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| Adaptivt klinisk forsøgsdesign× | Klausul / Ikke-underlegenhedsprøve× | Sekventielt / Gruppesekventielt forsøgsdesign× | |
|---|---|---|---|
| Fagområde | Forsøgsdesign | Forsøgsdesign | Forsøgsdesign |
| Familie | Hypothesis test | Hypothesis test | Hypothesis test |
| Oprindelsesår≠ | 1994 | 1987 | 1979 |
| Ophavsperson≠ | Bauer & Köhne | Schuirmann, D.J. / EMA regulatory framework | O'Brien & Fleming; Pocock; Lan & DeMets |
| Type≠ | Adaptive hypothesis test with interim analyses | Parametric equivalence / non-inferiority test | Adaptive stopping trial design |
| Oprindelig kilde≠ | Bauer, P. & Köhne, K. (1994). Evaluation of Experiments with Adaptive Interim Analyses. Biometrics, 50(4), 1029–1041. DOI ↗ | Schuirmann, D.J. (1987). A Comparison of the Two One-Sided Tests Procedure and the Power Approach. Journal of Pharmacokinetics and Biopharmaceutics, 15(6), 657–680. link ↗ | O'Brien, P.C. & Fleming, T.R. (1979). A Multiple Testing Procedure for Clinical Trials. Biometrics, 35(3), 549–556. DOI ↗ |
| Aliasser≠ | adaptive design, group sequential design, sample size re-estimation, platform trial | non-inferiority trial, bioequivalence study, active-control trial, Denklik ve Üstünlük Olmayan Çalışma (Equivalence / Non-Inferiority) | group sequential design, adaptive stopping design, Ardışık Deneme Tasarımı (Sequential / Group Sequential) |
| Relaterede≠ | 3 | 6 | 3 |
| Resumé≠ | Adaptive clinical trial design is a flexible experimental framework, formalised by Bauer and Köhne in 1994, in which pre-specified rules allow the trial to be modified mid-course — adjusting sample size, treatment arms, or randomisation ratios — based on accumulating interim data while rigorously controlling the Type I error rate. | An equivalence or non-inferiority trial is a clinical study design that tests whether a new intervention is clinically equivalent to, or no worse than, an established standard by a pre-specified margin. Codified in Schuirmann's 1987 Two One-Sided Tests (TOST) framework and embedded in EMA and FDA regulatory guidance, this design is the regulatory standard for generic drug approval and medical device testing. | Sequential and group sequential trial designs allow a study to be stopped early — or continued — based on interim analyses conducted as data accumulate. The core framework was formalised by O'Brien and Fleming in 1979 and extended by Lan and DeMets's alpha-spending approach, and it controls the overall Type I error rate across all planned looks by pre-specifying both efficacy and futility boundaries before enrolment begins. |
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