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Anti-TNF- a Strategies in CHF: Data from Randomized, Controlled Clinical Trials Arthritis Advisory Committee March 4, 2003. Ellis F. Unger, M.D. Office of Therapeutics Research and Review (OTRR) Center for Biologics Evaluation and Research (CBER) U.S. Food and Drug Administration (US FDA).
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Anti-TNF-a Strategies in CHF: Data from Randomized, Controlled Clinical TrialsArthritis Advisory CommitteeMarch 4, 2003 Ellis F. Unger, M.D. Office of Therapeutics Research and Review (OTRR) Center for Biologics Evaluation and Research (CBER) U.S. Food and Drug Administration (US FDA)
Why the Interest in Anti-TNF-a Strategies in CHF? • Clinical observations: • elevated TNF-a levels in patients with CHF, especially cardiac cachexia • Preclinical data showing: • TNF-a-induced LV dysfunction • deleterious effects on LV remodeling
Anti-TNF-a Hypotheses in CHF: • TNF-a contributes to the morbidity of CHF • Anti-TNF-a therapies would have salutary effects in patients with CHF
Randomized Controlled Trials of TNF-a Blockers in CHF: • Etanercept • 2 Randomized Controlled Studies: • “RENAISSANCE” • “RECOVER” • Infliximab • 1 Randomized Controlled Study: • “ATTACH”
Studies of Etanercept in CHF: “RENAISSANCE” “RECOVER”
Etanercept in CHF: • “RENAISSANCE” - conducted by Immunex in North America; ~900 subjects • “RECOVER” - conducted by Wyeth in Europe, Israel, Australia, New Zealand; ~1100 subjects • Both: • phase 2/3 • randomized • double-blind • placebo-controlled • multicenter
Inclusion Criteria: • CHF on ischemic or non-ischemic basis • ejection fraction < 30% • symptoms of CHF X 3 months • NYHA Functional Class 2, 3, or 4 • receiving diuretic and ACE inhibitor
Randomization - Dosing Regimens: Randomization 1:1:1 - blocked by study site, NYHA FC, and b-blocker use RENAISSANCERECOVER Enbrel1X per week 25 mg SC 2X per week *2X per week * 3X per week Placebo 2X or 3X per week Treatment duration > 24 weeks * regimen licensed for RA
RENAISSANCE & RECOVER: Endpoints • Primary endpoints: • “Clinical Composite Score” at 24 weeks • (Score º improved, worse, unchanged) • Combined endpoint across both studies: • Mortality or CHF hospitalization • (BIW + TIW) vs. placebo
Clinical Composite Score º “Worse” if: · subject died · was hospitalized for CHF · worsened NYHA FC · “Global Assessment” (judged by subject) moderately or markedly worse
Clinical Composite Score º “Improved” if: · the Clinical Composite Score was not worse AND · NYHA FC is improved OR · “Global Assessment” moderately or markedly improved
Clinical Composite Score º “Unchanged” if: Clinical Composite Score neither better nor worse.
March 2001: Studies Stopped for Futility At a planned interim review, the DSMB recommended that both RENAISSANCE and RECOVER be halted because the pre-specified results indicating futility had been observed. Median follow-up: RENAISSANCE - 12.7 months RECOVER - 5.7 months
Patient Demographic & Baseline Disease Characteristics: RENAISSANCE Age: 62.3 years (mean) Gender: 78% male Race: 84% Caucasian; 11% African Ancestry CHF duration: 5.6 years (mean) Ejection Fraction: 22.3% (mean) NYHA FC: FC II – 24% FC IIIa – 47% FC IIIb – 25% FC IV – 5%
Imbalances in Patient Demographics & Disease Characteristics: RENAISSANCE • Treatment groups well balanced with respect to demographic and baseline characteristics • 4 notable exceptions. For the placebo group, on average, baseline: • BP was higher • 6-minute walk was longer • antiarrhythmic use was less frequent • atrial fib/flutter was less frequent • These imbalances were small, but all would be associated with a more favorable prognosis in the placebo group.
