Clopidogrel (Plavix)

1. Clopidogrel (Plavix) By Oksana Ekkert

3. The routes of elimination for the 200 drugs sold by prescription in the United States according to the RxList data listed in April 2008 1

5. Variant alleles in CYP2C19 genotype. CYP2C19 Nucleotide change Effect Europeans Blacks Asians *1 Wild type 85% 82% 65% *2 681G->A Truncated protein 13-19% 10-25% 20-30% *3 636G->A Truncated protein <1% 0-2% 5-13% *17 -806C->T -3402C->T Increased translation 18% 18% 4%

7. Comparison of pro-drugs and active drugs and clinical consequences Drug type Metabolizer Phenotype Effect on drug metabolism Potential consequence Prodrug Needs metabolism to work (clopidogrel) Poor to intermediate Slow Poor drug efficacy, patient at risk of therapeutic failure due ↓ levels of active drug. Accumulation of prodrug, patient at increased risk of drug-induced side effects. Ultrarapid Fast Good drug efficacy, rapid effect. Possible accumulation of active drug -> potential of adverse effects. Active drug Metabolized to inactive drug (omeprazole) Poor to intermediate Slow Accumulation of active drug, patient is at increased risk of drug-induced side effects. Patient requires lower dosage . Ultrarapid Fast Poor drug efficacy, patient is at risk of therapeutic failure. Patient likely will require higher dosage.

9. P2X 1 P2Y 12 ATP Shape change Angiolillo DJ et al JACC 2007 P2Y 1 G q Initiation of Platelet Aggregation IP3 PKC GP IIb/IIIa receptor activation G 12 DAG + Shape change Granule secretion Stabilization of Platelet Aggregation β γ GP IIb/IIIa receptor activation Rap1b PKB/Akt α i AC cAMP VASP VASP-P cAMP PI3K Clopidogrel 85% inactive metabolites (Esterases in blood) Gastro-intestinal absorption ADP Ca 2+ flux Ca 2+ mobilization PLC β MLCK-P “ Rho” Hepatic CYP Biotransformation GP IIb/IIIa receptor activation PGE 1 PIP2 G i 15% active metabolite HOOC * HS N O Cl OCH 3 N S O Cl O CH 3 C AC G s

10. T.E. Klein , J.T. Chang, M.K. Cho, K.L. Easton, R. Fergerson, M. Hewett, Z. Lin, Y. Liu, S. Liu, D.E. Oliver, D.L. Rubin, F. Shafa, J.M. Stuart and R.B. Altman , &quot; Integrating Genotype and Phenotype Information: An Overview of the PharmGKB Project &quot; ( 220k PDF ), The Pharmacogenomics Journal (2001) 1, 167-170 .

13. Clopidogrel Response Variability 20% do not have adequate response GP IIb/IIIa receptor expression Hepatic Metabolism Cytochrome P450 pathway Poor compliance Inadequate administration Variable absorption Genetic polymorphisms CYP2C19PMs, CYP2C9*3, ABCB1 Drug-drug interactions Genetic polymorphisms P2Y12 receptor Alternate pathways of platelet activation Genetic polymorphisms O’Donoghue M, Wiviott SD. Circulation. 2006;114:e600-e606 Simon T et al.NEJM. 2009;363-75 Feher G et al. Clin Genetics. 2009; 75:1-18. Intestinal Absorption P2Y 12 Receptor (irreversible inhibition) Active Metabolite

14. Mechanisms of Clopidogrel Response Variability Inhibition of Platelet Aggregation (Wide Response Variability) 1 Clopidogrel Bisulfate Intestinal Absorption Inactive Carboxylic Acid Metabolite CYP3A4 CYP3A5 CYP2C19 CYP2C9 Active Thiol Metabolite P2Y 12 Receptor Limited absorption capacity with ceiling effect at 600mg loading dose 7 Hepatic P450 Cytochromes CYP3A4 inducers: rifampin CYP3A4 inhibitors: erythromycin 2C19 Genetic polymorphisms 2C19 inhibitors Multistep Conversion 15% Esterases 85% 1. Gurbel PA et al. Thromb Res . 2007;120:311-21. 2. Taubert et al. Clin Pharmacol . 2006;80:486-501. 3. von Beckerth et al. Eur Heart J. 2007;28:1814-9. P-glycoprotein (MDR1 3435T genotype) 2 ? Smoking (induction) CYP1A2 CYP2B6, 2C19 2C9*3 Genetic polymorphisms

15. Why do we need PPI’s with clopidogrel? Deepak LB, et al. Circulation 2008; 118:1894-1909

16. K i ( μ M) values of PPI’s for CYP2C19 enzyme Li X, Andersson TB, Ahlstrom M, Weidolf L. Comparison of inhibitory effects of the proton pump-inhibiting drugs omeprazole, esomeprazole, lansoprazole, pantoprazole, and rabeprazole on human cytochrome p450 activities. Drug Metab Dispos. 2004 August 1;32(8):821-7. Brand Generic Ki (μM) Model Inhibitor HLM a rCYP2C19 b Ticlopidine HLM 0.31±0.05 rCYP2C19 0.68±0.04 Prilosec omeprazole 6.2±0.8 2.4±0.05 Aciphex rabeprazole 21.3±2.8 (2.4±0.1) c 18.8±1.3 (2.8± 0.1) d Nexium esomeprazole 8.6±1.0 7.9±0.5 Prevacid lansoprazole 0.45±0.07 0.74±0.09 Protonix pantoprazole 69.4±9.2 15.3±1.1 a,b marker reaction used was S-Mephenytoin 4-Hydroxylation c,d rabeprazole thioether; HLM=human liver microsomes

17. Risk of All-Cause Mortality and Recurrent ACS in Patients Taking Clopidogrel and PPI Ho PM, Maddox TM, Wang L, et al. JAMA. 2009;301(9):937-944. 0.70 0.60 0.50 0.40 0.30 0.20 0.10 0 0 90 180 270 360 450 540 630 720 810 900 990 1080 Days Since Discharge Proportion of Deaths or Recurrent ACS Neither clopidogrel nor PPI PPI without clopidogrel Clopidogrel + PPI Clopidogrel without PPI