Table 1.
Summary of phase III ODYSSEY trials with Alirocumab
| Name of trial | Ref. Allocation and blinding | No. of patients | Inclusion criteria | Study arms (with dosing) | Primary end point | Results |
| LONG TERM (NCT01507831) | Seidah et al[7]; Randomized double blinded trial | 2341 | Either 1 or 2 below and who aren’t adequately controlled with their LLT: (1) Patients with heFH with or without CHD or CHD risk equivalents OR (2) Patients with HCL with CHD or CHD risk equivalents | Alirocumab (SC) (n = 1553) vs Placebo (SC) (n = 788) both with background LLT | Percentage change in calculated LDL cholesterol level from baseline to week 24 | -61.0% change with Alirocumab vs +0.8% change with placebo (CI: -64.3 to -59.4; P < 0.001) |
| FH I (NCT01623115) | Kastelein et al[66]; Randomized double blinded | 486 | Patients with heterozygous familial hypercholesterolemia who are not adequately controlled with their lipid-modifying therapy | Alirocumab (SC) vs Placebo (SC) both with background LLT | Percent change in calculated LDL-C at week 24 | -48.8% for Alirocumab compared with 9.1% for placebo (P < 0.0001) |
| FH II (NCT01709500) | Kastelein et al[66]; Randomized double blinded | 249 | Patients with heFH who are not adequately controlled with their LLT | Alirocumab (SC) vs Placebo (SC) both with background LLT | Percent change in LDL-C to week 24 | -48.7% for Alirocumab compared with 2.8% for placebo (P < 0.0001) |
| HIGH FH (NCT01617655) | Kastelein et al[67]; Randomized double blinded | 107 | Patients with heterozygous familial hypercholesterolemia who are not adequately controlled with their lipid-modifying therapy with LDL > 160 | Alirocumab (SC) (n = 72) vs Placebo (SC) (n = 35) both with background LLT | Percent change in calculated LDL-C at week 24 | Percent decrease from baseline was 45.7% vs 6.6%, difference 39.1, P < 0.0001 Absolute difference in values of LDL-C at 24 wk 107 mg/dL vs 182 mg/dL |
| COMBO I (NCT01644175) | Colhoun et al[60]; Randomized double blinded | 316 | Patients with hypercholesterolemia and estbl CHD or CHD risk equivalents; not controlled with a maximally tolerated LLT, both at stable dose for at least 4 to 6 wk prior to screening | Alirocumab (SC) (n = 205) vs Placebo (SC) (n = 106) | Percent change in calculated LDL-C at week 24 | -48.2% with Alirocumab (CI: -52.0% to -44.4%) and -2.3% with placebo (CI: -7.6% to 3.1%) for Alirocumab and placebo, respectively, an estimated mean difference of -45.9% (CI: -52.5% to -39.3%) (P < 0.0001) |
| COMBO II (NCT01644188) | Moriarty et al[65]; Randomized double blind | 720 | Patients with hypercholesterolemia and established CHD or CHD risk equivalents who are not adequately controlled with a maximally tolerated daily dose of statin at stable dose for at least 4 wk prior to the screening visit | Alirocumab (SC) + placebo (for ezetimibe) orally + background statin therapy (n = 467) vs Placebo (SC) + ezetimibe orally + Background statin therapy (n = 240) | Percent change in calculated LDL-C at week 24 | Reductions in LDL-C from baseline were 50.6% ± 1.4% for Alirocumab vs 20.7% ± 1.9% for ezetimibe (difference 29.8% ± 2.3%; P < 0.0001) |
| OPTIONS I (NCT01730053) | Robinson et al[63]; Randomized double-blinded | 355 | Patients with prior CV disease + LDL-C ≥ 70 mg/dL, or CV risk factors + LDL-C ≥ 100 mg/dL | Alirocumab with atorvastatin 20 mg vs Ezetimibe with atorvastatin 20 mg vs Atorvastatin 40 mg | Percent change in calculated LDL-C to week 24 | Percent reduction from baseline 44.1% (Alirocumab) vs 20.5% (ezetimibe) vs 5.0% (atorvastatin 40); P < 0.0001 |
