This tutorial outlines the most common questions reviewers ask during protocol assessments and offers best practices for preparing sound, compliant answers.

✅ 1. How was the selection of stability storage conditions justified?

Reviewers often ask whether the selected conditions (e.g., 25°C/60% RH or 30°C/75% RH) reflect the product’s intended market. This requires referencing ICH Q1A (R2) for global zones or WHO guidelines for specific regional deployments.

• ➤ For a product intended for Zone IVB, why test only at 30°C/65% RH?
• ➤ Have you included appropriate long-term and accelerated conditions?
• ➤ Are refrigerated or frozen conditions evaluated for thermolabile products?

✅ 2. What is the rationale behind the chosen frequency of time points?

Agencies want to ensure the time points are sufficient to detect degradation trends without introducing unnecessary redundancy. For a 12-month study, reviewers may question missing data at months 3, 6, or 9.

Include justification such as:

• Historical knowledge from similar molecules
• ICH guidance for minimum time points (0, 3, 6, 9, 12, 18, 24 months)
• Regulatory alignment with past submissions

✅ 3. How did you determine the container closure system used in stability studies?

Agencies expect the tested packaging to represent the final marketed configuration. If using surrogate containers, provide strong rationale and risk analysis. You may get questions like:

• ➤ Does the material differ in permeability, surface area, or headspace?
• ➤ Are protective coatings or desiccants accounted for?
• ➤ How does this packaging impact photostability or moisture ingress?

✅ 4. Were Bracketing or Matrixing used? What’s the scientific basis?

If these statistical designs are applied to reduce testing, reviewers will ask for:

• ➤ A clear description of the design model
• ➤ Risk-based justification supported by prior data or literature
• ➤ Clarification on worst-case configurations tested

Referencing process validation strategies can support your rationale for product consistency across strength or pack sizes.

✅ 5. What analytical methods are being used? Are they stability-indicating?

Any protocol must explicitly state the validated, stability-indicating nature of the methods employed. Expect these questions:

• ➤ Are the methods specific to degradation products?
• ➤ Are LOD and LOQ values reported?
• ➤ Has forced degradation been conducted to prove specificity?

Consider referencing GMP compliance for analytical method validation expectations.

✅ 6. What criteria define stability failure?

Regulators expect predefined acceptance limits based on pharmacopeial or in-house specifications. Reviewer queries often focus on:

• ➤ How are OOS/OOT events handled?
• ➤ Are trending criteria included in protocol?
• ➤ Is microbiological stability covered for sterile products?

✅ 7. How does the protocol address photostability and thermal degradation?

Reviewers will ask if your protocol includes ICH Q1B compliant photostability testing or dedicated thermal cycling studies. You may need to explain:

• ➤ What light source and lux/hours were used
• ➤ Was the product exposed inside and outside of the packaging?
• ➤ Were visual changes, assay, and impurity levels monitored?

Similarly, thermal degradation studies might be required for thermosensitive compounds or to simulate shipping conditions.

✅ 8. How are significant changes or trends reported?

Regulatory bodies want clarity on how data trends will be handled. Include details such as:

• ➤ Trend analysis methodology (e.g., regression, control charts)
• ➤ Criteria for initiating investigations
• ➤ Impact of trends on shelf-life estimation and label claim

Stability trending is especially scrutinized for narrow therapeutic index drugs or injectable formulations.

✅ 9. Is the protocol designed to support extrapolated shelf life?

If you’re planning to use accelerated data or extrapolate beyond tested time points, reviewers will challenge your statistical justification:

• ➤ Do you have at least 6 months of accelerated + 6 months of long-term data?
• ➤ Has the Arrhenius equation or similar model been applied?
• ➤ Is shelf life extrapolation within regulatory limits (per ICH Q1E)?

✅ 10. Are critical quality attributes (CQAs) clearly defined?

Stability protocol reviewers look for clear CQA justification for tested parameters. Be prepared to answer:

• ➤ Why was a certain assay, impurity, or microbiological test chosen?
• ➤ Which attributes are considered stability-limiting?
• ➤ Are test methods qualified for those CQAs?

✅ 11. How is the protocol aligned with the overall control strategy?

Agencies will evaluate whether the protocol reflects product knowledge gathered during development and validation. Questions include:

• ➤ Is the protocol updated post-registration to incorporate change controls?
• ➤ Does the strategy link with ongoing product lifecycle monitoring?
• ➤ Are protocol revisions managed through your regulatory compliance process?

✅ 12. Has any harmonization been attempted across different markets?

Multinational submissions may receive queries on whether a single global protocol or multiple regional versions are used. Address these concerns by showing:

• ➤ Harmonized study designs meeting ICH, WHO, or local requirements
• ➤ Region-specific deviations and their rationale
• ➤ Impact of variations on global supply chain and labeling

✅ Best Practices to Minimize Reviewer Queries

• ➤ Follow ICH Q1A–Q1E, WHO Annex 10, and regional stability expectations
• ➤ Include a protocol review checklist aligned to agency focus areas
• ➤ Reference applicable guidances or past approvals where relevant
• ➤ Conduct internal QA review before submission
• ➤ Respond promptly and factually to agency information requests

Proactively addressing these common reviewer questions in your protocol helps reduce deficiency letters, improves review timelines, and builds regulatory trust.

Use this tutorial as a foundation for preparing your teams during protocol drafting and submission planning phases.