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Ticagrelor versus clopidogrel in African-American patients with stable coronary artery disease: a randomized, open-label, multiple-dose, crossover study.

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Presentation on theme: "Ticagrelor versus clopidogrel in African-American patients with stable coronary artery disease: a randomized, open-label, multiple-dose, crossover study."— Presentation transcript:

1 Ticagrelor versus clopidogrel in African-American patients with stable coronary artery disease: a randomized, open-label, multiple-dose, crossover study Ron Waksman, MD Washington Hospital Center, Washington DC On behalf of J Maya AstraZeneca LP, Wilmington, DE DJ Angiolillo University of Florida, Jacksonville, FL G Carlson AstraZeneca LP, Wilmington, DE R Teng AstraZeneca LP, Wilmington, DE R Caplan AstraZeneca LP, Wilmington, DE K Ferdinand Tulane University, New Orleans, LA

2 Ron Waksman, MD Consulting: Abbott Laboratories, AstraZeneca, Biotronik Inc., Boston Scientific Corporation, Medtronic Inc. Grant Support: Volcano Therapeutics, Inc. Honoraria: Abbott Laboratories, AstraZeneca, Boston Scientific Corporation, Medtronic Inc.

3 Disclosure Statement of Financial Interest
Within the past 12 months, I or my spouse/partner have had a financial interest/arrangement or affiliation with the organization(s) listed below Affiliation/Financial Relationship Company Grant/Research Support Consulting Fees/Honoraria Boston Scientific Biotronik Astra Zeneka Lilly Dahichi Medtronic Abbott Vascular Astra Zeneca

4 Rationale: pharmacodynamic study of ticagrelor in African-American patients
Ticagrelor is an oral, reversibly binding ADP receptor antagonist acting via the P2Y12 receptor The PLATelet inhibition and patient Outcomes (PLATO) phase III study evaluated ticagrelor vs clopidogrel in patients with ACS1 at 12 months, composite endpoint of death from vascular causes, MI, or stroke was significantly lower with ticagrelor versus clopidogrel: 9.8% vs. 11.7%; HR = 0.84 (95% CI: 0.77−0.92); p<0.0011 Few African-American patients were enrolled in the PLATO trial Ticagrelor 1. Wallentin et al. N Engl J Med. 2009;361:

5 Variability in clopidogrel response in African-American patients
High post-treatment platelet reactivity (HPR) is an independent risk factor for 12-month cardiovascular death and non-fatal MI1 Clopidogrel hyporesponse has been reported in up to 30% of patients1,2   CYP2C19 is the primary enzyme involved in converting the clopidogrel prodrug into an active metabolite1,3 African-Americans have a high prevalence of the loss-of-function allele CYP2C19*2, which could contribute to their higher rate of clopidogrel non-response2 1. Smith SC Jr et al. Circulation. 2006; 113: e166–e Pendyala LK et al. Am Heart J. 2013; 166:266– FDA Drug Safety Communication: Reduced effectiveness of Plavix (clopidogrel) in patients who are poor metabolizers of the drug. Available at: Accessed: 12 February

6 Randomized, open-label, crossover study of the antiplatelet effects of ticagrelor versus clopidogrel in African-American patients with stable CAD We evaluated platelet reactivity during the onset and repeated dose administration of ticagrelor compared with clopidogrel in African American patients with stable coronary artery disease (CAD) receiving chronic low-dose acetylsalicylic acid (ASA; 75 to 100 mg) as background therapy

7 Study sites and investigators
DE, MD, DC Ron Waksman Washington DC Michael Main Kansas City MO Alberto Yataco Towson MD Michael Stillabower Newark DE Rodolfo Sotolongo Beaumont TX Dominick Angiolillo Jacksonville FL Keith Ferdinand Atlanta GA Anthony Alfieri Wilmington Luis Tami Hollywood

8 Study design Treatment Period 1 Treatment Period 2 7–9 days 7–9 days
Randomization Treatment A: clopidogrel 600mg/75mg OD Treatment B: ticagrelor 180mg/90mg BID Platelet tests Platelet tests Platelet tests Platelet tests Screening Visit 1 10–14 day washout period Treatment B: ticagrelor 180mg/90mg BID Treatment A: clopidogrel 600mg/75mg OD Platelet tests Platelet tests Platelet tests Platelet tests Visit 2 Visits 3 & 4 Visit 5 Visits 6 & 7 Study D5130L00013; ClinicalTrials.gov Identifier: NCT

