Clinical trial phases MCQs With Answer

Clinical trial phases MCQs With Answer

by

Clinical trial phases MCQs With Answer is a focused practice set designed for B.Pharm students to master the objectives, design, and regulatory aspects of drug development. Covering Phase 0 through Phase IV, including Phase I dose-escalation, Phase II proof-of-concept, Phase III pivotal trials, and Phase IV pharmacovigilance, this resource emphasizes safety, efficacy, pharmacokinetics, pharmacodynamics, GCP and regulatory submissions. Questions also address trial designs, endpoints, randomization, blinding, adaptive trials, DSMBs and ethical considerations. The concise MCQs with answers help strengthen exam readiness and practical understanding for clinical research roles and pharmacy practice. Now let’s test your knowledge with 30 MCQs on this topic.

Q1. What is the primary objective of a Phase I clinical trial?

  • To confirm drug efficacy in thousands of patients
  • To assess safety, tolerability and pharmacokinetics in healthy volunteers or patients
  • To monitor long-term safety after marketing
  • To compare two approved drugs

Correct Answer: To assess safety, tolerability and pharmacokinetics in healthy volunteers or patients

Q2. Which phase primarily focuses on proof-of-concept and initial assessment of efficacy and dose-ranging?

  • Phase I
  • Phase II
  • Phase III
  • Phase IV

Correct Answer: Phase II

Q3. Which phase is designed to provide the definitive evidence of efficacy and safety for regulatory approval?

  • Phase I
  • Phase II
  • Phase III
  • Phase 0

Correct Answer: Phase III

Q4. What is the main purpose of Phase IV studies?

  • Initial human microdosing studies
  • Exploratory safety and PK in a few subjects
  • Post-marketing surveillance and long-term safety monitoring
  • Determining maximum tolerated dose in healthy volunteers

Correct Answer: Post-marketing surveillance and long-term safety monitoring

Q5. Phase 0 trials are best described as:

  • Large randomized controlled trials for efficacy
  • Microdosing exploratory studies to assess early PK/target engagement
  • Post-approval observational studies
  • Bioequivalence studies for generics

Correct Answer: Microdosing exploratory studies to assess early PK/target engagement

Q6. What does SAD and MAD stand for in early clinical studies?

  • Single-Animal Dosage and Multiple-Animal Dosage
  • Single-Ascending Dose and Multiple-Ascending Dose
  • Safety Assessment Design and Main Assessment Design
  • Standardized Adaptive Design and Modified Adaptive Design

Correct Answer: Single-Ascending Dose and Multiple-Ascending Dose

Q7. Which sequence correctly orders typical sample sizes from smallest to largest across phases?

  • Phase III < Phase II < Phase I
  • Phase I < Phase II < Phase III
  • Phase II < Phase III < Phase I
  • Phase IV < Phase III < Phase II

Correct Answer: Phase I < Phase II < Phase III

Q8. A pivotal trial intended to support a New Drug Application (NDA) is most commonly which phase?

  • Phase I
  • Phase II
  • Phase III
  • Phase 0

Correct Answer: Phase III

Q9. Randomized controlled trial (RCT) design becomes most essential in which phase to reduce bias in efficacy assessment?

  • Phase I
  • Phase II
  • Phase III
  • Phase 0

Correct Answer: Phase III

Q10. What is the primary role of a Data Safety Monitoring Board (DSMB)?

  • To recruit subjects across sites
  • To conduct laboratory analyses for sponsors
  • To independently monitor safety and interim data and recommend continuation/modification
  • To market the investigational product post-approval

Correct Answer: To independently monitor safety and interim data and recommend continuation/modification

Q11. What regulatory submission is typically required to start clinical trials in humans in the U.S.?

  • New Drug Application (NDA)
  • Investigational New Drug (IND) application
  • Marketing Authorization Application (MAA)
  • Post-marketing surveillance report

Correct Answer: Investigational New Drug (IND) application

Q12. Which submission seeks approval to market a new drug after successful clinical trials?

  • IND
  • Clinical Trial Authorization (CTA)
  • New Drug Application (NDA) or Biologics License Application (BLA)
  • Investigator’s Brochure

Correct Answer: New Drug Application (NDA) or Biologics License Application (BLA)

Q13. GCP refers to which set of standards in clinical research?

  • General Clinical Procedures
  • Good Clinical Practice
  • Global Compliance Protocols
  • Guaranteed Clinical Performance

Correct Answer: Good Clinical Practice

Q14. Which event qualifies as a Serious Adverse Event (SAE)?

