مقایسهٔ روشها
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| طراحی افزایش دوز (روش ارزیابی مداوم)× | استنتاج بیزی× | طراحی کارآزماییهای ترتیبی / گروهی ترتیبی× | |
|---|---|---|---|
| حوزه≠ | طراحی آزمایش | آمار | طراحی آزمایش |
| خانواده≠ | Process / pipeline | Bayesian methods | Hypothesis test |
| سال پیدایش≠ | 1990 | 1763 | 1979 |
| پدیدآور≠ | John O'Quigley, Margaret Pepe & Lloyd Fisher | Thomas Bayes; Pierre-Simon Laplace | O'Brien & Fleming; Pocock; Lan & DeMets |
| نوع≠ | Adaptive Bayesian dose-finding design | Probabilistic inference paradigm | Adaptive stopping trial design |
| منبع بنیادین≠ | O'Quigley, J., Pepe, M., & Fisher, L. (1990). Continual reassessment method: a practical design for phase 1 clinical trials in cancer. Biometrics, 46(1), 33–48. DOI ↗ | Bayes, T. (1763). An essay towards solving a problem in the doctrine of chances. Philosophical Transactions of the Royal Society of London, 53, 370–418. link ↗ | O'Brien, P.C. & Fleming, T.R. (1979). A Multiple Testing Procedure for Clinical Trials. Biometrics, 35(3), 549–556. DOI ↗ |
| نامهای دیگر≠ | Continual Reassessment Method, CRM Design, Phase I Dose-Finding Design, Doz Artırma Tasarımı | Bayes inference, Bayesian statistics, Bayesian updating, posterior inference | group sequential design, adaptive stopping design, Ardışık Deneme Tasarımı (Sequential / Group Sequential) |
| مرتبط≠ | 2 | 3 | 3 |
| خلاصه≠ | Dose-Escalation Design, formalized as the Continual Reassessment Method (CRM), is a Bayesian adaptive algorithm for identifying the Maximum Tolerated Dose (MTD) in Phase I clinical trials. Introduced by John O'Quigley, Margaret Pepe, and Lloyd Fisher in 1990, CRM treats dose-toxicity response as a parametric curve, updates a prior probability model after each patient's outcome, and assigns subsequent patients to the dose currently estimated closest to a pre-specified target toxicity probability. | Bayesian inference is a statistical paradigm in which probability represents degrees of belief rather than long-run frequencies. It encodes prior knowledge about parameters in a prior distribution, combines that prior with the likelihood of observed data via Bayes' theorem, and produces a posterior distribution that quantifies updated uncertainty. The foundational theorem was published posthumously by Thomas Bayes in 1763 and subsequently systematized by Pierre-Simon Laplace in his 1812 Théorie analytique des probabilités. | 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. |
| ScholarGateمجموعهداده ↗ |
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