Why Dosage Form Affects Packaging Strategy

The physicochemical properties of the dosage form determine its susceptibility to degradation. Solid tablets may be vulnerable to moisture and oxidation, while liquid formulations require protection from microbial contamination, evaporation, and chemical instability. Hence, packaging material and design must align with the dosage form’s specific vulnerabilities.

Common Packaging Types for Oral Dosage Forms

Key Differences in Packaging Criteria

• Barrier Properties: Solid dosage forms need low WVTR (Water Vapor Transmission Rate); liquids require low extractables and leachables
• Seal Integrity: Critical for liquids to prevent leakage and microbial ingress
• Material Compatibility: Some liquids may react with plastics, while solids are generally inert
• Dosage Delivery: Liquids often require dosing spoons/syringes, impacting closure design

Stability Testing Focus: Solid vs. Liquid Forms

In long-term and accelerated stability studies:

• Solids: Assessed for hardness, friability, impurity growth, disintegration time
• Liquids: Evaluated for pH, microbial limits, viscosity, precipitation, color change

Packaging must prevent these changes by maintaining physical and chemical protection across ICH stability zones.

Regulatory Requirements for Packaging Selection

According to EMA and ICH Q1A(R2), packaging used in stability studies must reflect the final market configuration. This ensures that results are representative of real-world conditions. Packaging details must be captured in CTD Module 3.2.P.7:

• ✓ Container material and type
• ✓ Closure components and liners
• ✓ Description of protective features (e.g., UV barrier, desiccant use)
• ✓ Container closure integrity results

Physical Testing of Packaging During Stability

• Torque Testing (for screw caps on liquids)
• Seal Integrity Testing (for blister packs or vials)
• Moisture Uptake Evaluation (for solids in high humidity)
• Leachables and Extractables (for plastic bottles with syrups)
• Label Durability and Print Adhesion

Case Study: Packaging Selection for a Moisture-Sensitive Tablet vs. Syrup

A moisture-sensitive antihypertensive tablet was packaged in Alu-Alu blister with desiccant carton, while its pediatric syrup version was stored in amber PET bottle with child-resistant cap. The tablet remained stable across 40°C/75% RH zones for 6 months. However, the syrup exhibited color change due to poor UV barrier. Switching to amber glass prevented degradation. Lesson: Each dosage form demands custom packaging strategy validated through stability data.

Checklist: Dosage Form-Specific Packaging Evaluation

• ☑ Have the moisture and light sensitivity of the API been evaluated?
• ☑ Is the container material compatible with the dosage form?
• ☑ Are extractables and leachables under control for liquids?
• ☑ Is seal integrity verified for blister/vial/pouch?
• ☑ Are delivery devices (e.g., droppers, syringes) included in stability?
• ☑ Does the packaging match the final marketed presentation?

Stability Protocol Adaptations Based on Packaging

The stability protocol should specify storage orientations (upright for liquids), light protection measures, and specific test intervals for packaging integrity checks. For solids, blister packs require ongoing visual inspection for delamination, while liquids may need pH and viscosity tests at each pull point.

Best Practices in Packaging Documentation

To maintain GMP compliance and audit readiness:

• Include detailed packaging specifications in the stability protocol
• Ensure traceability of packaging material lots used in stability
• Archive container-closure validation reports
• Document change control for packaging-related updates

Refer to resources at GMP guidelines for documentation templates and packaging validation SOPs.

Conclusion

Solid and liquid oral dosage forms present distinct packaging challenges. Stability testing must account for these differences to select the right packaging configuration. Through rigorous evaluation of compatibility, permeability, and container closure integrity, pharmaceutical manufacturers can ensure product stability, regulatory compliance, and patient safety throughout the product’s shelf life.

References:

• ICH Q1A(R2) Stability Testing of New Drug Substances and Products
• USP Containers – Performance Testing
• FDA Guidance for Industry: Container Closure Systems
• EMA Guideline on Plastic Immediate Packaging Materials
• WHO Guidelines for Stability Testing of Pharmaceutical Products