Title: Epidemiology and Biostatistics Clinical Trials
1Epidemiology and BiostatisticsClinical Trials
Christine E. McLaren, Ph. D. Epidemiology
Division
2Topics
-
- Clinical trials
- Selection of subjects
- Controls
- Randomization
- Data collection
- Crossover
- Noncompliance
- Generalizability of results
- Phase I, II, III, and IV trials
- Ethical concerns
3Clinical Trial
-
- Intervention study in medicine that in
- involves humans as research subjects
- Controlled clinical trial clinical trial
- that compares treatment(s) to a control
-
- Control seen as very important. Many
- examples in literature in which
- uncontrolled studies or use of historical
- controls (results taken from literature
- or records ( yields misleading results).
4Controls
-
- Passive control
- No treatment placebo
- Active control
- Standard treatment often gold standard
- or standard of care
-
5Import Ethical Considerations
- Nuremberg Code
- Belmont Report
- Informed consent of human subject or
- VOLUNTEER
- Signed document on file
- Patient may withdraw at any time
- Confidentiality of patient guaranteed
- Good Clinical Practice GCP.
- Only use active control if current treatment
- standard exists
6Treatment Arms
-
- Each treatment modality referred to as
- arm, e.g. Control arm,
- Treatment arm
- Multi-arm Trial
- More than one control
- More difficult to analyze
- Often not controls
- e.g., comparing 3 drugs in a
- three-arm trial
7Randomization
-
- Subject assignment to an arm of a clinical
- trial by randomization.
- Patients recruited to a clinical trial after
- they report for treatment to a medical
- facility belong to what is called a
- convenience sample.
-
8Randomized Controlled Clinical Trial
-
- Gold standard of medical research
- Intervention is assigned to patient in an
- unbiased, random manner
- Randomization method may be complicated
- Simple or sophisticated strategies for
- statistical analysis
-
9Randomization
-
- Objective treatment assignmentrule out
- Conscious or unconscious bias of
- Investigators
- Steering of promising patients to
- treatment group is to be avoided.
- Also avoid steering poor prognosis
- patients
- Balances effects of unknown factors among
- treatment groups
- Want treatment groups to be comparable
- Does not solve all bias problems
-
10Randomization list
11Why Gold Standard?
-
- Timelyprospective, dealing with a current
- issue
- Prospective
- Investigator can control bias and
- variability with careful planning and
- sample size calculations
- Randomization
- Balances groups to make them
- comparable
- Balances adjuvant care over time, as
- opposed historical controls
-
12Bias vs. Confounding
-
- Bias systematic error in study results
- Confounding confusion or error in study
- results due to hidden or mixed-up factors
- e.g., Clinical trial in which males make up
- the treatment group, females make up
- control groupan extreme but
- illuminating example. Confounding cannot
- be reliably corrected by statistical
- adjustment (the information is not there).
13In a study
- Internal validity
- Are the results correct for the study itself?
- External validity
- Are the results correct for the target
- population?
- A significant p-value is not enough
- Must show sample is representative of
- target population
14Special Trials Cross-over Trial
- Usually for chronic disease (why?)
- Randomize to whether receive
- treatment first or control first
- Wash-out period for each subject
- between periods
- Dropouts a problem
-
15Phases of Clinical Trials
-
- Phase IEarly stage of clinical pharmacology
- Phase II IIILater stages of clinical
development - Phase IV Post-marketing surveillance
16Cancer Trials
Phase Goal
Endpoint
I Establish Maximum Toxicity tolerated dose
(MTD) II Establish activity Tumor Shrink
age III Establish quantitative Disease-free ef
fect survival/ overall survival
17Phase I Study of ILX23-7553 in Patients with
Advanced Malignancies
Treatment dosages and cycles Â
Treatment dosages and cycles
Wider et al.. Investigational New Drugs 212003.
18Phase I Study of ILX23-7553 in Patients with
Advanced Malignancies
Distribution of patients with grade 1 or 2
drug-related toxicities among dose levels
Other Toxicity
Â
G1
G2
G1
G2
G1
G2
Â
Wider et al.. Investigational New Drugs 212003.
19Phase II
- Establish efficacy, while monitoring safety
- Endpoint often dichotomous response
- Stop early if evidence of low activity and
- reject treatment for further study
- Back to Phase I if no activity and can
- alleviate toxicity with other drugs.
20A Phase II Trial of Gemcitabine and Docetaxel in
Patients with Chemotherapy-Naïve, Advanced
Nonsmall Cell Lung Carcinoma
Patient Characteristics (N32)
Popa et al., CANCER 95 2002
21A Phase II Trial of Gemcitabine and Docetaxel in
Patients with Chemotherapy-Naïve, Advanced
Nonsmall Cell Lung Carcinoma
Popa et al., CANCER 95 2002
22Phase III
- Comparative trials
- Larger trials
- In cancer trials, endpoints are usually
- survival, disease-free survival, or event-free
- survival
-
23Randomized Phase III Trial of Paclitaxel,
Etoposide, and Carboplatin versus Carboplatin,
Etoposide, and Vincristine in Patients with
Small-Cell Lung Cancer
Reck, et al. JNCI 95, 2003
24Randomized Phase III Trial of Paclitaxel,
Etoposide, and Carboplatin versus Carboplatin,
Etoposide, and Vincristine in Patients with
Small-Cell Lung Cancer
Results of he Cox model (univariate and
multivariate analyses) to adjust the risk
associated with therapy for various prognostic
factors
HR hazard ratioT Tumor N Node M
metastasis
Reck, et al. JNCI 95, 2003
25Internal and External Validity
-
-
- Must have absence of bias and confounding
- for internal validity
- In addition, must have representation
- of general or target population for
- external validity
26Important Documents in Clinical Trials
- Protocolthe plan for the trial
- Informed Consent Document
- Patient assignment sheet
- Data collection sheets (Case Report forms)
- Statistical analysis plan
- Final report or article
27Data Collection
- Primary outcome The measurement that will
give the most important answer for this trial - Often efficacy
- How well does the treatment work?
- Secondary outcomes
- Side effects, toxicities
- Patient satisfaction, Quality of Life
- Cost
28Data Types Used in Clinical Trials
29Safeguards for Ethical Concerns
Alphabet Soup The ABCs of Clinical Research
IRB - Institutional Review Board HIPAA -
Health Insurance Portability
and Accountability Act -
Protected Health Information FDA - Food and
Drug Administration NIH - National
Institutes of Health ICH -International
Conference on Harmonisation