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FAZAIA RUTH PFAU MEDICAL COLLEGE ,KARACHI,PAKISTAN
FAZAIA RUTH PFAU MEDICAL COLLEGE ,KARACHI,PAKISTAN

Learning Objectives: After completing the topic, the student will be able to: • Recognize the importance of hemostasis and thrombosis in health and disease. • Describe the process that leads to platelet aggregation. • Classify anti-platelets drugs and the mechanism by which they inhibit platelet aggregation. • Describe indications, contraindications, drug interactions & adverse effects of anti- platelets drugs. • Describe treatment recommendations for antiplatelet agents Acetylsalicylic Acid (Aspirin) • Irreversibly inhibits COX1 and, in higher doses, COX2. • COX1 inhibition (main antithrombotic mechanism); the formation of prostaglandin H2 is blocked, thus thromboxane A2 cannot be synthesized (TxA2 stimulates platelets aggregation). Drug interactions • Co-administration of non-selective COX1 inhibitors may impair its efficacy. • About one-third of patients receiving aspirin manifest treatment failure (Thrombotic Complication or Death). Adverse Events • Resulting from rebound thrombocyte activation after aspirin withdrawal. • Single binding site and does not influence other thrombocyte receptors results in aspirin having less antithrombotic effect than many other agents

Education
1 of 15
Anti-platelets & Thrombolytic ANTI-PLATELET DRUGS Dr AWAIS IRSHAD
Learning Objectives: After completing the topic, the student will be able to: • Recognize the importance of hemostasis and thrombosis in health and disease. • Describe the process that leads to platelet aggregation. • Classify anti-platelets drugs and the mechanism by which they inhibit platelet aggregation. • Describe indications, contraindications, drug interactions & adverse effects of anti- platelets drugs. • Describe treatment recommendations for antiplatelet agents
Classification Thromboxane(TXA2)synthesis inhibitor Glycoprotein IIb / IIIa receptor Inhibitors Purinergic receptor antagonists Phosphodiesterase Inhibitors Aspirin Abciximab, Tirofiban, and Eptifibatide Clopidogrel and Ticlopidine Dipyridamole and Cilostazol
Acetylsalicylic Acid (Aspirin) • Irreversibly inhibits COX1 and, in higher doses, COX2. • COX1 inhibition (main antithrombotic mechanism); the formation of prostaglandin H2 is blocked, thus thromboxane A2 cannot be synthesized (TxA2 stimulates platelets aggregation). Drug interactions • Co-administration of non-selective COX1 inhibitors may impair its efficacy. • About one-third of patients receiving aspirin manifest treatment failure (Thrombotic Complication or Death). Adverse Events • Resulting from rebound thrombocyte activation after aspirin withdrawal. • Single binding site and does not influence other thrombocyte receptors results in aspirin having less antithrombotic effect than many other agents
P2Y12 ReceptorAntagonists • Adenosine Diphosphate (ADP) receptors expressed on the surface of thrombocytes, which can be blocked chemically. • Effect of ADP on platelets: change of conformation, emergence of pseudopodia, platelet aggregation, and interaction with other cellular or plasma components to promote coagulation, is reduced. • Currently, Clopidogrel, Prasugrel, and Ticagrelor are in use, and Cangrelor has recently been licensed.
Clopidogrel • A thienopyridine and a prodrug, of which 85% is hydrolyzed to an inactive metabolite. • The remaining part is activated via cytochrome P3A4/3A5. • The active metabolite binds irreversibly to P2Y12. • An initial loading dose is necessary. • Clopidogrel susceptible to drug interactions (CYP450 dependency). • Proton-pump inhibitors reduces its effect.
Prasugrel • A prodrug, converted by CYP450 enzymes to its active metabolite. • It binds irreversibly to P2Y12, inhibiting platelet function. • More effective platelet inhibition than clopidogrel.