9 Patient population Target patient population Key exclusion criteria
African-American patients with stable CAD taking mg acetylsalicylic acid (ASA) daily Stable angina pectoris (current or history of) Objective evidence of CAD Previous myocardial infarction (MI) or previous revascularisation, i.e. percutaneous coronary intervention (PCI) or coronary artery bypass graft (CABG) Key exclusion criteria Any indication for oral anticoagulant or dual antiplatelet treatment during study period Concomitant therapy with strong CYP3A inhibitors, CYP3A substrates with narrow therapeutic index, or strong CYP3A inducers Increased bleeding risk Diabetic patients with HbA1c ≥10%

10 Primary and secondary objectives
Primary objective Compare on-treatment platelet reactivity 2 hours after a loading dose of ticagrelor or clopidogrel P2Y12 Reaction Units (PRU) using VerifyNow™; least squares means and 2-sided 95% confidence intervals (CIs) Secondary objectives Compare on-treatment platelet reactivity with ticagrelor vs clopidogrel at 0.5 and 8 hours after loading dose; at 2 hours and 8 hours on Day 7; end of dosing on Day 8 (12 hours after last evening dose of ticagrelor; 24 hours after the last morning dose of clopidogrel) P2Y12 Reaction Units (least squares means; 95% CI) inhibition of P2Y12 receptor at 2 hours after loading dose = 1−{PRU after study drug/PRU at baseline} X 100 % Evaluate plasma concentration of ticagrelor and its active metabolite AR–C124910XX Assess safety of ticagrelor by AEs, physical examination and vital signs

11 Study population (n=34) Treatment and characteristics
Randomized and dosed: n (%) 34 (100.0) Completed 14 days’ treatment: n (%)1 30 (88.2) Completed follow-up period: n (%) 31 (91.2) Median age: years (range) 62.5 (50–75) Age ≥65: n (%) 12 (35.3) Male: n (%) 23 (67.6) Black or African American: n (%) Median weight: kg (range) 91 (49-177) Hypertension: n (%) Dyslipidemia: n (%)2 34 (100) Type II diabetes: n (%) 17 (50.0) Coronary artery disease history Stable angina pectoris: n (%) 6 (17.6) Past MI: n (%) Median time since last MI: years (range) 15 (44.1) 4.8 (1.1–25.6) Previous PCI: n (%) 22 (64.7) Previous CABG: n (%) 16 (47.1) Congestive heart failure: n (%) Past Current (not symptomatic) 2 (5.9) Valvular heart disease: n (%) Current peripheral arterial occlusive disease: n (%) Past pulmonary embolism: n (%) 1 (2.9) 1Patients who completed 7, 8, or 9 days of both sequences were identified as Completed 14 days of treatment 2Including hypercholesterolemia

12 Primary outcome: platelet reactivity 2 hours after loading dose
Difference in least squares mean −183.6 (95% CI: −213.9, −153.3) p<0.001 P2Y12 reaction units: values expressed as the least-squares means with 2-sided confidence intervals (CI)

13 Time course of platelet reactivity
350 Clopidogrel Ticagrelor 300 250 200 *** P2Y12 reaction units 150 100 50 *** *** *** *** *** *** –50 Baseline 0.5 2 8 Baseline 2 8 12–24 Hours post loading dose Hours post maintenance dose Values are expressed as the least-squares mean and 95% confidence intervals. ***p<0.001 for ticagrelor versus clopidogrel Note: patients with low baseline PRU values (indicating an incomplete washout from anti-platelet therapy) are excluded from this analysis during the period corresponding to the low baseline value

14 Inhibition of platelet reactivity over time
12–24 0.5 8 100 90 80 70 60 50 20 –20 2 Reduction from baseline (%) Clopidogrel Ticagrelor *** Hours post loading dose Baseline Hours post maintenance dose 40 30 10 –10 ***p<0.001 Inhibition of P2Y12 receptor after loading dose = 1−{PRU after study drug/PRU at baseline} X 100 % Note: Patients with low baseline PRU values (indicating an incomplete washout from anti-platelet therapy) excluded during the period corresponding to the low baseline value.

