Download - Anticoagulants
ANTICOAGULANTS
Dr. D. K. BrahmaDepartment of Pharmacology
NEIGRIHMS, Shillong
Blood Vessel Injury
IX IXa
XI XIa
X Xa
XII XIIa
Tissue Injury
Tissue Factor
Thromboplastin
VIIa VII
X
Prothrombin Thrombin
Fibrinogen Fribrin monomer
Fibrin polymerXIII
Intrinsic Pathway Extrinsic Pathway
Factors affectedBy Heparin
Vit. K dependent FactorsAffected by Oral Anticoagulants
Recall !
Why anticoagulants ?To reduce the coagulability of bloodBlood clots – ThrombusArterial Thrombosis:
Adherence of platelets to arterial walls – “White” in color - Often associated with MI, stroke and ischemia
Venous Thrombosis:Develops in areas of stagnated blood flow (deep vein thrombosis),
“Red” in color- Associated with Congestive Heart Failure, Cancer, Surgery
Thrombus dislodge from arteries and veins and become an embolusVenous emboli can block arterioles in the lung and pulmonary
circulationThromboembolism
Available AnticoagulantsUsed in vivo:
1. Parenteral anticoagulants:– Indirect thrombin inhibitors: Heparin, Low molecular weight heparin,
Fondaparinux, Danaparoid– Direct thrombin inhibitors: Lepirudin, Bivalirudin
2. Oral anticoagulants:– Coumarin Derivative: Bishydroxycoumarin (dicumarol), Warfarin sodium,
Acenocoumarol – Inandione derivatives: Phenindione– Direct factor Xa inhibitors: Rivaroxaban
Used in vitro: Heparin: (150 U in 100 ml of blood) Calcium complexing agents: Sodium citrate 1.65 gm for 350
ml of blood – acid citrate dextrose solution – 75 ml in one unit of blood
For investigation: Sodium oxalate (10 mg for 1 ml blood and Sodium edetate – 2 mg for 1 ml of blood)
Heparin as PrototypeEndogenous - strongest organic acid present in the
BodyPresent in mast cells (MW – 75,000) – lungs, liver and
intestinal mucosaCommercially - from Ox lung and Pig mucosa
(slaughter house)Chemically, non-uniform mixture of straight chain
mucopolysaccharides with MW 10,000 to 20,000Carries strong electro-negative charges
Types - (i) Regular or unfractionated (UFH) Heparin (MW 5000 to 30,000) – IV or SC and (ii) LMWH (MW 2000 to 6000) – mostly SC
Heparin Actions• Indirect acting - Activates plasma antithrombin III (AT III)• Heparin-AT III complex inactivates clotting factors - Xa, IIa, IXa, XIIa
and XIIIa, but not VIIa (extrinsic pathway)– At low conc. Xa mediated conversion of Prothrombin to thrombin affected– Overall, Xa and IIa mediated conversion of fibrinogen to fibrin
• AT III (suicide inhibitor) – binds to clotting factors slowly to form stable complex. Heparin enhances it by
1.Heaprin creates scaffolding to bind each (clotting factors) other with AT III
2.A specific polysaccharide in heparin binds to AT III and induce conformational changes – bind factors
Heparin Actions – contd.• Inhibition of Xa needs only the 2nd mechanism (LMWH) -
fondaparinuxs • IIa needs both the mechanism • Antiplatelet action: High doses prevents platelet aggregation
prolongs Bleeding time• Lipaemic clearing• Pharmacokinetics:
– Highly ionized, not absorbed orally – given IV (instant action) and SC (slow action)
– Does no cross BBB and placenta– 100 U/kg dose half life is 1 Hr., but above this dose 1 – 4 Hrs– Should not with – Penicillin, hydrocortisone or tetracycline
Heparin mechanism of action
Heparin
Antithrombin IIIThrombin
Heparin – Contd.• Adverse effects:
1. Bleeding due to overdose – haematuria is 1st sign2. Thrombocytopenia – aggregation of platelets3. Hypersensitivity – urticaria, rigor, fever and
anaphylaxis etc.4. Alopecia and osteoporosis
• Contraindications: Bleeding disorders, Severe hypertension, GIT ulcer, Piles, SABE & malignancy, Ocular & neurosurgery, Chronic alcoholism, cirrhosis etc.
