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Impact of ISDN-hydralazine on mortality and morbidity of African-American patients with Heart Failure A-Heft Trial Presented at American Heart Association.

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Presentation on theme: "Impact of ISDN-hydralazine on mortality and morbidity of African-American patients with Heart Failure A-Heft Trial Presented at American Heart Association."— Presentation transcript:

1 Impact of ISDN-hydralazine on mortality and morbidity of African-American patients with Heart Failure A-Heft Trial Presented at American Heart Association Scientific Sessions 2004 Presented by Dr. A.L. Taylor

2 www. Clinical trial results.org Isosorbide dinitrate (ISDN) plus hydralazine Tablet containing 20 mg ISDN and 37.5 mg hydralazine (BiDil ®, NitroMed) 3X daily. Dosage could be doubled by enrolling physician. n=518 44.2% female 44.8% diabetic Isosorbide dinitrate (ISDN) plus hydralazine Tablet containing 20 mg ISDN and 37.5 mg hydralazine (BiDil ®, NitroMed) 3X daily. Dosage could be doubled by enrolling physician. n=518 44.2% female 44.8% diabetic Primary Endpoint:  Weighted composite of all-cause death, first hospitalization for heart failure, and change in quality of life at a mean follow-up of 10 months Primary Endpoint:  Weighted composite of all-cause death, first hospitalization for heart failure, and change in quality of life at a mean follow-up of 10 months A-Heft Trial Presented at AHA 2004 Placebo  n=532 36.1% female 37.0% diabetic Placebo  n=532 36.1% female 37.0% diabetic 1,050 African-American patients with advanced heart failure New York Heart Association (NYHA) class 3-4 for > 3 months LV function < 35% (< 40% if LV dilated per echo) 90% receiving diuretics, 69% ACE-inhibitor, 17% angiotensin receptor blocker, 74% beta-blocker 1,050 African-American patients with advanced heart failure New York Heart Association (NYHA) class 3-4 for > 3 months LV function < 35% (< 40% if LV dilated per echo) 90% receiving diuretics, 69% ACE-inhibitor, 17% angiotensin receptor blocker, 74% beta-blocker

3 www. Clinical trial results.org A-Heft Trial: Primary Endpoint Presented at AHA 2004 Primary Composite Score p = 0.01 The primary weighted composite of all-cause mortality, first hospitalization for HF and change in quality-of-life was significantly lower in the ISDN- hydralazine group than in the placebo group at a mean follow- up of 10 months

4 www. Clinical trial results.org A-Heft Trial: Primary Endpoint Presented at AHA 2004 All individual components of the primary composite endpoint were significantly improved with ISDN-hydralazine therapy, namely death, first hospitalization for heart failure, and change in the quality-of-life score (a larger negative score indicates a better quality of life).

5 www. Clinical trial results.org A-Heft Trial: Mortality Presented at AHA 2004 Mortality p = 0.01 A significant reduction in mortality in the ISDN- hydralazine group began to emerge at 6 months and continued to diverge through follow-up, prompting an early end to the trial

6 www. Clinical trial results.org A-Heft Trial: Adverse effects Presented at AHA 2004 Adverse events of headache and dizziness were significantly higher in the ISDN- hydralazine group, while the more serious adverse events of exacerbation of CHF were significantly lower in the ISDN-hydralazine group than in the placebo group p=<0.001 p=0.04 p=0.005

7 www. Clinical trial results.org A-Heft Trial: Summary Among African-American patients with advanced heart failure, the primary weighted composite of all-cause death, first hospitalization for heart failure, and change in quality of life was significantly lower in the ISDN-hydralazine group than in the placebo group at a mean follow-up of 10 months All individual components of the primary endpoint were significantly improved with ISDN-hydralazine therapy compared to placebo The trial was stopped after 1,050 of the planned 1,100 patients had been enrolled due to the significantly lower incidence of mortality in the ISDN- hydralazine group This was the first study of this therapy to be conducted solely in African- American patients, a population disproportionately affected by heart failure Future studies are warranted for the identification of genetic markers more specific to drug efficacy to replace the broader category of race as a treatment criteria Among African-American patients with advanced heart failure, the primary weighted composite of all-cause death, first hospitalization for heart failure, and change in quality of life was significantly lower in the ISDN-hydralazine group than in the placebo group at a mean follow-up of 10 months All individual components of the primary endpoint were significantly improved with ISDN-hydralazine therapy compared to placebo The trial was stopped after 1,050 of the planned 1,100 patients had been enrolled due to the significantly lower incidence of mortality in the ISDN- hydralazine group This was the first study of this therapy to be conducted solely in African- American patients, a population disproportionately affected by heart failure Future studies are warranted for the identification of genetic markers more specific to drug efficacy to replace the broader category of race as a treatment criteria


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