Classification and control of investigational drugs MCQs With Answer

Classification and control of investigational drugs MCQs With Answer is a focused review designed for B. Pharm students to master regulatory and quality aspects of investigational medicinal products. This introduction covers classification (IND/IMP, placebo, comparator, orphan drugs), essential control measures (GMP, GLP, GCP, stability testing, analytical method validation), documentation (IB, IMP dossier, CMC), labeling, storage, release testing, and pharmacovigilance requirements. Emphasis is on practical control points, regulatory submissions, and quality systems that ensure patient safety during clinical trials. Clear understanding of these topics is critical for roles in QC, QA, regulatory affairs, and clinical supply management. Now let’s test your knowledge with 30 MCQs on this topic.

Q1. Which document primarily summarizes the quality, preclinical, and clinical data of an investigational drug for initial regulatory review?

• Investigator Brochure (IB)
• Common Technical Document (CTD)
• Investigational Medicinal Product Dossier (IMPD)
• Clinical Study Report (CSR)

Correct Answer: Investigational Medicinal Product Dossier (IMPD)

Q2. Under regulatory classification, an IMP refers to:

• Any marketed drug dispensed in hospitals
• An investigational medicinal product used in clinical trials
• A nutritional supplement used in studies
• A placebo only

Correct Answer: An investigational medicinal product used in clinical trials

Q3. Which regulatory submission is required in the United States before initiating human clinical trials?

• Marketing Authorization Application (MAA)
• Investigational New Drug (IND) application
• Clinical Trial Application (CTA)
• New Drug Submission (NDS)

Correct Answer: Investigational New Drug (IND) application

Q4. Which quality system specifically addresses laboratory study conduct and data integrity for nonclinical studies?

• GMP (Good Manufacturing Practices)
• GCP (Good Clinical Practice)
• GLP (Good Laboratory Practice)
• GDP (Good Distribution Practice)

Correct Answer: GLP (Good Laboratory Practice)

Q5. A stability-indicating method is defined as an analytical method that:

• Measures only the active pharmaceutical ingredient without detecting degradants
• Separates and quantifies the API in presence of degradation products
• Measures excipient purity only
• Is used only for biological products

Correct Answer: Separates and quantifies the API in presence of degradation products

Q6. Which label element is essential on an investigational drug container for a blinded phase II clinical trial?

• Dosage form only
• “For Investigational Use” with trial identifier
• Full SPC (Summary of Product Characteristics)
• Marketing authorization number

Correct Answer: “For Investigational Use” with trial identifier

Q7. Which parameter is NOT typically part of release testing for an IMP batch?

• Assay of active substance
• Sterility (if applicable)
• Marketing price
• Related substances/degradation products

Correct Answer: Marketing price

Q8. In clinical trials, the term “IMP accountability” refers to:

• Tracking production costs of the IMP
• Documenting receipt, dispensing, return, and destruction of IMP
• Pharmacovigilance reporting only
• Laboratory storage validation

Correct Answer: Documenting receipt, dispensing, return, and destruction of IMP

Q9. Which agency is primarily responsible for drug regulation in India?

• FDA (Food and Drug Administration)
• EMA (European Medicines Agency)
• CDSCO (Central Drugs Standard Control Organization)
• MHRA (Medicines and Healthcare products Regulatory Agency)

Correct Answer: CDSCO (Central Drugs Standard Control Organization)

Q10. Which concept ensures that manufacturing processes consistently produce IMPs meeting predefined quality attributes?

• Randomization
• Quality by Design (QbD)
• Double-blinding
• Placebo control

Correct Answer: Quality by Design (QbD)

Q11. Which test is critical for parenteral investigational products to ensure safety?

• pH only
• Microbial limits/sterility testing
• Color measurement only
• Viscosity only

Correct Answer: Microbial limits/sterility testing

Q12. A Suspected Unexpected Serious Adverse Reaction (SUSAR) must be reported to regulatory authorities within what context?

• Only after study completion
• Expedited reporting timelines per regulation
• At annual safety report submission only
• Never required for placebo subjects

Correct Answer: Expedited reporting timelines per regulation

Q13. Which section of the regulatory dossier describes manufacturing process, controls, and specifications for the IMP?

• Clinical overview
• Preclinical pharmacology
• CMC (Chemistry, Manufacturing, and Controls)
• Biostatistics plan

Correct Answer: CMC (Chemistry, Manufacturing, and Controls)

Q14. For temperature-sensitive IMPs, which control measure is most important during shipment?

• Using any available courier
• Validated cold chain packaging with temperature monitoring
• Labeling as “do not refrigerate”
• Increasing batch size

Correct Answer: Validated cold chain packaging with temperature monitoring

Q15. Blinding integrity is threatened when:

• IMP and placebo are identical in appearance and packaging
• Different manufacturers produce visually distinct study treatments
• Emergency unblinding procedures are in place
• Randomization codes are securely stored

Correct Answer: Different manufacturers produce visually distinct study treatments

Q16. Which analytical validation parameter evaluates the method’s ability to produce consistent results over time?