• Aspirin and antiplatelet drugs - caution
Low Molecular Weight Heparin (LMWH)
• MW : 2000 to 6000• MOA: Acts only by interfering with Xa –
inducing conformational change in AT III – smaller effect on aPTT – whole blood clotting time– Lesser antipatelet action and lower
incidence of haemorrhagic complications– Better Bioavailability on SC administration
(once daily dosing)– Better half life (4-6 Hrs)– Laboratory monitoring not needed (aPTT
and clotting time affected little)
• Uses: (1) Prophylaxis of DVT and Pulmonary embolism in Surgery, stroke and immobilized patients (2) DVT (3) UA and MI (4) RHD and AF (5) Haemodialysis patients
Interfered PT aPTT
IP N P
EP P N
CP P P
Dosage of Heparin• Unitage: Expressed in units as it is standardized by bioassay –
variable molecular size• 1 mg = 120-140 U activity• Administered as IV bolus 5000-10,000 u followed by 1000 u
/hr IV drip – adjusted with aPTT value– Pretreatment aPTT value and followed by 1.5 to 2.5 times during
therapy• Alternate: 10,000-20,000 deep SC every 8 Hrly (fine needle)• Or, Low dose SC – 5000 SC 8-12 Hry before and after surgery
to prevent DVT• Protamine Sulfate: Heparin antagonist – given IV (1mg =
100U) – cardiac and vascular surgery
Oral Anticoagulants
Warfarin • In vivo not in vitro• MOA: Competitive antagonist of
Vit.K – lowers the plasma level of vit. K dependent clotting factors– Inhibits VKOR needed to
generate active Vit.K
• Synthesis of clotting factors diminishes within few hours- at different times by diff. factors
• But anticoagulant action starts in 1-3 days only
• Commercially, mixture of R and S enantiomers
Warfarin – contd.• Kinetics: Completely absorbed from intestine and
99% plasma protein bound – only 1% free (many drugs can displace (sulfonamides, phenytoin – toxicity) – half life 36 hrs.
• Dosing: Risky – calculate risk-benefit ratio– Dose is individualized by repeated measurement of PT– Optimum ratio of PT: 2-2.5 in prophylaxis of DVT, 2-3
in DVT treatment and 3-3.5 in MI etc.• Uses: DVT, Pulmonary embolism and atrial
fibrillation (drug of choice – 3-4wks before and after conversion)
Warfarin
• ADRs: Bleeding – epistaxis, haematuria, bleeding GIT Intracranial haemorrhage– Minor bleeding – Vit K (takes long)– Fresh blood transfusion or blood factors– Other ADRs: Alopecia, dermatitis and diarrhoea etc.
• Contraindications: Same as heparin– Foetal warfarin syndrome: skeletal abnormality –
hypoplasia of nose, eye socket, hand bones and growth retardation
Warfarin• Factors enhancing warfarin effect: (1) Debility, malnutrition
etc. (2) Liver diseases, chronic alcoholism (3) Newborn (4) prolonged antibiotic therapy
• Factors decreasing warfarin effect: Pregnancy, Nephrotic syndrome and genetic warfarin resistance
• Drugs enhancing anticoagulant action: Broad spectrum antibiotics, Aspirin (platelet aggregation inhibition and hypoprothobinemic action), Newer cephalosporins (hypoprothobinemic; Chloramphenicol, allopurinol, tolbutamide and phenytoin (inhibits metabolism)
• Drugs reducing effect: Barbiturates, carbamazepine, OCP and Rifampicin
FIBRINOLYTICS
Fibrinolytics• Drugs used to lyse thrombi/clot to
recanalize occluded vessels – coronary artery
• MOA: Produce more plasmin - dissolves fibrin thread
• Drugs: Streptokinase, urokinase, alteplase (rt-PA), reteplase and tenecteplase
• Streptokinase – once popular – Binds to plasminogen and generate
plasmin– Non-specific – activates circulating +
fibrin bound plasminogen– non-specific fibrinogen depletory – but less effect than newer ones in fibrinolysis
Alteplase and Tenecteplase• Recombinant tissue plasminogen activator (rt-PA) – human tissue culture
– costlier than Streptokinase• MOA: tissue specific thrombolytic (acts on fibrin bound plasminogen
within thrombus) – also interferes with circulating plasminogen (50%) – inactivated by PAI-1
• Plasma half life 5 minutes – given slow IV (heparin needed)• MI: 1o mg IV bolus – followed by rest 90 mg infusion for 90 minutes• Pulmonary embolism: 100 mg slow IV for 2 Hrs
• Tenecteplase: genetically engineered, higher fibrin selectivity, not inactivated by PAI-1, can be injected over 10 seconds single bolus
Uses of Thrombolytics
• AMI – alternative to PCI with stent placement – aspirin + heparin co-administered to prevent re-occlusion
• DVT: leg, pelvis and shoulder• Pulmonary embolism• Stroke: selected patients
Antifibrinolytics
• Epsilon amino-caproic acid (EACA) and Tranexamic acid
• MOA: Inhibit Plasminogen activation and clot dissolution
• EACA: Specific antidote for fibrinolytic agents – also adjunctive value in other conditions
• Tranexamic acid: More potent than EACA– Uses: fibrinolytic drugs, Bypass surgery, Menorrhagia,
Recurrent epistaxis, tonsillectomy & tooth extraction (haemophiliacs)
Antiplatelet Drugs (antithrombotic drugs)
Antiplatelet Drugs (antithrombotic drugs)
• Drugs which interferes with platelet function and used in prophylaxis of thromboembolic disorders.
