral nutrition, recent surgery • Plasma factors: factor VII, VIII, IX • Desmopressin acetate (increase the factor VIII activity) • Autoplex (factor VIII) • Cryoprecipitate (plasma protein fraction) Used in DIC

  26. Fibrinolytic Inhibitors • Aminocaproic acid • Tranexamic acid

  27. Uses of antifibrinolytic drugs • Adjunctive therapy in hemophilia • Control bleeding from fibrinolytic therapy • Prophylaxis for bleeding from intracranial aneurysms • Post-surgical GI bleeding • Bladder hemorrhage secondary to radiation & drug-induced cystitis • Gynecological bleeding – fibroids, PPH

  28. Anticoagulants used in vitro • Calcium complexing agents sodium oxalate sodium edetate

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