Table 1.
Approaches to Group Sequential Monitoring of HIV Vaccine Efficacy in Past Efficacy Trials.
| Efficacy Trial | Monitoring Type | Number and Timing of Interim Analyses | Null and Alternative Hypotheses | Alpha level | Boundary Type |
|---|---|---|---|---|---|
|
Vax004 Phase 3 1998-2003 |
Efficacy | 1; when 50% infections expected | H0: VE ≤ 30% vs. H1: VE > 30% |
0.025 | O'Brien-Fleming |
|
Vax003 Phase 3 1999-2003 |
Efficacy | 1; when 50% infections expected | H0: VE ≤ 30% vs. H1: VE > 30% |
0.025 | O'Brien-Fleming |
|
Step/HVTN 502 Phase 2b 2004-2007 |
Non-efficacy | 1; 30 PP infections1 | H0: VE ≤ 0% vs. H1: VE > 60% |
0.05 | Conditional Power < 20% |
| Efficacy | 1; 30 PP infections | H0: VE ≤ 0% vs. H1: VE > 0% |
0.05 | Custom | |
|
Phambili/HVTN 503 Phase 2b 2005-2007 |
Non-efficacy | 1; 60 PP infections | H0: VE ≤ 50% vs. H1: VE > 50% |
N/A | Conditional Power < 20% |
| Efficacy | 1; 60 PP infections | H0: VE ≤ 0% vs. H1: VE > 0% |
0.05 | Custom | |
|
RV144 Phase 2b 2004-2009 |
Harm | Monthly | H0: VE ≥ 0% vs. H1: VE < 0% |
0.05 | Pocock-type2 |
| Non-efficacy | 8; every 6 to 12 months | H0: VE ≤ 0% vs. H1: VE > 50% |
N/A | Conditional Power < 10% | |
| Efficacy | 1; 2/3 of follow-up information | H0: VE ≤ 30% vs. H1: VE > 30% |
0.025 | O'Brien-Fleming |
1
Per-protocol (PP) infections are those diagnosed after the Week 12 visit in volunteers HIV negative at baseline and who received the first two doses of either vaccine or placebo, excluding those who were either diagnosed with HIV infection before or at the Week 12 visit or who violated the protocol on the basis of pre-defined criteria (Buchbinder et al., 2008). The interim analysis was triggered by the 30th PP infection in the primary analysis group of subjects with Adenovirus-5 neutralization titers ≤ 200.
2
Continuous stopping boundary of Betensky (1998).