Table 2. Possible approaches for estimating HIV incidence in hypothetical placebo group or effectiveness of the control drug in an active-control trial.
| Unobserved parameter | Approach | Validity |
|---|---|---|
| HIV incidence in hypothetical placebo group | Run-in period without active treatment or Trial within a Cohort (TwiC) i.e. establish a cohort of individuals potentially interested in PrEP before trial drug becomes available.(7, 24) | Potential interest does not equate to agreement to be randomised. Number of infections usually small and estimates therefore imprecise. Potentially inaccurate if long period of follow-up and change in HIV incidence over time. |
| Recent HIV prevention studies in the same geographic region in population with similar characteristics | Potentially unreliable if HIV incidence changing rapidly | |
| Estimates from epidemiological surveillance systems(4) | Likely to under-estimate incidence as diluted by low-risk individuals testing largely for reassurance | |
| Infer incidence from tests for recent infection on baseline samples(8) | Number of recent infections usually small and estimates therefore imprecise. Incidence just prior to trial entry may not reflect incidence over whole follow-up period. |
|
| Measure STI incidence within trial, and calibrate from ecological association between incidence of HIV and other STIs | Ecological association not strong. HIV incidence possibly less stable than that of common STIs such as gonorrhoea. | |
| Effectiveness of active control drug (versus placebo) | Meta-analysis of previous trials comparing active control to placebo(1) | Hinges on “constancy” assumption i.e. that effectiveness can be validly extrapolated from meta-analysis (but studies often highly heterogeneous) |
| Measure adherence within trial and infer effectiveness from meta-regression or PK/PD models(7, 25) | Elicited adherence often inaccurate. Drug levels more reliable but expensive to collect samples. |