An#- Coagulant An#- Thrombo#c An#- Platelet Drugs

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Transcription:

An#- Coagulant An#- Thrombo#c An#- Platelet Drugs 1

ANTICOAGULANT CLASSES INHIBITORS OF CLOTTING FACTOR SYNTHESIS WARFARIN (COUMADIN ) Rivaroxaban (Xarelto ) INHIBITORS OF THROMBIN HEPARIN, LEPIRUDIN (REFLUDAN ) Dabigatran Etexilate Mesylate (Pradax ) PREVENTION OF PLATELET AGGREGATION ASA TICLOPIDINE (TICLID ) CLOPIDOGREL (PLAVIX ) TIROFIBAN (AGGRASTAT ) EPTIFIBATIDE (INTEGRILIN ) Prasugrel (Effient ) Ticagrelo (Brilinta ) 2

ANTICOAGULANTS WARFARIN (COUMADIN) ACTS IN LIVER BY INHIBITING REDUCTION OF VIT. K TO A FORM NEEDED FOR SYNTHESIS OF FACTORS VII, IX, X, AND PROTHROMBIN HEPARIN POTENTIATES THE ANTICOAGULANT ACTIVITY OF ENDOGENOUS ANTITHROMBIN III 3

COUMADIN EFFECT IN 24 HRS. PEAK 3 4 DAYS MAY CAUSE SERIOUS HEMORRHAGE ANTIDOTE VIT. K REQUIRES 12 24 HRS. MAY REQUIRE TRANSFUSION 4

Warfarin 5

Warfarin Outpa#ent Rx s 2004-31 million Ranked 1 st in 2003 and 2004 for drug related deaths due to adverse effects in therapeu#c use 10 to 16 % of pa#ents will have a major bleed at some point No longer acceptable to D/C warfarin rou#nely!!! 5

COUMADIN MONITOR WITH INR (INTERNATIONAL NORMALIZED RATIO) STANDARIZES THE VARIOUS LABORATORIES THROMBOPLASTINS (human or rabbit) 6

Recommended range for oral 7

Recommended range for oral INR target range 2.0 to 3.0 Prophylaxis/treatment of venous thrombosis Treatment of pulmonary embolism Prevention of systemic embolism recurrent systemic embolism Acute myocardial infection Valvular heart disease Valvular replacement with tissue Atrial fibrillation INR target range 2.5 to 3.5 Mechanical replacement heart valves (High risk) 7

INTERNATIONAL NORMALIZED RATIO (INR) INR < 2.0 out of therapeutic range (poorly managed needs adjustment) INR 2.0 4.0 ok to do surgery with local measures INR > 4.0 out of therapeutic range (warfarin dosage needs adjustment ) 8

Warfarin (Coumadin ) Good Con#nue warfarin therapy Hemorrhagic disorders Correct INR Bad D/C warfarin therapy Malpractice Cerebrovascular complications Thrombosis formation 9

10 10

11 11

12 12

John Kern PhD - email communica#on Thanks, Jim, for the update. I have removed article 00179 from my queue. Also, I have finished reviewing the OOOOE article on warfarin. Bottom line, there is no statistical weight whatsoever behind the article's recommendation to withhold warfarin. The EUV estimates are separated by only 0.02, and all of the probabilities used to estimate the two EUV values are themselves estimates (from other literature, no less). This article is in no way a breakthrough or landmark. Would it be okay for me to call you and discuss in more detail my critique of the article? I can call most any time/day this week or next; just let me know. I hope your new year has gotten off to a great start! 13 13

Ref. Herman W., et. al., Current Perspec#ves On Dental Pa#ents Receiving Coumarin An#coagulant Therapy, JADA March 1997 James L. Rutkowski D.M.D., Ph.D. 14

TAKE-HOME MESSAGE MUST HAVE A RECENT INR (WITHIN 30 DAYS IF NO CHANGES IN MEDS) IF ANY MED OR DOSAGE CHANGES THEN MUST REPEAT INR BEST IF SAME- DAY FOR MAJOR PROCEDCURES!!! 15

Rivaroxaban (Xarelto ) Mechanism: Factor Xa inhibitor In coagula#on factor X Xa (produces fibrin) 16 16

Rivaroxaban (Xarelto ) Prophylaxis of deep vein thrombosis (DVT) which may lead to pulmonary embolism (PE) in pts undergoing knee or hip replacement surgery 10 mg once daily 5-6% pts have a bleeding event 17 17

Rivaroxaban (Xarelto ) Measurement of Effect Prolongs prothrombin #me (PT) and ac#vated par#al thromboplas#n #me (aptt) Predic#ve treatment values not established No data on INR use Hip replacement - 35 days Knee replacement - 12 days 18 18

Rivaroxaban (Xarelto ) Dental considera#ons bleeding occurs with 10mg/day Consult No reports of interac#ons with amoxicill, cephalexin, cefazolin, ampicillin, & clindamycin 19 19

Rivaroxaban (Xarelto ) Drug interac#ons Inhibitors of CYP3A4 Ketocanazole (an#fungal) Clarithromycin (Biaxin ) Erythromycin NSAIDS 20 20

