Table 2.
True underlying relative risk (PPI vs placebo) | ||||
0.7 | 0.6 | 0.5 | ||
Event rate in placebo group | 3% | 47.1% | 74.6% | 92.6% |
4% | 60.1% | 86.6% | 97.8% | |
5% | 70.7% | 93.4% | 99.4% | |
6% | 79.1% | 96.9% | 99.9% |
This table highlights consideration for clinically important gastrointestinal (GI) bleeding. It presents combinations of relative risk reductions ranging from 30% to 50%, and baseline risks between 3% and 6% for which we will achieve 85% power. With a baseline risk of 3% and a relative risk reduction of 50%, the absolute benefit of will be a 1.5% difference. Other highlighted cells correspond to absolute risk reduction of greater than 1.5%. In summary, across the range of plausible baseline risks in the shaded boxes, 4800 patients will provide at least 85% power to detect effects of pantoprazole as large as, or greater than, this small important reduction in clinically important GI bleeding. This sample size reflects feasible enrolment in an acceptable 4-year time frame, accounting for any non-compliance or loss to follow-up, in the context of hybrid serial funding for Re-Evaluating the Inhibition of Stress Erosions.
PPI, proton pump inhibitor.