A drug development team is preparing a New Drug Submission for Health Canada. The stability data package — generated over 18 months at a contract laboratory — looks complete on its face. But during the internal review, a question arises: were the storage conditions selected based on the ICH Q1A(R2) guidance, or were they carried over from a study designed for a different market? The answer matters, because Health Canada reviewers will assess the stability data against the ICH Q1A(R2) framework, and gaps in study design can result in deficiency notices that delay approval.
This article is for pharmaceutical development teams, CMOs, and CROs responsible for designing, conducting, or reviewing stability studies for Health Canada submissions. We cover the ICH Q1A(R2) requirements as they apply in the Canadian context, the storage conditions relevant to the Canadian market, and the most common study design gaps we encounter.
ICH Q1A(R2), formally titled Stability Testing of New Drug Substances and Products, is the primary ICH guideline governing stability study design for new chemical entities and their drug products. Health Canada has adopted ICH Q1A(R2) as the standard for stability data submitted in support of drug submissions. The guideline applies to new drug substances and new drug products intended for human use.
ICH Q1A(R2) is part of a family of ICH stability guidelines that includes:
For most small-molecule drug products, ICH Q1A(R2) is the primary reference. Biological products are covered by ICH Q5C, which has different requirements.
One of the most practically important aspects of ICH Q1A(R2) is the specification of storage conditions for long-term, intermediate, and accelerated stability studies. The conditions are defined by ICH climate zones, which reflect the temperature and humidity conditions in different regions of the world.
Canada is classified as ICH Climate Zone I/II (temperate/subtropical), which corresponds to:
| Study Type | Temperature | Relative Humidity | Minimum Duration |
|---|---|---|---|
| Long-term | 25°C ± 2°C | 60% RH ± 5% | 12 months at submission; 24 months at approval |
| Intermediate | 30°C ± 2°C | 65% RH ± 5% | 6 months |
| Accelerated | 40°C ± 2°C | 75% RH ± 5% | 6 months |
For products intended for refrigerated storage (2–8°C), the long-term condition is 5°C ± 3°C, and the accelerated condition is 25°C ± 2°C / 60% RH ± 5%.
For products intended for frozen storage, the long-term condition is the intended storage temperature (e.g., -20°C ± 5°C), and no accelerated condition is typically required.
A common error we see is stability studies designed for ICH Climate Zone III/IV (hot/dry or hot/humid) conditions — appropriate for markets in parts of Asia, Africa, or South America — being submitted to Health Canada without confirmation that the Zone I/II conditions were also included. Health Canada reviewers will assess whether the submitted data supports the proposed storage conditions for the Canadian market specifically.
For new drug substances, ICH Q1A(R2) requires:
Stress testing is not the same as formal stability studies. The purpose of stress testing is to identify degradation products and establish the specificity of the stability-indicating analytical method. Stress testing data supports the method validation package and the impurity profile, but it does not substitute for the formal long-term and accelerated studies.
For new drug products, ICH Q1A(R2) requires long-term and accelerated studies on the drug product in its proposed commercial container-closure system. The container-closure system used in the stability study must be representative of the commercial packaging.
Key design considerations include:
Batch selection: A minimum of three primary batches of the drug product should be included in the formal stability program. At least two of the three batches should be at pilot scale or larger. The batches should be manufactured using a process representative of the commercial process.
Testing frequency: For long-term studies, testing is typically conducted at 0, 3, 6, 9, 12, 18, and 24 months, then annually. For accelerated studies, testing is conducted at 0, 3, and 6 months.
Stability-indicating methods: The analytical methods used in stability studies must be validated as stability-indicating — that is, they must be capable of detecting and quantifying degradation products without interference from excipients or other components. This is a critical requirement that links the stability program to the method validation package.
Specification setting: Stability data is used to set specifications for degradation products at the time of release and at the end of shelf life. Proposed specifications must be scientifically justified and consistent with the safety data for the identified degradation products.
ICH Q1A(R2) provides guidance on the statistical evaluation of stability data to determine shelf life. The recommended approach involves regression analysis of the quantitative stability attribute (e.g., assay, degradation product) over time, with a 95% confidence limit applied to determine when the attribute is predicted to fall outside its specification.
For attributes that show little or no change over time, a statistical analysis may not be necessary, and shelf life can be based on the available data without extrapolation. For attributes that show significant change, extrapolation beyond the observed data period is generally limited to 12 months beyond the last time point — and only if the data supports a linear trend.
Health Canada reviewers assess the statistical analysis as part of the submission review. Submissions that propose shelf lives based on limited data or that extrapolate beyond what the data supports will receive deficiency notices.
Stability study design decisions made early in development have long-term consequences for the submission timeline and the approved shelf life. Requirements may vary depending on the drug substance, the dosage form, and the proposed storage conditions. We recommend consulting a regulatory expert when designing stability programs for new submissions.
At Androxa, we provide stability testing services and regulatory support for Health Canada submissions, including study design review, method validation, and data interpretation. Contact us at testing-lab.ca to discuss your stability program.