Порівняння методів
Переглядайте обрані методи поруч; рядки з відмінностями підсвічено.
| Клінічне дослідження Фази I з урахуванням ризику× | Клінічне дослідження Фази I× | |
|---|---|---|
| Галузь | Епідеміологія | Епідеміологія |
| Родина | Process / pipeline | Process / pipeline |
| Рік появи≠ | 1990s–2000s | 1960s (formal regulatory framework established ~1963–1970s) |
| Автор методу≠ | Evolved from the Continual Reassessment Method (O'Quigley et al., 1990) extended with patient-level risk covariates | Regulatory and clinical pharmacology community; formalized in U.S. FDA IND regulations (1963) and ICH guidelines |
| Тип≠ | Interventional clinical trial design | Interventional clinical study design |
| Основоположне джерело≠ | Iasonos, A., Wilton, A. S., & Gonen, M. (2008). A review of stochastic dose-finding methods. Statistics in Medicine, 27(25), 5031–5046. link ↗ | Storer, B. E. (1989). Design and analysis of phase I clinical trials. Biometrics, 45(3), 925–937. DOI ↗ |
| Інші назви | risk-stratified Phase I trial, risk-adaptive dose-escalation study, covariate-adjusted Phase I study, risk-based dose-finding trial | Phase 1 trial, first-in-human study, FIH study, dose-escalation study |
| Пов'язані≠ | 5 | 6 |
| Підсумок≠ | A risk-adjusted Phase I clinical trial is a first-in-human or dose-finding study that explicitly incorporates patient-level risk covariates — such as organ function, prior therapy, or genetic markers — into the dose-escalation model. Rather than treating all enrolled participants as homogeneous, the design accounts for individual differences in tolerance, allowing the recommended dose to vary by risk stratum. This approach is especially common in oncology, where patients with impaired renal function or heavily pre-treated disease may tolerate lower doses than the broader population. | A Phase I clinical trial is the first stage of human testing for a new drug, biologic, or intervention. Its primary objective is to evaluate safety, tolerability, pharmacokinetics (PK), and pharmacodynamics (PD) rather than therapeutic efficacy. Small cohorts of participants — typically healthy volunteers or patients with advanced disease — receive sequentially increasing doses to identify the maximum tolerated dose (MTD) and the dose-limiting toxicities (DLTs) that define the boundary for subsequent trials. |
| ScholarGateНабір даних ↗ |
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