THROMBOGENESIS PLATELET AGGREGATION COAGULATION 21

ARTERIAL COAGULATION CASCADE TO FIBRIN STRANDS ARTERIES PLATELETS ADHERE TO DAMAGED VESSSEL WALLS AGGREGATE CORE FOR FIBRIN STRANDS OCCLUDE ARTERIAL FLOW ISCHEMIA OF LOCAL TISSUES 22

VENOUS THROMBI FIBRIN STRANDS EMBOLIZE GREAT DISTANCES LODGE IN PULMONARY ARTERIES 23

THROMBOGENESIS LOCALIZED RESPONSE INITIATED BY SUBSTANCES RELEASED FROM PLATELETS AND ENDOTHELIUM LIMITED BY LOCALIZED ANTICOAGULANT MECHANISMS ANTITHROMBIN II 24

ANTIPLATELET DRUG ASPIRIN TX: PREVENTION OF MI & THROMBOTIC STROKE 81 mg/day LITTLE RISK FOR DENTAL SURGERY 25

ANTIPLATELET DRUG DIPYRIDAMOLE (PERSANTINE) PREVENTS PLATELET ADHESION TO ENDOTHELIAL SURFACES MIXED WITH ASA ENHANCES ANTITHROMBOTIC ON ARTIFICIAL SURFACES VALVULAR & CARDIAC PROSTHESES DIALATES CORONARY ARTERIES 26

PLAVIX - CLOPIDOGREL BLOCKS THE ADP RECEPTOR WHICH PREVENTS THE BINDING OF FIBRINOGEN TO THAT SITE DOES NOT ALTER THE RECEPTOR REDUCES # OF FUNCTIONAL ADP RECEPTORS 27

PLAVIX - CLOPIDOGREL 28

PLAVIX - CLOPIDOGREL MONITOR WITH PLATELET AGGREGATION INITIAL 2 TO 4 WEEKS MAY CAUSE THROMBOCYTOPENIA CHECK PLATELETS RARELY NECESSARY TO D/C SURGERY IF MULTIPLE SITES OR EXTENSIVE? get consulta#on DISCONTINUE 7 DAYS PRIOR TO PROCEDURE (RARELY NECESSARY!) 28

PLAVIX - CLOPIDOGREL - WOW!!!! 30% of popula#on has a gene#c variant in liver metabolizing enzymes that affect efficacy of clopidogrel - no effect at all CYP2C19 converts clopidogrel to an ac#ve metabolite. Genes which encode and express liver enzymes responsible for metabolism exist in several polymorphic states (CYP2C19 has 4 variants with reduced func#on) Rela#ve reduc#on of 32% in ac#ve metabolite 53% higher risk for primary efficacy outcome of death from cardiovascular causes, MI, stroke Stent thrombosis in carriers 3 X that of non- carriers Ref. Mega JL et al., Cytochrome P- 450 Polymorhisms and Response to Clopidogrel NEJM, 2009, 360(4):354-62 29 29

Prasugrel (Effient ) An#platelet agent and aggrega#on inhibitor For thrombo#c cardiovascular events (stent thrombosis Clopidogrel Non- fatal subsequent heart a?acks Prasugrel Non- fatal subsequent heart a?acks 9.1% 7.0% Deaths and strokes equal Risk of significant fatal bleeding + ++ 30 30

Effient - lilly 31 31

Pro- drug Prasugrel (Effient ) Irreversibly blocks P2Y12 component of adenosine diphosphate (ADP) receptors on platelets for their lifespan platelet ac#va#on and platelet aggrega#on Normal platelet ac#vity does not return (new platelets in 5 to 9 days azer D/C Loading dose 60 mg followed by maintenance dose of 10 mg daily. Should take with ASA 75 to 325 mg daily 32 32

Prasugrel (Effient ) Gene#c variants in liver metabolizing enzymes do not affect efficacy Undergoes rapid intes#nal and serum metabolism via esterase- mediated hydrolysis to a thiolactone (inac#ve metabolite), which is then converted, via CYP3A4 & CYP2B6 enzyme oxida#on, to the ac#ve metabolite designated as R- 138727. 33 33

Ticagrelor (Brilinta ) Reduce rate of thrombo#c cardiovascular events in pts with acute coronary syndrome (ACS): unstable angina, non- ST eleva#on MI, ST eleva#on MI More effec#ve than clopridogrel 34 34

Ticagrelor (Brilinta ) Drug interac#ons Inhibitors of CYP3A4 Ketocanazole Itaconazole Voriconazole Clarithromycin (Biaxin ) Erythromycin NSAIDs 35 35

Ticagrelor (Brilinta ) Mechanism: An ac#ve, reversible platelet inhibitor CYP3A4 converts #cagrelor to another ac#ve reversible platelet inhibitor - which is the major ac#ve metabolite Act at the ADP- receptor Loading dose 180 mg then 90 mg BID Give with loading dose ASA 325 mg then 75-100 mg. Daily ASA doses above 100 mg/day reduce effec#veness of #cagrelor and should be avoided 36 36

Ticagrelor (Brilinta ) Dental considera#ons Do NOT D/C without consulta#on Expect bleeding and echymosis Pts ozen have SOB No coagula#on parameters suggested 37 37