Clinical Trial Design

Question 1

Why do a clinical trial?

Answer 1

Provides evidence, medical practice is evidence based but you you need to be able to critically evaluate evidence for what you do.

Use SIGN guidelines or Grampian Joint Formulary

Question 2

Preclinical development

Answer 2

• Animal pharmacology (dose, adverse effects)
• Animal toxicology (teratogenicity, fertility, mutagenicity)
• Tissue culture

Question 3

Phase I

Answer 3

• Volunteer studies
• Clinical pharmacology in normal volunteers generating pharmacokinetic, metabolic and pharmacodynamic data
• Usually involves around 100 subjects
• Certain drugs such as cytotoxics can bypass this phase

Question 4

Phase II

Answer 4

• Clinical investigation to confirm kinetic and dynamics in patients
• Provides some evidence of efficacy and identifies a likely dosage range
• Involve up to 500 patients
• Looks at how the drug behaves in patients that may have comorbidities that affect how the drug works
• In case of cytotoxics it could be patients with late stage cancer and nothing to lose

Question 5

Phase III

Answer 5

• Formal therapeutic trials where efficacy will be established and evidence safely obtained
• Involves 1000-3000 patients
• All data submitted on completion

Question 6

Phase IV

Answer 6

• Post-marketing surveillance to produce evidence of long term safety
• May have involved tens or hundred of thousands of patients worldwide
• Clinicians have to report on first 10,000 pts
• There may be secondary benefits on another group of diseases

Question 7

Types of trials

Answer 7

• Double blind: neither patient nor doctor knows
• Single blind: patient doesn’t know, doctor does
• Prospective: more robust
• Retrospective

Question 8

Placebo controlled study

Answer 8

• 50 patients on active drug and 50 patients on placebo: compare outcome.
• Then compare with other therapy so 50 on study drug and 50 on comparison
• Can then assess what is more effective

Question 9

Cross over design

Answer 9

• 50 patients on study drug and 50 on compared
• Cross over after a set amount of time and a wash out period
• Then the patients are swapped

Question 10

Randomised

Answer 10

• Gold standard

- Patients assigned at random to either treatments or control

Question 11

Disadvantages of randomised

Answer 11

Subjects may not represent general patient population
Tend to be better at complying with medication
Need twice as many patients
Administratively complex
Some physicians and patients refuse

Question 12

Designing a study

Answer 12

• Need definitive hypothesis and end point
• Superiority or non-inferiority? Better than control or not worse?
• Choice of placebo or control drug… 50% placebo effective for anxiety
• Choice of patients: age and sex matched, race, other disease and drugs
• Are pts going to drop out? Comply?

Question 13

Importance of statistical power

Answer 13

• Need to choose statistical test
• Analyse if differences are due to chance…
• p<0.05 is usually taken as significance

Question 14

How can something have statistical significance and lack clinical significance?

Answer 14

• A drug may prove to be statistically good but not any better than the one on market at the moment
• Or it might be that there’s evidence that there’s no long term effect e.g. statins and cholesterol