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LBCT March 29, 08 ISAR REACT 3 A. Kastrati, F.-J. Neumann, J. Mehilli, S. Schulz, G. Richardt, R. Iijima, R.A. Byrne, P.B. Berger, A. Schömig Bivalirudin.

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Presentation on theme: "LBCT March 29, 08 ISAR REACT 3 A. Kastrati, F.-J. Neumann, J. Mehilli, S. Schulz, G. Richardt, R. Iijima, R.A. Byrne, P.B. Berger, A. Schömig Bivalirudin."— Presentation transcript:

1 LBCT March 29, 08 ISAR REACT 3 A. Kastrati, F.-J. Neumann, J. Mehilli, S. Schulz, G. Richardt, R. Iijima, R.A. Byrne, P.B. Berger, A. Schömig Bivalirudin Versus Unfractionated Heparin in Biomarker Negative Patients With Stable and Unstable Angina Undergoing PCI ISAR-REACT 3 (Intracoronary Stenting and Antithrombotic Regimen- Rapid Early Action for Coronary Treatment 3) ClinicalTrials.gov Identifier NCT00262054

2 LBCT March 29, 08 ISAR REACT 3 Background Bivalirudin has not been compared with unfractionated heparin during PCI in the modern era, or in patients who have received optimal pretreatment with clopidogrel.

3 LBCT March 29, 08 ISAR REACT 3 Aim To compare bivalirudin alone to unfractionated heparin alone in biomarker negative pts undergoing PCI pretreated with clopidogrel 600 mg for >2 hours Hypothesis Bivalirudin is superior to UFH for biomarker negative patients undergoing PCI after optimal pretreatment with clopidogrel

4 LBCT March 29, 08 ISAR REACT 3 Exclusion Criteria Acute coronary syndromes with positive biomarkers or ST-segment elevation on ECG Cardiogenic shock Active bleeding, bleeding diathesis Impaired renal function (creatinine >3 mg/dl)

5 LBCT March 29, 08 ISAR REACT 3 Primary (Quadruple) Endpoint at 30 Days Composite rate of: –Death –Myocardial infarction (defined as CK-MB ≥2x upper limit normal ) –Urgent target vessel revascularization –Major bleeding (according to the REPLACE-2 criteria, JAMA ′03 ) Intracranial, intraocular, or retroperitoneal bleeding, or Clinically overt bleeding resulting in a decrease in Hb>3 g/dL, or Any decrease in Hb>4 g/dL, or Transfusion of >2 units of packed red blood cells or whole blood

6 LBCT March 29, 08 ISAR REACT 3 Secondary (Triple) Endpoint at 30 Days Composite rate of: –Death –Myocardial infarction –Urgent target vessel revascularization

7 LBCT March 29, 08 ISAR REACT 3 2,289 Pts 30-day Follow-up 2,281 Pts UFHBivalirudin PCI 4,570 Patients (600 mg clopidogrel) Study Population Double-blind randomization; double-dummy administration

8 LBCT March 29, 08 ISAR REACT 3 DES 84% DES 82% BMS PTCA 6% 10% 7% 11% Type of PCI Bivalirudin UFH

9 LBCT March 29, 08 ISAR REACT 3 Cumulative incidence (%) 0 2 4 6 8 10 05 15202530 Days after randomization Secondary (Triple) Endpoint Death, MI, UTVR 5.0% 5.9% RR=1.16 [95% CI, 0.91-1.49], P=0.23 Bivalirudin UFH

10 LBCT March 29, 08 ISAR REACT 3 Incidence (%) P=0.008 Bleeding Events P=0.0001P=0.15 Bivalirudin UFH

11 LBCT March 29, 08 ISAR REACT 3 Days after randomization Cumulative incidence (%) 0 2 4 6 8 10 05 15202530 Primary (Quadruple) Endpoint Death, MI, UTVR, Major Bleeding 8.3% 8.7% RR=0.94 [95% CI, 0.77-1.15], P=0.57 Bivalirudin UFH

12 LBCT March 29, 08 ISAR REACT 3 Conclusion In biomarker negative patients with stable and unstable angina undergoing PCI pretreated with clopidogrel 600 mg for >2 hours, bivalirudin does not improve “net clinical benefit” – the quadruple endpoint – at 30 days compared to UFH, although it significantly reduces bleeding

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