15 High on-treatment platelet reactivity: % patients with PRU ≥208
Ticagrelor Clopidogrel p< Percent of patients p<0.0001 p<0.001 p<0.01 p=0.0102 Hours post loading dose Hours post maintenance dose Baseline (BL); P2Y12 reaction units (PRU); p = Fisher’s Exact Test p value (2-tail)

16 Plasma concentration-time profiles: ticagrelor
Mean ticagrelor plasma concentration (ng/mL) ONSET-OFFSET (n = 52–57) RESPOND non-responders Tic  Clop (n = 15–20) RESPOND responders Tic  Clop (n = 11–14) RESPOND responders Tic  Tic (n = 10–13) Time (hours) 1 100 10,000 4 8 12 16 20 24 10 1,000 Mean ticagrelor plasma concentration (ng/mL) 3000 2000 1500 1000 500 70 10 0.5 2 8 12 Hours post loading dose Hours post maintenance dose Left hand plot: geometric mean (± standard deviation) ticagrelor plasma concentrations in African-American patients following a loading dose (180mg) and subsequent maintenance dose (90mg) of ticagrelor; patients with low baseline PRU values (indicating an incomplete washout from anti-platelet therapy) are excluded from this analysis during the period corresponding to the low baseline value. Right hand plot: similar geometric mean ticagrelor plasma concentrations following a ticagrelor loading dose (180mg) in patients with coronary artery disease (Husted et al. Clin Pharmacokinet 2012;51:397–409). Baseline (BL); clopidogrel (Clop); P2Y12 reaction units (PRU); ticagrelor (Tic)

17 Plasma concentration-time profiles: AR-C124910XX
Mean AR-C124910XX plasma concentration (ng/mL) 700 500 300 200 100 10 1 0.5 2 8 12 Hours post loading dose Hours post maintenance dose Mean AR-C124910XX plasma concentration (ng/mL) Time (hours) 1 10 1,000 4 8 24 100 16 20 12 ONSET-OFFSET (n = 34–57) RESPOND non-responders Tic  Clop (n = 10–20) RESPOND responders Tic  Clop (n = 9–14) RESPOND responders Tic  Tic (n = 5–13) Left hand plot: geometric mean (± standard deviation) AR-C124910XX plasma concentrations in African-American patients following a loading dose (180mg) and subsequent maintenance dose (90mg) of ticagrelor; patients with low baseline PRU values (indicating an incomplete washout from anti-platelet therapy) are excluded from this analysis during the period corresponding to the low baseline value. Right hand plot: similar AR-C124910XX geometric mean plasma concentrations following a ticagrelor loading dose (180mg) in patients with coronary artery disease (Husted et al. Clin Pharmacokinet 2012;51:397–409). Baseline (BL); clopidogrel (Clop); P2Y12 reaction units (PRU); ticagrelor (Tic)

18 Safety: patients with at least one adverse event
Preferred term, n (%) Ticagrelor (n=34) Clopidogrel (n=31) Hemorrhoidal hemorrhage 1 ( 2.9%) 0 ( 0.0%) Epistaxis Dyspnea 2 ( 5.9%) Application site bruise 1 ( 3.2%) Vessel puncture site bruise Blood glucose decreased Contusion Musculoskeletal pain Acute MI Vaginal hemorrhage One patient experienced a serious AE (moderate intensity acute MI) but this was not considered to be treatment-related (the last dose of ticagrelor was taken 14 days earlier) No deaths were reported during the study No other notable safety findings occurred in terms of adverse events, vital signs or physical examinations

19 Conclusions In African-American patients with stable CAD on low-dose daily aspirin, ticagrelor compared with clopidogrel provided faster onset and greater extent of platelet inhibition Plasma concentrations of ticagrelor and AR-C124910XX were consistent with those observed in previous studies of ticagrelor There were no unexpected safety findings with ticagrelor These findings suggest that the benefit/risk profile seen with ticagrelor in PLATO may be extrapolated to African-American patients with ACS


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