• Drugs: Aspirin, Dipyridamole, Ticlodipine, Clopidogrel and Prasugrel
• Aspirin as antiplatelet:– Irreversible Inhibition of COX 1 and TX synthase– Suppress TXA2 (generated by platelets) in low doses (75-150 mg) – till
fresh platelets are formed – prolonged bleeding time– Suppress COX-1 and decrease PGI2 synthesis in vessel wall – but
endothelial cells immediately re-synthesize fresh enzyme– Also inhibits release of ADP from platelets and their sticking to each
other – but not to adhesion to damaged vessel walls
Antithrombotic drugs - Dipyridamole
• Powerful coronary dilator – increases total coronary flow
• MOA: Adeosine is local mediator involved in autoregulation of coronary flow in response to Ischaemia– Dipyridamole prevents uptake and degradation of
adenosine and increases platelete cAMP – potentiates PGI2 – interferes platelete aggregation
• Uses: Enhance antiplatelet action of Aspirin – lowers the risks of TIAs – 150-300 mg / day
Antithrombotic drugs - Ticlodipine• First thienopyridine derivative – Prodrug (active
metabolites in liver)• MOA: Inhibits fibrinogen as well as ADP induced platelet
aggregation– Gi coupled P2Y12 (P2YAC) purinergic receptors mediate adeylyl
cyclase inhibition due to ADP – blocked irreversibly– No effect on TXA2– Irreversible blockade of P2YAC – platelet inhibiton cumulates –
effects appear in 8-10 days• Uses: Stroke prevention, TIA, intermittent claudication,
unstable angina, coronary bypass, prevention of MI• Serious ADRs – Bleeding, neutropenia, hamolysis,
thrombocytopenia and jaundice - replaced by Clopidogrel
Antithrombotic drugs - Clopidogrel• Similar MOA to Ticlodipine – irreversible blockade of platelet
function– Safer and better tolerated than Ticlodipine
• Advantages over Aspirin in Ischaemia – lower incidence of ischaemic events
• Synergistic action with aspirin – prevention of Ischaemic episodes• Kinetics: Prodrug like Ticlodipine, 50% absorbed orally
– Only a fraction slowly activated in liver by CYP2C19 slow acting– CYP2C19 – genetic polymorphism - interindivdual variability in
antiplatelet action– Takes 5-7 days for action
• ADRs: Bleeding most common, neutropenia and thrombocytopenia rarely
• Dose: 75 mg OD
Antithrombotics – Other Drugs• Prasugrel: Faster and potent P2Y12 (P2YAC)
purinergic receptors Blocker• Newer Drugs: Glycoprotein (GP) IIb/IIIa receptor
antagonists: Abciximab, Ebtifibatide and Tirofiban– Newer class of drugs– Blocks the key receptor involved in platelet
aggregation– Collagens, thrombin, TXA2 and ADP etc. – acts
through - GLP IIb/IIIa is an adhesive receptor (integrin) on platelet surface
– GLP IIb/IIIa antagonists block platelet aggregation
Uses of antithrombotics • Coronary Artery Disease: Aspirin 75-150 mg/day in all
individuals with evidence of coronary artery disease – clopidogrel is an alternative in ischaemia
• Acute Coronary Syndromes: Aspirin 325 mg orally and LMW heparin – NSTEMI and STEMI
• Cerebrovascular accidents: Do not alter the course of cerebral thrombosis – reduces incidence of TIA
• Prosthetic Heart Valves and arteriovenous shunts: In conjunction with warfarin
• Venous thrombosis: DVT and PE• Peripheral vascular disease
Must Know
• Heparin, LMWH and Protamine sulfate• Warfarin• Fibrinolytics (Thrombolytics)• Antiplatelet Drugs – Aspirin, Dipyrydamole
and Clopidogrel
THANK YOU