Post on 18-Nov-2014
Anticoagulant, Antithrombotic and Anti-Platelet Drugs
Department of Pharmacology
Robert Taylor, MD, Ph.D.
Clinical Thrombosis
• >2.5 million cases of deep venous thrombosis (DVT) per year
• >600,000 cases of pulmonary embolism (PE) per year
• >50,000 deaths per year from PE• PE contributes to another 150,000 deaths
per year• > 11,000 postsurgical PE deaths per year
Indications For Antithrombotic Therapy
• Venous thromboembolic disease– Deep venous thrombosis (DVT)– Pulmonary embolism (PE)– Primary prophylaxis of DVT or PE
• Arterial thromboembolic disease• Prosthetic heart valves• Mitral valve disease, especially with atrial fibrillation• Congestive cardiomyopathies, especially with atrial fibrillatio• Atrial fibrillation• Mural cardiac thrombi• Transient ischemic attacks• Stroke in evolution
• Disseminated intravascular coagulation• Maintenance of patency of vascular grafts, shunts, bypasses
Recombinant Human Activated Protein C
• Drotrecogin alfa (activated)- Xigris• Indicated for Severe Sepsis in Adults with
Acute Organ Dysfunction with High Risk of Death
• Reduction in Death as Primary End Point
• Antithrombotic, Antiinfammatory, Profibrinolytic Properties
• Serious Bleeding is Major Side Effect
Antithrombin III Inhibits the Following Serine Proteases
• Coagulation
• Factor XIIa• Factor XIa• Factor IXa• Factor Xa• Thrombin
• Fibrinolysis
• Plasmin
Inhibitory activity against all these enzymes is substantially accelerated by heparin
Heparin• Heterogeneous; 3,000-30,000 d
• Average=15,000 d (~45monosaccharide chains)
• About 1/3 of dose binds to AT III
• To form the AT III:Heparin:Clotting Factor Complex- requires at least 18 saccarides except
• Unique high affinity pentasaccaride heparin sequences catalyze inhibition of Xa by AT
Anticoagulant Properties of Heparin
1. Inhibits the thrombin-mediated conversion of fibrinogen to fibrin
2. Inhibits the aggregation of platelets by thrombin
3. Inhibits activation of fibrin stabilizing enzyme
4. Inhibits activated factors XII, XI, IX, X and II
Heparin
• Biologic Sources• Bioavailability• Metabolism• Elimination• Side Effects• Overdose• Contraindications• Pregnancy- YES
Unfractionated Heparin
• High Dose– Treatment of venous/arterial thrombi– Requires monitoring– IV- 5,000 Units bolus, then 30,000-35,000
units/24 hrs– 80 Units/kg bolus, then 18 Units/kg/hr to
maintain aPTT in therapeutic range
Monitoring of Anticoagulant Therapy
Heparin
s.q. – no monitoring required
i.v. - partial thromboplastin time (P.T.T.)
*daily or more frequent if PTT varies
mechanism – measures intrinsic pathway
therapeutic goal – 2-2.5 times normal control value (-30 sec)
Low Dose Unfractionated Heparin
• Surgical Prophylaxis– 5,000 Units SQ 2 hr preop– 5,000 Units SQ every 12 hours
• Medical Prophylaxis– 5,000 Units SQ every 12 hours
• No monitoring required
Indications for and Contraindications to Parenteral Anticoagulant Agents
Anticoagulant Agent Class Approved & Appropriate Indications
Contraindication
Unfractionated heparin
Enoxaparin
(Lovenox)
Dalteparin
(Fragmin)
Tinzaparin
(Innohep)
Antithrombin III inhibitor
Low-molecular-weight heparin
Low-molecular-weight heparin
Low-molecular-weight heparin
Treatment of venous thromboembolism or unstable angina; used when rapid reversal is important
Prophylaxis in moderate-risk or high-risk patients, treatment of venous thromboembolism or unstable angina
Prophylaxis in moderate-risk or high-risk patients, treatment of venous thromboembolism or unstable angina
Prophylaxis in moderate-risk or high-risk patients, treatment of venous thromboembolism
? Prophylactic treatment
Regional anesthesia
Pregnancy
Prosthetic Heart Valves
Regional anesthesia
Regional anesthesia
Indications for and Contraindications to Parenteral Anticoagulant Agents (cont’d)
Ardeparin
Lepirudin
Argatroban
Danaparoid
Bivalirudin
Fondaparinux
(Arixtra)
Low-molecular-weight heparin
Hirudin derivative
Direct thrombin inhibitor
Heparinoid
Hirudin derivative
Synthetic factor Xa inhibitor
Approved; not being marketed
Heparin-induced thrombocytopenia with thrombosis
Heparin-induced thrombocytopenia with thrombosis
Prophylaxis against thrombosis in heparin-induced thrombocytopenia
Unstable angina or angioplasty
Prophylaxis in high-risk patients?