  • Mild local redness that resolves in 24 hours
  • Transient headache not requiring treatment
  • Hospitalization, life-threatening event, disability or death
  • Minor laboratory fluctuation within normal limits

Correct Answer: Hospitalization, life-threatening event, disability or death

Q15. Blinding in clinical trials is primarily intended to:

  • Reduce drug manufacturing costs
  • Prevent unblinding of laboratory assays
  • Minimize bias in outcome assessment by participants and/or investigators
  • Ensure faster recruitment

Correct Answer: Minimize bias in outcome assessment by participants and/or investigators

Q16. An adaptive clinical trial allows investigators to:

  • Ignore interim safety data
  • Change design elements (e.g., sample size, dose arms) based on interim analyses under pre-specified rules
  • Enroll only a single subject indefinitely
  • Bypass ethical review boards

Correct Answer: Change design elements (e.g., sample size, dose arms) based on interim analyses under pre-specified rules

Q17. Bridging studies are designed to:

  • Compare two marketed drugs head-to-head
  • Extrapolate clinical data between different ethnic or regional populations to support approval
  • Replace Phase III trials entirely
  • Test new excipients in formulations

Correct Answer: Extrapolate clinical data between different ethnic or regional populations to support approval

Q18. What distinguishes an equivalence trial from a non-inferiority trial?

  • Equivalence trials aim to show two treatments are identically the same in all aspects
  • Equivalence trials test whether differences lie within a pre-specified margin both above and below; non-inferiority only tests not worse than margin
  • Non-inferiority trials require placebo groups always
  • Equivalence trials are always open-label

Correct Answer: Equivalence trials test whether differences lie within a pre-specified margin both above and below; non-inferiority only tests not worse than margin

Q19. Bioequivalence studies for generics primarily assess:

  • Therapeutic equivalence by long-term clinical outcomes
  • Similarity in rate and extent of absorption (Cmax and AUC) between formulations
  • Manufacturing process validation
  • Market share potential

Correct Answer: Similarity in rate and extent of absorption (Cmax and AUC) between formulations

Q20. Pharmacokinetics (PK) studies measure which of the following?

  • Drug effect on the body (PD)
  • Absorption, distribution, metabolism and excretion of the drug
  • Only adverse effects occurring post-marketing
  • Cost-effectiveness of therapy

Correct Answer: Absorption, distribution, metabolism and excretion of the drug

Q21. Pharmacodynamics (PD) primarily examines:

  • How the body affects the drug (PK)
  • The mechanism of drug action and relationship between concentration and effect
  • Only toxicology in animals
  • Stability of the drug product

Correct Answer: The mechanism of drug action and relationship between concentration and effect

Q22. The recommended Phase II dose (RP2D) is typically determined from:

  • Phase IV observational data
  • Phase I dose-escalation studies defining MTD or biologically effective dose
  • In vitro cell line experiments only
  • Marketing considerations only

Correct Answer: Phase I dose-escalation studies defining MTD or biologically effective dose

Q23. The primary efficacy endpoint of a pivotal Phase III trial should be:

  • Exploratory and decided post hoc
  • Clearly defined, clinically meaningful, and pre-specified in the protocol
  • Based only on biomarkers with no clinical relevance
  • Vague to allow flexible interpretation

Correct Answer: Clearly defined, clinically meaningful, and pre-specified in the protocol

Q24. Which body is responsible for independent ethical review of a clinical trial site?

  • Data Safety Monitoring Board (DSMB)
  • Institutional Review Board (IRB) or Ethics Committee (EC)
  • Regulatory agency reviewer only
  • Study sponsor’s marketing team

Correct Answer: Institutional Review Board (IRB) or Ethics Committee (EC)

Q25. Expanded access (compassionate use) programs allow patients to receive an investigational drug when:

  • There are adequate, approved alternatives available
  • The patient has a serious or immediately life-threatening condition and no comparable therapies exist
  • The drug has completed Phase IV only
  • The trial sponsor has already withdrawn the product

Correct Answer: The patient has a serious or immediately life-threatening condition and no comparable therapies exist

Q26. Placebo-controlled trials are ethically acceptable when:

  • There is an effective established therapy that must be withheld
  • Participants are not informed about placebo possibility
  • No proven effective therapy exists or withholding treatment does not cause harm
  • They are cheaper to run

Correct Answer: No proven effective therapy exists or withholding treatment does not cause harm

Q27. A surrogate endpoint is best defined as:

  • A direct clinical outcome such as survival
  • A biomarker or intermediate outcome that predicts clinical benefit
  • Always an unreliable measure
  • A statistical test for randomization quality

Correct Answer: A biomarker or intermediate outcome that predicts clinical benefit

Q28. Randomization in clinical trials primarily prevents:

  • Placebo effects entirely
  • Selection bias and helps balance confounding factors between groups
  • All adverse events from occurring
  • Need for statistical analysis

Correct Answer: Selection bias and helps balance confounding factors between groups

Q29. A multi-center clinical trial offers which main advantage?

  • Results are only valid for one hospital
  • Increases external validity and allows larger, more diverse populations
  • Eliminates the need for standard protocols
  • Reduces regulatory oversight

Correct Answer: Increases external validity and allows larger, more diverse populations

Q30. Phase III trials are usually powered to detect:

  • Pharmacokinetic parameters only
  • Statistically significant differences in primary clinical efficacy endpoints between treatments
  • Only safety signals without efficacy assessment
  • Purely biomarker fluctuations with no clinical meaning

Correct Answer: Statistically significant differences in primary clinical efficacy endpoints between treatments

Leave a Comment