| Alirocumab with atorvastatin 40 mg vs ezetimibe with atorvastatin 40 mg vs atorvastatin 80 mg vs rosuvastatin 20 mg | Percent reduction from baseline 54% (Alirocumab) vs 22.6% (Ezetimibe) vs 4.8% (Atorvastatin 80) vs 21.4% (rosuvastatin 40); P < 0.0001 | |||||
| OPTIONS II | Robinson et al[63]; Randomized double-blinded | 305 | Patients with prior CV disease + LDL-C ≥ 70 mg/dL, or CV risk factors + LDL-C ≥ 100 mg/dL | Alirocumab with rosuvastatin 10 mg vs ezetimibe with rosuvastatin 10 vs rosuvastatin 20 | Percent change in calculated LDL-C to wk 24 | Percent reduction from baseline 50.6% (Alirocumab) vs 14.4% (ezetimibe) vs 16.3% (rosuvastatin 20); P < 0.0001 |
| Alirocumab with rosuvastatin 20 mg vs ezetimibe with rosuvastatin 20 vs Rosuvastatin 40 | Percent reduction from baseline 36.3% (Alirocumab) vs 11.0% (Ezetimibe) vs 20.3% (rosuvastatin 40); P < 0.0001 | |||||
| ALTERNATIVE (NCT01709513) | Moriarty et al[65]; Randomized double-blinded | 314 | Primary heFH with moderate, high or very high CV risk and history of statin intolerance | Alirocumab + oral placebo vs ezetimibe (10 mg/d) + sc placebo vs atorvastatin (20 mg/d) + sc placebo | Percent change in calculated LDL-C to week 24 in intention to treat group | Percent reduction from baseline 45% (Alirocumab) vs 14.6% (Ezetimibe) with a mean difference of -30.4%; P < 0.0001 |
| CHOICE I (NCT01926782) | Stroes et al[78]; Randomized, double-blinded | 803 | Patients not having adequate control of their hypercholesterolemia based on their individual level of CVD risk | Alirocumab at q4 week regimen vs Placebo | Percent change in LDL from baseline to week 24 for Alirocumab q4w vs placebo in patients with hypercholesterolemia at moderate, high, or very high CVD risk with concomitant statin therapy (n = 547) Percent change in LDL from baseline to week 24 for Alirocumab q4w vs placebo in patients with hypercholesterolemia not on concomitant statin therapy (n = 256) | LDL was reduced by 58.7% with Alirocumab in patients on maximally tolerated statins (P < 0.001) |
| CHOICE II (NCT02023879) | Stroes et al[78]; Randomized, double-blinded | 231 | Patients with primary hypercholesterolemia (heFH or non-FH) not adequately controlled with their non statin lipid modifying therapy or diet and statin intolerance | Alirocumab (SC) vs placebo (SC) | The percent change in LDL-C from baseline to week 24 | Alirocumab reduced LDL-C by 56.4% (P < 0.0001) vs placebo |
| LONG TERM (NCT01507831) | Robinson et al[62]; Randomized, double-blinded | 2341 | Either A or B below and who are not adequately controlled with their LLT: (1) Patients with heFH with or without established CHD or CHD risk equivalents OR (2) Patients with hypercholesterolemia together with established CHD or CHD risk equivalents | Alirocumab (SC) 150 mg every 2 wk vs placebo (SC) every 2 wk | Percentage change in calculated LDL cholesterol level from baseline to week 24, analyzed with the use of an intention-to-treat approach | 150 mg Alirocumab every 2 wk had a 62% reduction in LDL as opposed to a 1% increase in LDL with placebo at 24 wk |
SC: Subcutaneous; LLT: Lipid lowering therapy; heFH: Heterozygous familial hypercholesterolemia; CHD: Coronary heart disease; HCL: Hypercholesterolemia; MACE: Major adverse cardiovascular events; MI: Myocardial infarction; UA: Unstable angina; HR: Hazards ratio; CI: Confidence interval.