Ticagrelor • An oral non-thienopyridine reversible P2Y12-blocking agent. • CYP3A4 and CYP3A5 are the enzymes involved in the hepatic metabolism of ticagrelor. • Digoxin concentrations should be monitored in the event of concomitant use. • Serum concentrations of some statins (lovastatin and simvastatin) are increased. • Concomitant use of CYP3A4 inhibitors (Ketoconazole, Ritonavir, And Clarithromycin) or inducers (Rifampicin, Phenytoin, Carbamazepine, And Dexamethasone) should be avoided.
Cangrelor • I.V. non-thienopyridine, reversible P2Y12-blocking agent. • Steady-state concentrations are achieved after 18–24 h of i.v infusion without a loading dose or a preliminary bolus being recommended. • Platelet inhibition is >90%. • Inactivated by plasma enzymes, and within 60 min of stopping the infusion the platelet function has recovered to normal. • These favorable pharmacokinetic properties make Cangrelor a promising agent for bridging of high-risk patients in the perioperative setting.
Glycoprotein IIb/IIIa inhibitors • Glycoprotein IIb/IIIa inhibitors block the adhesion of fibrinogen to the activated platelet, preventing the building of interplatelet bridges. • Adhesion of fibronectin, von Willebrand factor, and vitronectin are inhibited. • Abciximab, Triofiban, and Eptifibatide are i.v. GpIIb/IIIa inhibitors that are currently in use.
Abciximab • A humanized monoclonal mouse antibody. • It reversibly binds to thrombocytes within 1 min of administration. • A loading dose is necessary to achieve a >80% receptor blockage. • It shows the highest affinity to the GpIIb/IIIa receptor of the three licensed drugs. • It has a short plasma half-life, but a long biological activity.
Tirofiban and eptifibatide • Synthetic GpIIb/IIIa inhibitors that reversibly bind and rapidly dissociate (10–15 s) from the GpIIb/ IIIa receptor. • Both molecules compete with fibrinogen for the binding of the GpIIb/IIIa receptor. • The affinity for the receptor is greater for tirofiban than for eptifibatide.
OtherAntiplateletAgents Cilostazol and dipyridamole: • Phosphodiesterase inhibitors that interfere with degradation of cyclic adenosine monophosphate and cyclic guanosine monophosphate. • Cause vasodilation. • Protease-activated receptor-1 antagonists: • Vorapaxar and Atopaxar, inhibit platelet activation through alternative routes, including thrombin-mediated platelet aggregation. • Platelet surface proteins: (Glycoprotein VI, Glycoprotein Ib, Prostaglandin E, Nitrous Oxide, and Thromboxane A) are potential targets for inhibitory drugs currently under investigation.
Summary of the characteristics of currently available antiplatelet drugs Characteristic Aspirin Clopidogrel Prasugrel Ticagrelor Cangrelor Abciximab Eptifibatide Tirofiban Route of administration Oral once daily, (i.v) Oral once daily Oral once daily Oral once daily i.v i.v i.v i.v Bioavailability 68% 50% 80% 36% Plasmapeak concentration 30–40 min 1 h 30 min 1.5 h Seconds Dose dependent Dose dependent Dose dependent Time to plasma steady state ------------- 2–8 h 30 min to 4 h 30 min to 2 h Initial bolus and continuous application Initial bolus and continuous application 4– 6 h Initial bolus and continuous application 10 min Initial bolus and continuous application 10 min Plasma half-life 15–30min 8 h 7 h 7 h 2–5 min 10–15 min 2.5 h 2 h Plasma protein binding Strong Strong Strong Strong Time from last dose to offset 7–10 days 7–10 days 7–10 days 5 days 60 min 12 h 2–4 h 2–4 h Reversibility of platelet inhibition No No No Yes Yes Yes Yes Yes Recommended period of discontinuation before surgical intervention 0–5 days 7 days 10 days 7 days 1–6 h 48 h 8 h 8 h