Regional anesthesia
Thrombocytopenia other than heparin-induced thrombocytopenia
Thrombocytopenia other than heparin-induced thrombocytopenia
Thrombocytopenia other than heparin-induced thrombocytopenia
Unknown
Unknown
Heparin-Antibiotic Interactions
• The second-generation cephalosporins- cefamandole, cefotetan, and cefoperazone, contain an N-methylthiotetrazole (NMTT) side chain. This NMTT group can:
• - Dissociate from the parent antibiotic in solution or in vivo and competitively inhibit vitamin K action, leading to prolongation of the prothrombin time and bleeding.
• - This side chain is also associated with a disulfiram-like reaction to alcohol.
• - Clinical bleeding has been less frequently reported with Cefotetan than with cefoperazone or cefamandole.
Mechanisms of HIT
• Type 1: In most of these cases, the fall in platelet count occurs within the first two days after heparin initiation, often returns to normal with continued heparin administration, and is of no clinical consequence. The mechanism of the thrombocytopenia is non-immune and appears to be due to a direct effect of heparin on platelet activation.
• Type 2: Approximately 0.3 to 3 percent of patients receiving heparin develop an immune thrombocytopenia, mediated by antibodies to a heparin-platelet factor 4 complex. One study, for example, randomly assigned 665 patients to therapy with unfractionated heparin or LMW heparin. Type 2 HIT developed in 2.7 percent of patients treated with unfractionated heparin but in none of those receiving LMW heparin.
Therapy of HIT
• There are two recommended approaches: – Use of the heparinoid danaparoid – The direct thrombin inhibitor lepirudin (recombinant
hirudin)– Based upon the data published to date, either
danaparoid or lepirudin should be used to treat HIT that is complicated by thrombosis; these agents should also be considered for prophylactic therapy in patients with HIT without thrombosis until the platelet count has recovered
Warfarin• Bioavailability• Metabolism• Serum Protein Binding• Vitamin K Status• Protein C Effects• Elimination• Side Effects• Overdose• Contraindications• Pregnancy- NO
Contraindications to Antithrombotic Therapy
• General risk factors-Pre-existing coagulation or platelet defect,
thrombocytopenia, or other bleeding abnormality-Inaccessible ulcerative lesion (e.g., gastrointestinal tract
lesion)-Central nervous system lesion (e.g., caused by stroke,
surgery, trauma)-Spinal anesthesia or lumbar puncture-Malignant hypertension-Bacterial endocarditis-Advanced retinopathy-Old age (relative)-Aspirin or other antiplatelet drugs-Neoplastic disease
Contraindications to Antithrombotic Therapy
• Specific to warfarin (ambulatory patients)
-Early and late pregnancy
-Poor patient cooperation, understanding, reliability
-Unsatisfactory laboratory or patient follow-up
-Occupational risk to trauma
Contraindications to Antithrombotic Therapy
• Specific to thrombolytic agents-Recent thoracic, abdominal, or central
nervous system surgery-Recent cerebrovascular accident, trauma,
or neoplasm-Bleeding ulcer-Hypertension-Anticipated invasive procedures (arterial
punctures, biopsies, central lines)-Concurrent hemostatic dysfunction
Platelet Receptor Mediated Pathways: Drugs
Arachidonic Acid ASA
NSAIDs
ADP Ticlopidine
Clopidogrel
Thrombin
-Final Common Pathway
-Promotes Platelet Adhesion (Fibrinogen, vWF)
GP IIB/IIIA Inhibitors
Abciximab (ReoPro)
Eptifibatide (Integrilin)
Tirofiban
Anti Platelet DrugsDrug Mechanism Uses
Aspirin Permanently inhibits COX-1 and COX-2
CAD
Stroke-TIAs
NSAIDs Reversibly inhibits COX-1
Limited
Dipyridamole Inhibits PDE; increases cAMP
TIAs
Ticlopidine
Clopidrgrel
Inhibits ADP PlatAg;active metabolite
TIAs;Stroke
CAD;PVD