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. 2023 Aug 16;24(16):12866. doi: 10.3390/ijms241612866

Table 7.

Clinical studies of HCN channel blocker.

Drug Study Population Treatment Primary and Secondary Endpoints Main Findings and Conclusions
Ivabradine
(BEAUTIFUL trial)
[117]
  • Patients with CAD and LV systolic dysfunction

  • LVEF < 40%

  • Resting HR ≥ 60 bpm (N = 10,917)

Ivabradine 5–7.5 mg BID or placebo Primary:
  • A composite of CV death, admission to hospital for acute MI, and admission to hospital for new-onset or worsening HF.

  • Ivabradine reduced HR of 6 and 5 bpm at 12 and 24 months, respectively.

  • Reduction in HR could be used to reduce the incidence of CAD outcomes in patients who have HR ≥ 70 bpm.

Ivabradine
(Echo substudy of BEAUTIFUL)
[118]
Subgroup analysis of the BEAUTIFUL trial
(N = 590)
Primary:
  • Change in LV end-systolic volume index (LVESVI).

Secondary:
  • Changes in LVEF, LVEDVI, and NT-proBNP.

  • Ivabradine was associated with a decrease in LVESVI and an increase in LVEF.

  • Ivabradine may reverse detrimental LV remodeling.

Ivabradine
(SHIFT trial)
[119]
  • Patients with symptomatic HF and LVEF ≤ 35%

  • HR ≥ 70 bpm (N = 6558)

Ivabradine titrated to a maximum of 7.5 mg BID or placebo Primary:
  • A composite of CV death or hospital admission for worsening HF.

  • Ivabradine reduced major risks associated with HF.

  • Ivabradine reduced the risk of the primary endpoint.

  • No difference in reducing CV and all-cause deaths.

Ivabradine
(Echo substudy of SHIFT)
[120]
Subgroup analysis of the SHIFT trial
(N = 411)
Primary:
  • Change in LVESVI from baseline to 8 months.

Secondary:
  • Changes in LVEF, LVEDVI, LVESV, and LVEDV

  • Ivabradine reduced LVESVI.

  • Ivabradine reverses cardiac remodeling in HF patients with LV systolic dysfunction.