Treatment Recommendations forAntiplateletAgents Condition Treatment Recommendations Primary Prevention Aspirin (Risk vs benefit evaluation) Acute Coronary Syndrome PCI (Percutaneous Coronary Intervention): Aspirin lifelong plus Ticagrelor, Prasugrel, or clopidogrel ≥12 months Non-PCI (Percutaneous Coronary Intervention): Aspirin lifelong plus Clopidogrel or Ticagrelor ≥12 months Stable Angina or former Myocardial Infarction Aspirin lifelong plus Clopidogrel BMS (Bare Metal Stent) ≥1 month DES (Drug-eluting Stent) ≥6 months Recent stroke Aspirin in high-risk situation plus Clopidogrel 90 days Past Stroke Aspirin or Clopidogrel PVD (Peripheral Vascular Disease) Aspirin or Clopidogrel BMS: Bare Metal Stent; DES: Drug-eluting Stent; PCI: Percutaneous Coronary Intervention; PVD: Peripheral Vascular Disease

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ANTIPLATELET DRUGS.pptx

  • 2. Learning Objectives: After completing the topic, the student will be able to: • Recognize the importance of hemostasis and thrombosis in health and disease. • Describe the process that leads to platelet aggregation. • Classify anti-platelets drugs and the mechanism by which they inhibit platelet aggregation. • Describe indications, contraindications, drug interactions & adverse effects of anti- platelets drugs. • Describe treatment recommendations for antiplatelet agents
  • 3. Classification Thromboxane(TXA2)synthesis inhibitor Glycoprotein IIb / IIIa receptor Inhibitors Purinergic receptor antagonists Phosphodiesterase Inhibitors Aspirin Abciximab, Tirofiban, and Eptifibatide Clopidogrel and Ticlopidine Dipyridamole and Cilostazol
  • 4. Acetylsalicylic Acid (Aspirin) • Irreversibly inhibits COX1 and, in higher doses, COX2. • COX1 inhibition (main antithrombotic mechanism); the formation of prostaglandin H2 is blocked, thus thromboxane A2 cannot be synthesized (TxA2 stimulates platelets aggregation). Drug interactions • Co-administration of non-selective COX1 inhibitors may impair its efficacy. • About one-third of patients receiving aspirin manifest treatment failure (Thrombotic Complication or Death). Adverse Events • Resulting from rebound thrombocyte activation after aspirin withdrawal. • Single binding site and does not influence other thrombocyte receptors results in aspirin having less antithrombotic effect than many other agents
  • 5. P2Y12 ReceptorAntagonists • Adenosine Diphosphate (ADP) receptors expressed on the surface of thrombocytes, which can be blocked chemically. • Effect of ADP on platelets: change of conformation, emergence of pseudopodia, platelet aggregation, and interaction with other cellular or plasma components to promote coagulation, is reduced. • Currently, Clopidogrel, Prasugrel, and Ticagrelor are in use, and Cangrelor has recently been licensed.
  • 6. Clopidogrel • A thienopyridine and a prodrug, of which 85% is hydrolyzed to an inactive metabolite. • The remaining part is activated via cytochrome P3A4/3A5. • The active metabolite binds irreversibly to P2Y12. • An initial loading dose is necessary. • Clopidogrel susceptible to drug interactions (CYP450 dependency). • Proton-pump inhibitors reduces its effect.
  • 7. Prasugrel • A prodrug, converted by CYP450 enzymes to its active metabolite. • It binds irreversibly to P2Y12, inhibiting platelet function. • More effective platelet inhibition than clopidogrel.
  • 8. Ticagrelor • An oral non-thienopyridine reversible P2Y12-blocking agent. • CYP3A4 and CYP3A5 are the enzymes involved in the hepatic metabolism of ticagrelor. • Digoxin concentrations should be monitored in the event of concomitant use. • Serum concentrations of some statins (lovastatin and simvastatin) are increased. • Concomitant use of CYP3A4 inhibitors (Ketoconazole, Ritonavir, And Clarithromycin) or inducers (Rifampicin, Phenytoin, Carbamazepine, And Dexamethasone) should be avoided.
  • 9. Cangrelor • I.V. non-thienopyridine, reversible P2Y12-blocking agent. • Steady-state concentrations are achieved after 18–24 h of i.v infusion without a loading dose or a preliminary bolus being recommended. • Platelet inhibition is >90%. • Inactivated by plasma enzymes, and within 60 min of stopping the infusion the platelet function has recovered to normal. • These favorable pharmacokinetic properties make Cangrelor a promising agent for bridging of high-risk patients in the perioperative setting.
