Phases of trials
From TrialTree Wiki
Phases of trials
Clinical trials are commonly conducted in phases, each with a distinct purpose, scope, and methodology. Understanding these phases helps clarify where a trial fits within the larger research pipeline, from early safety assessments to widespread implementation.
Phase 0: Exploratory (Microdosing) Trials
Also known as “first-in-human” studies. Phase 0 trials are optional early-phase studies involving very small doses of a drug (sub-therapeutic) given to a small number of participants, usually fewer than 15.
Purpose:
- Assess pharmacokinetics (PK) and pharmacodynamics (PD)
- Inform go/no-go decisions before Phase I
Key Features:
- Non-therapeutic
- No clinical benefit expected
- Helps identify promising candidates for further testing
Phase I: Safety and Dose-Finding
Phase I trials are the first stage of testing in humans, usually involving 20–100 healthy volunteers or patients (for high-risk drugs like cancer treatments).
Purpose:
- Assess safety and tolerability
- Determine safe dosage range
- Identify side effects
Design Elements:
- Open-label or dose-escalation design (e.g., 3+3 or Bayesian adaptive models)
- Focus on maximum tolerated dose (MTD)
Phase II: Efficacy and Side Effects
Phase II trials further evaluate the efficacy of an intervention and continue to assess its safety, typically in 100–300 participants with the target condition.
Purpose:
- Preliminary evidence of clinical effect
- Continued safety assessment
- Optimal dosing
Design Elements:
- Often randomized and controlled
- May use surrogate outcomes
- Can be split into Phase IIa (dose exploration) and Phase IIb (efficacy confirmation)
Phase III: Confirmatory Efficacy Trials
Phase III trials are large-scale RCTs involving hundreds to thousands of participants across multiple sites. These trials provide the definitive evidence needed for regulatory approval.
Purpose:
- Confirm therapeutic benefit
- Compare to standard of care
- Identify less common side effects
- Establish risk-benefit profile
Design Elements:
- Often multicenter, randomized, double-blind
- Pre-specified primary hypothesis
- May include interim analyses and data safety monitoring boards (DSMBs)
Phase IV: Post-Marketing Surveillance
Phase IV trials are conducted after regulatory approval to monitor the long-term effectiveness and safety of a treatment in real-world settings.
Purpose:
- Detect rare or long-term adverse effects
- Study effectiveness in diverse populations
- Assess cost-effectiveness and quality of life
Design Elements:
- Observational or pragmatic RCTs
- May be mandated by regulators
- Often use registry data or health records
Summary Table
| Phase | Primary Goal | Participants | Design Focus |
|---|---|---|---|
| Phase 0 | PK/PD, feasibility | <15 | Microdosing, no therapeutic intent |
| Phase I | Safety, dose range | 20–100 | Dose-escalation, tolerability |
| Phase II | Preliminary efficacy | 100–300 | Controlled, surrogate outcomes |
| Phase III | Confirm efficacy, safety | 300–3000+ | Hypothesis-driven, regulatory-focused |
| Phase IV | Long-term effects, safety | Thousands | Real-world, post-approval |
Integration with Trial Design
The phase of a trial often influences the:
- Type of hypothesis tested (Hypothesis)
- Level of monitoring and oversight
- Statistical methods used
- Ethical considerations (e.g., acceptable risk-benefit ratio)
Conclusion
Understanding the phases of clinical trials is essential for designing, conducting, and interpreting research appropriately. Each phase serves a distinct purpose in the journey from bench to bedside, ensuring that interventions are safe, effective, and beneficial to patients.
Bibliography
- U.S. Food and Drug Administration (FDA). The Drug Development Process: Step 3 – Clinical Research. Available from: https://www.fda.gov
- Chow S-C, Liu JP. Design and Analysis of Clinical Trials: Concepts and Methodologies. 3rd ed. Wiley; 2013. Chapter 2: Clinical trial phases and regulatory framework.
- van Norman GA. Drugs, devices, and the FDA: Part 1. An overview of approval processes for drugs. JACC: Basic to Translational Science. 2016;1(3):170–179.
- Thiers FA, Sinskey AJ, Berndt ER. Trends in the globalization of clinical trials. Nature Reviews Drug Discovery. 2008;7(1):13–14. Discusses operational characteristics of different trial phases.
- ICH Harmonised Guideline. General Considerations for Clinical Studies E8(R1). International Council for Harmonisation; 2019. Describes objectives and design considerations by phase.
Adapted for educational use. Please cite relevant trial methodology sources when using this material in research or teaching.