#PAGE_PARAMS# #ADS_HEAD_SCRIPTS# #MICRODATA#

Ivabradine in the treatment of ischemic heart disease – results of the BEAUTIFUL study


Authors: J. Hradec
Authors place of work: III. interní klinika 1. lékařské fakulty UK a VFN, Praha
Published in the journal: Kardiol Rev Int Med 2010, 12(1): 33-37

Summary

The aim of the BEAUTIFUL clinical trail was to evaluate whether lowering of the heart rate (HR) with the specific sinoatrial node If channels inhibitor ivabradine in patients with stabilized ischemic heart disease (IHD) and left ventricular systolic dysfunction leads to a reduction in cardiovascular mortality and morbidity. The study placebo arm served for testing the hypothesis that elevated resting HR is a marker of subsequent cardiovascular mortality and morbidity. The study involved 10 970 patients with documented IHD and left ventricular ejection fraction of < 0.40, who were randomized to take either ivabradine or placebo. The primary clinical endpoint was the sum of cardiovascular deaths, hospitalisations due to myocardial infarction and hospitalizations due to cardiac failure. The patients were followed up for a median of 19 months. The mean basal HR of the patients entering the study was 71.6/ min. Patients in the placebo arm with resting HR ≥ 70/ min had, in comparison to those with resting HR < 70/ min, higher risk of cardiovascular death (by 34%; p=0.0041), hospitalizations due to cardiac failure (by 53%; p < 0.001), hospitalizations due to myocardial infarction (by 46 %; p = 0.0066) and coronary revascularization (by 38%; p = 0.037). Administration of ivabradine did not affect the incidence of the composite clinical endpoint (HR = 1.0; n.s.). Treatment with ivabradine in a pre‑defined subgroup of patients with basal resting HR ≥ 70/ min significantly reduced the number of post myocardial infarction hospitalizations (HR = 0.94; p = 0.001) and the need for coronary revascularization (HR = 0.70; p = 0.016). Post hoc analysis published a year later showed that ivabradine significantly reduced incidence of primary clinical endpoint by 24% and the number of hospitalizations for myocardial infarction by 42% in patients who suffered from limiting angina at baseline. The majority of patients included in the study (87%) took beta‑blockers. Administration of ivabradine was safe and well tolerated. HR reduction with ivabradine in patients with IHD and left ventricular systolic dysfunction did not reduce the risk of cardiovascular events. Elevated resting HR (≥ 70/ min) identifies the patients with significantly increased risk of cardiovascular events. Reduction of HR with ivabradine in these patients had a positive effect on patient prognosis. Ivabradine also reduced the incidence of cardiovascular events in patients suffering from limiting angina at baseline. The results suggested that the positive effects of ivabradine are multiplied in patient with higher HR and co‑ morbid angina.

Key words:
angina pectoris – ivabradine – BEAUTIFUL clinical trial – heart rate reduction – cardiovascular mortality – cardiovascular morbidity


Zdroje

1. Fox K, Ferrari R, Tendera M et al. BEAUTIFUL Steering Comitee. Rationale and design of a randomized, double‑blind, placebo‑ controlled trial of ivabradine in patients with stable coronary artery disease and left ventricular systolic dysfunction: the morBidity‑ mortality EvAlUaTion of the If inhibitor ivabradine in patiens with coronary disease and left ventricULar dysfunction (BEAUTIFUL) study. Am Heart J 2006; 152: 860– 866.

2. DiFrancesco D, Camm AJ. Heart rate lowering by a specific and selective If current inhibition with ivabradine: A new therapeutic perspective in cardiovascular disease. Drugs 2004; 64: 1757– 1765.

3. Kannel WB, Kannel C, Paffenberger RS jr et al. Heart rate and cardiovascular mortality: the Framingham study. Am Heart J 1987; 113: 1489– 1494.

4. Palatini P, Casiglia E, Paulleto P. Relation between physical training and ambulatory blood pressure in stage I hypertensive subjects: results of the HARVEST trial. Circulation 1994; 90: 2870– 2872.

5. Diaz A, Bourassa MG, Guertin MC et al. Long‑term prognostic value of resting heart rate in patients with suspected or proven coronary artery disease. Eur Heart J 2005; 26: 967– 974.

6. Hjalmarson A, Gilpin EA, Kjekshus J et al. Influence of heart rate on mortality after acute myocardial infarction. Am J Cardiol 1990; 65: 547– 553.

7. Kjekhus J, Gullestad L. Heart rate as a therapeutic target in heart failure. Eur Heart J 1999; (suppl H): H64– H69.

8. Hradec J. Selektivní ovlivnění srdeční frekvence – nový fenomén v kardiovaskulární farmakoterapii. Remedia 2008; 18: 114– 119.

9. Reil JC, Böhm M. The role of heart rate in the development of cardiovascular disease. Clin Res Cardiol 2007; 96: 585– 592.

10. Kjekshus JK. Importance of heart rate in determining beta‑blocker efficacy in acute and long‑term acute myocardial infarction intervention trials. Am J Cardiol 1986; 57: 43F– 49F.

11. Cucherat M. Quantitative relationship between resting heart rate reduction and magnitude of clinical benefits in post‑myocardial infarction. A meta‑regression of randomized clinical trials. Eur Heart J 2007; 28: 3012– 3019.

12. Fox K, Ford I, Steg PG et al. BEAUTIFUL Investigators. Ivabradin for patients with stable coronary artery disease and left‑ ventricular systolic dysfunction (BEAUTIFUL): a randomised, double‑blind, placebo‑ controlled trial. Lancet 2008; 372: 807– 816.

13. Fox K, Ford I, Steg PG et al. BEAUTIFUL Investigators. Heart rate as a prognostic risk factor in patients with coronary artery disease and left‑ ventricular systolic dysfunction (BEAUTIFUL): a subgroup analysis of a randomised cotrolled trial. Lancet 2008; 372: 817– 821.

14. Fox K, Ford I, Steg G et al. BEAUTIFUL Investigators. Relationship between ivabradine treatment and cardiovascular outcomes in patients with stable coronary artery disease and left ventricular systolic dysfunction with limiting angina: a subgroup analysis of the randomized, controlled BEAUTIFUL trial. Eur Heart J 2009; 30: 2337– 2345.

15. Fonarow GC, Abraham WT, Albert NM et al. Dosing of beta‑blocker therapy before, during, and after hospitalization for heart failure (from Organized Program to Initiate Lifesaving Treatment in Hospitalized Patients With Heart Failure). Am J Cardiol 2008; 102: 1524– 1529.

16. Gislason GH, Rasmussen JN, Abildstrom SZ et al. Long‑term compliance with beta‑blocker, angiotensin‑converting enzyme inhibitors, and statins after acute myocardial infarction. Eur Heart J 2006; 27: 1153– 1158.

17. Wiest FC, Bryson CL, McDonnel MB et al. Suboptimal pharmacotherapeutic management of chronic stable angina in the primary care setting. Am J Med 2004; 117.

Štítky
Paediatric cardiology Internal medicine Cardiac surgery Cardiology
Prihlásenie
Zabudnuté heslo

Zadajte e-mailovú adresu, s ktorou ste vytvárali účet. Budú Vám na ňu zasielané informácie k nastaveniu nového hesla.

Prihlásenie

Nemáte účet?  Registrujte sa

#ADS_BOTTOM_SCRIPTS#