Demographic & Baseline Characteristics: RECOVER Age: 64.6 years Gender: 78% male Caucasian: 99% CHF duration: 4.6 years Ejection Fraction: 24.2% NYHA FC: FC II – 27% FC IIIa – 45% FC IIIb – 25% FC IV – 3% * Good balance across treatment groups
1° Endpoint: All-Cause Mortality and CHF Hospitalizations Across Both Studies (Enbrel BIW + TIW vs. placebo) log-rank p-value = 0.15 Placebo (n=682) Enbrel BIW +TIW (n=991)
All-Cause Mortality: RENAISSANCE 1/4 remain at risk 14.2% 17.9% 19.8% Placebo (n=309) Enbrel BIW (n=308) Enbrel TIW (n=308)
All-Cause Mortality: RECOVER 5.9% 7.2% 8.8% 1/4 remain at risk Placebo (n=373) Enbrel QW (n=375) Enbrel BIW (n=375)
Comparison of Subject Populations: RENAISSANCE vs. RECOVER
RENAISSANCE: Mortality by Treatment and NYHA Functional Class FC II FC IIIa FC IIIb Placebo (n=77) Enbrel BIW (n=75) Enbrel TIW (n=75) Placebo (n=142) Enbrel BIW (n=141) Enbrel TIW (n=141) Placebo (n=76) Enbrel BIW (n=76) Enbrel TIW (n=77)
Summary: Etanercept in CHF (1) • No evidence that Etanercept is beneficial in CHF • The data suggest harm, though the results are not conclusive. • The key finding of concern was a trend towards higher mortality in Etanercept-treated subjects in RENAISSANCE; this was heightened by the apparent dose-response relation. • The results of RECOVER do not substantiate the findings of Renaissance with respect to Etanercept-induced mortality in CHF. • The greatest concern is for an Enbrel dose higher than that currently licensed for RA in the US.
Summary: Etanercept in CHF (2) • The data do not suggest a specific mechanism of action leading to Etanercept-related adverse outcomes in the CHF patient population. • Exploratory analyses failed to identify specific factors associated with increased risk of adverse events. In particular, patients in Renaissance with milder CHF (NYHA FC II) did not appear to be at a lower risk of adverse outcomes. • Inlabeling, thereisnobasistoprovide: • a measure of reassurance for patients with mild forms of CHF; • a listing of factors that appear to predispose to worsening CHF
Study of Infliximab in CHF: “ATTACH”
ATTACH: • phase 2 pilot trial • randomized • double-blind • placebo-controlled • multicenter (32 centers in USA)
Randomization - Dosing Regimens: • 150 subjects randomized 1:1:1 to: • infliximab 5 mg/kg at 0, 2 and 6 weeks • infliximab 10 mg/kg at 0, 2 and 6 weeks • placebo at 0, 2 and 6 weeks
ATTACH: Inclusion Criteria • symptoms of CHF X 3 months • NYHA functional class 3, or 4 • LV ejection fraction £ 35% • receiving diuretic and ACE inhibitor
ATTACH: Primary Endpoint “Clinical Status” at 14 weeks: improved, worse, or unchanged
Infliximab: Dear Healthcare Professional letter issued October 18, 2001
Summary: Infliximab in CHF • No evidence that Infliximab is beneficial in patients with CHF. • Although the numbers of subjects treated are small, there is a strong trend suggesting increased mortality in CHF patients treated with Infliximab. • The data do not show an increase in mortality with the 5 mg/kg dose; however, adverse event data suggest that the 5 mg/kg dose is deleterious. • The mechanism underlying this apparent effect is unclear.
Post-Marketing Reports of CHF: • 51 cases reported as of February, 2002: • 30 received Etanercept; 21 received Infliximab • 42 reports of new onset CHF - - half with no identifiable risk factors • 9 reports of CHF exacerbation • Median age = 64 yrs (range 19 to 87 years) • Median time to onset 3.5 months (range: 24 hours to 24 months) • 20% were < 50 years old
CHF Cases in Patients Under 50 Years Old • 10 cases: • 6 received infliximab & 4 received etanercept • Median ejection fraction = 20% (range 10 to 45%, n=9) • 3 with underlying risk factors for CHF • After discontinuation of TNF antagonists and HF treatment: • 3 reported complete resolution of CHF • 6 reported improvement • 1 reported death
Summary: TNF Blockers and CHF: • Significant overlap between CHF and RA in the general population, to a lesser extent CHF & Crohn’s Disease • Data from RCT’s in the CHF population raise concerns about the safety of Infliximab and Etanercept. • Post-marketing data raise concern regarding new-onset CHF. • CBER plans comprehensive analyses of the RCT databases of all 3 TNF-blockers. • Specific language for labeling is under discussion.