• Specificity
• Precision
• Limit of detection
• Robustness

Correct Answer: Precision

Q17. The Investigator Brochure (IB) primarily provides investigators with:

• Detailed GMP manufacturing instructions
• Nonclinical and clinical safety and efficacy summary
• Shipping manifests for IMP supply
• Marketing strategies

Correct Answer: Nonclinical and clinical safety and efficacy summary

Q18. Which control is essential to manage protocol deviations affecting IMP handling at a trial site?

• Ignoring minor deviations
• Documenting deviations, root cause analysis, and corrective actions
• Destroying all remaining IMP immediately
• Transferring responsibility to another site without records

Correct Answer: Documenting deviations, root cause analysis, and corrective actions

Q19. Which document lists critical quality attributes and acceptance criteria for the investigational product?

• Investigator’s CV
• Specification sheet
• Patient informed consent
• Trial protocol synopsis

Correct Answer: Specification sheet

Q20. In clinical supply management, “reconciliation” refers to:

• Comparing planned vs actual patient recruitment
• Accounting for IMP quantities: received, dispensed, returned, and destroyed
• Resolving ethical committee comments
• Pharmacokinetic sample analysis

Correct Answer: Accounting for IMP quantities: received, dispensed, returned, and destroyed

Q21. Which parameter is most relevant when selecting a primary container for a liquid investigational drug?

• Container color matching marketing samples
• Container-closure compatibility to prevent leachables and adsorption
• Vendor logo visibility
• Country of manufacture only

Correct Answer: Container-closure compatibility to prevent leachables and adsorption

Q22. What is the primary purpose of batch release testing before supplying an IMP to clinical sites?

• To calculate manufacturing costs
• To ensure each batch meets predefined quality and safety criteria
• To obtain marketing approval
• To randomize patients

Correct Answer: To ensure each batch meets predefined quality and safety criteria

Q23. Which action is required when a temperature excursion occurs during IMP storage at a trial site?

• Continue use without documentation
• Quarantine affected stock, document event, and follow sponsor assessment
• Discard entire site inventory immediately without assessment
• Blame courier and resume normal use

Correct Answer: Quarantine affected stock, document event, and follow sponsor assessment

Q24. Which term describes the marketed product used as a comparator in a clinical trial?

• Placebo
• Reference medicinal product
• Investigational buffer
• Blank control

Correct Answer: Reference medicinal product

Q25. Which element is mandatory in an informed consent regarding investigational drug risks?

• Guaranteed therapeutic benefit
• Description of foreseeable risks and adverse effects
• Manufacturer’s profit margin
• Exact mechanism of drug synthesis

Correct Answer: Description of foreseeable risks and adverse effects

Q26. Which of the following is a key component of pharmacovigilance in clinical trials?

• Drug marketing campaigns
• Active and passive adverse event collection and signal detection
• Only preclinical toxicity monitoring
• Shipment scheduling

Correct Answer: Active and passive adverse event collection and signal detection

Q27. For method validation, “specificity” demonstrates that the method:

• Produces the same result regardless of operator
• Can measure the analyte distinctly in presence of other components
• Is unaffected by temperature changes
• Has a low limit of detection only

Correct Answer: Can measure the analyte distinctly in presence of other components

Q28. Which regulatory concept ensures that labelling and packaging information protects blinded studies?

• Full disclosure of identity on outer packaging
• Use of coded labelling and trial identifiers
• Advertising labels on IMP
• Including marketing claims

Correct Answer: Use of coded labelling and trial identifiers

Q29. The primary role of GMP in investigational drug manufacture is to:

• Ensure promotional claims are accurate
• Ensure consistent product quality, safety, and traceability
• Replace the need for clinical monitoring
• Control patient randomization

Correct Answer: Ensure consistent product quality, safety, and traceability

Q30. Which document should describe procedures for emergency unblinding of an IMP for a subject?

• Investigator Brochure (IB) only
• Protocol and unblinding SOP
• Marketing Authorization
• Shipping manifest

Correct Answer: Protocol and unblinding SOP

G S Sachin

I am a Registered Pharmacist under the Pharmacy Act, 1948, and the founder of PharmacyFreak.com. I hold a Bachelor of Pharmacy degree from Rungta College of Pharmaceutical Science and Research. With a strong academic foundation and practical knowledge, I am committed to providing accurate, easy-to-understand content to support pharmacy students and professionals. My aim is to make complex pharmaceutical concepts accessible and useful for real-world application.

Mail- Sachin@pharmacyfreak.com