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Welcome Ask The Experts March 24-27, 2007 New Orleans, LA.

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Presentation on theme: "Welcome Ask The Experts March 24-27, 2007 New Orleans, LA."— Presentation transcript:

1 Welcome Ask The Experts March 24-27, 2007 New Orleans, LA

2 FUSION II: Follow-Up Serial Infusions of Nesiritide for the Management of Patients With Heart Failure Clyde W. Yancy, MD, FACC, FAHA, FACP Medical Director Baylor Heart & Vascular Institute Dallas, TX

3 Results of the Follow-up Serial Infusions of Nesiritide for the Management of Patients With [Advanced] Heart Failure (FUSION II) Trial American College of Cardiology 56th Annual Scientific Session New Orleans, Louisiana March 25, 2007 Clyde W. Yancy, M.D. on behalf of the FUSION II Steering Committee Henry Krum, MD; Barry M. Massie, MD; Marc A Silver, MD; Lynne W. Stevenson, MD and the FUSION II Investigators

4 FUSION I: Mortality & All-cause Hospitalization (High Risk Patients- ACC/AHA Stage D HF or ‘CDHF’)
P-value for FUSION I (Nes vs Nes 0.01) time to death/all-cause hospitalization is (NS) *High risk defined as patients with 4 of 7 prespecified indicators of high risk: SCr >2 mg/dL; NYHA Class IV; 65 years; history of sustained VT; ischemic etiology; diabetes; previous outpatient nesiritide or inotropic use Log-rank Test: Standard Care vs. Nesiritide (0.005 mcg/kg/min) P=0.019 Standard Care vs. Nesiritide (0.01 mcg/kg/min) P=0.269 Standard Care vs. All Nesiritide P=0.034

5 FUSION II Study Design Nesiritide* 2x/wk Intensive Disease Management (n = 300) Placebo 2x/wk Intensive Disease Management (n = 150) n = 900 Nesiritide* 1x/wk Intensive Disease Management (n = 300) Phase IIb Double-blind Randomized Multi-center Placebo 1x/wk Intensive Disease Management (n = 150) 12 week treatment period 12 week blinded follow-up period *Dosing: 2 g/kg bolus, then 0.01 g/kg /min infusion x 4-6 hours 1° and 2° Endpoints Additional Endpoints Yancy CW et al. Am Heart J 2007; in press. Available online 3/10/2007, DOI: /j.ahj

6 Efficacy Endpoints Primary
Time to all cause death or first CV and/or renal hospitalization through Week 12 Secondary* Number of CV and/or renal hospitalizations adjusted for observation period duration Days alive and out of hospital Change in KCCQ summary score Time to CV death *from day of randomization through week 12, or week 13 for KCCQ Yancy CW et al. Am Heart J 2007; in press. Available online 3/10/2007, DOI: /j.ahj

7 Demographics Placebo Combined Groups N=306 Nesiritide N=605
Age, years, Mean  SD, 65  13 Male, (%) 72.2% 70.4% Ethnicity, (%) Caucasian African American Hispanic Asian 60.1% 23.5% 6.2% 6.5% 64.8% 20.3% 6.0% 6.4% Ischemic etiology, (%) Ischemic Idiopathic Hypertensive 63.4% 20.6% 4.2% 64% 18.7% 5.6% LVEF, Mean  SD 25%  8% Body Mass Index, Mean  SD 28.9  7.1 28.3  6.8 NYHA class, (%) III IV 46.1% 53.9% 47.1% 52.9%

8 Baseline Therapy FUSION I vs. FUSION II
530% increase 56% increase 160% increase Percent of patients treated *Includes both carvedilol and extended release metoprolol in FUSION II and any beta- blocker in FUSION I

9 Inotrope Infusions FUSION I vs FUSION II
Percent of patients treated FUSION II FUSION II Pre-randomization Inotropes Outpatient Inotropes During Study *Refers to exposure to inotropes within 2 weeks of randomization

10 FUSION II: Primary Composite Endpoint Through Week 12
Placebo Combined N=306 Nesiritide Combined N=605 *P-value All cause mortality and CV/renal hospitalization† 36.8% 36.7% 0.79 All Cause Mortality 9.6% 9.5% 0.98 CV/renal hospitalization 33.9% 32.9% 0.95 *P value: NES vs. placebo stratified by dose group †Modified ITT: all treated ITT patients

11 FUSION II: Secondary Endpoints Week 12
Placebo Combined N=306 Nesiritide Combined N=605 *P-value Number of CV/renal Hospitalizations Mean  SD 0.8  1.88 1.0  3.95 0.38 Days Alive and Out of Hospital 74.8  17.5 72.5  20.5 0.09 Change in KCCQ Mean  SD 14.2  21.1 13.0  24.1 0.52 CV Mortality 9.2% 8.1% 0.68 *P value nesiritide vs. placebo stratified by dose group

12 SAFETY Any Adverse Event
Placebo Combined Groups N=306 Nesiritide N=605 P-value All AEs 86.9% 88.7% 0.45 All drug-related AEs 27.5% 42.0% <0.01 All SAEs 56.5% 60.4% 0.29 All drug-related SAEs 8.2% 8.0% 0.90 All AEs that caused permanent study drug discontinuation 25.5% 27.0% 0.63 AE, adverse event: any untoward medical occurrence in a subject from the time of randomization through 7 days after the subject’s last dose of study drug SAE, serious adverse event: any adverse drug experience occurring at any dose level that is fatal, life-threatening, requires new or prolonged hospitalization, causes a persistent or significant disability, incapacity, congenital anomaly or birth defect, or requires intervention to prevent any of these outcomes. AE: Adverse event SAE: Serious adverse event that results in death, is life-threatening, requires inpatient hospitalization, or prolongation of existing hospitalization, or results in persistent or significant disability/incapacity.

13 SAFETY Protocol Specified Changes in Serum Creatinine*
Percent of patients with SCr increases P=0.931 P=0.458 *Outpatient Clinic Visit Values Only

14 FUSION II – Conclusions
In this patient population with advanced HF and serial infusions of nesiritide: No evidence of drug induced renal harm compared to placebo No evidence of increased mortality at pre-specified endpoints

15 FUSION II - Conclusions
In the context of optimal adherence to evidence based medical and device therapies and in concert with excellent disease management, serial infusions of nesiritide did not result in a demonstrable clinical benefit over intensive outpatient management of patients with CDHF Adherence to guideline based therapy AND meticulous follow-up should be optimized for patients with CDHF

16 Question & Answer

17 Thank You! Please make sure to hand in your evaluation and pick up a ClinicalTrialResults.org flash drive

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