  • 10. Glycoprotein IIb/IIIa inhibitors • Glycoprotein IIb/IIIa inhibitors block the adhesion of fibrinogen to the activated platelet, preventing the building of interplatelet bridges. • Adhesion of fibronectin, von Willebrand factor, and vitronectin are inhibited. • Abciximab, Triofiban, and Eptifibatide are i.v. GpIIb/IIIa inhibitors that are currently in use.
  • 11. Abciximab • A humanized monoclonal mouse antibody. • It reversibly binds to thrombocytes within 1 min of administration. • A loading dose is necessary to achieve a >80% receptor blockage. • It shows the highest affinity to the GpIIb/IIIa receptor of the three licensed drugs. • It has a short plasma half-life, but a long biological activity.
  • 12. Tirofiban and eptifibatide • Synthetic GpIIb/IIIa inhibitors that reversibly bind and rapidly dissociate (10–15 s) from the GpIIb/ IIIa receptor. • Both molecules compete with fibrinogen for the binding of the GpIIb/IIIa receptor. • The affinity for the receptor is greater for tirofiban than for eptifibatide.
  • 13. OtherAntiplateletAgents Cilostazol and dipyridamole: • Phosphodiesterase inhibitors that interfere with degradation of cyclic adenosine monophosphate and cyclic guanosine monophosphate. • Cause vasodilation. • Protease-activated receptor-1 antagonists: • Vorapaxar and Atopaxar, inhibit platelet activation through alternative routes, including thrombin-mediated platelet aggregation. • Platelet surface proteins: (Glycoprotein VI, Glycoprotein Ib, Prostaglandin E, Nitrous Oxide, and Thromboxane A) are potential targets for inhibitory drugs currently under investigation.
  • 14. Summary of the characteristics of currently available antiplatelet drugs Characteristic Aspirin Clopidogrel Prasugrel Ticagrelor Cangrelor Abciximab Eptifibatide Tirofiban Route of administration Oral once daily, (i.v) Oral once daily Oral once daily Oral once daily i.v i.v i.v i.v Bioavailability 68% 50% 80% 36% Plasmapeak concentration 30–40 min 1 h 30 min 1.5 h Seconds Dose dependent Dose dependent Dose dependent Time to plasma steady state ------------- 2–8 h 30 min to 4 h 30 min to 2 h Initial bolus and continuous application Initial bolus and continuous application 4– 6 h Initial bolus and continuous application 10 min Initial bolus and continuous application 10 min Plasma half-life 15–30min 8 h 7 h 7 h 2–5 min 10–15 min 2.5 h 2 h Plasma protein binding Strong Strong Strong Strong Time from last dose to offset 7–10 days 7–10 days 7–10 days 5 days 60 min 12 h 2–4 h 2–4 h Reversibility of platelet inhibition No No No Yes Yes Yes Yes Yes Recommended period of discontinuation before surgical intervention 0–5 days 7 days 10 days 7 days 1–6 h 48 h 8 h 8 h
  • 15. Treatment Recommendations forAntiplateletAgents Condition Treatment Recommendations Primary Prevention Aspirin (Risk vs benefit evaluation) Acute Coronary Syndrome PCI (Percutaneous Coronary Intervention): Aspirin lifelong plus Ticagrelor, Prasugrel, or clopidogrel ≥12 months Non-PCI (Percutaneous Coronary Intervention): Aspirin lifelong plus Clopidogrel or Ticagrelor ≥12 months Stable Angina or former Myocardial Infarction Aspirin lifelong plus Clopidogrel BMS (Bare Metal Stent) ≥1 month DES (Drug-eluting Stent) ≥6 months Recent stroke Aspirin in high-risk situation plus Clopidogrel 90 days Past Stroke Aspirin or Clopidogrel PVD (Peripheral Vascular Disease) Aspirin or Clopidogrel BMS: Bare Metal Stent; DES: Drug-eluting Stent; PCI: Percutaneous Coronary Intervention; PVD: Peripheral Vascular Disease