Particle Size and Polymorph of Drug Substance

1. Particle Size and Polymorph of Drug Substance Summary Slides

2. Polymorph

3. Screening for Polymorph • Diversity in approaches • Focus on DS manufacturing process solvents • Investigate beyond solvents in DS manufacturing process and impact on DP process • Data should be discussed at the EOP2 meeting • Reviewers want assurance of “due diligence”

4. Polymorph Acceptance Criteria • Qualitative test may be adequate when only one of multiple polymorphs is consistently produced • “Sunset” or “Skip” testing might be an option after demonstration of control • More complicated situations may need bioavailability data to resolve • compare polymorph performance of mixtures and pure forms

5. Complicated Situations • DS polymorph changes throughout a manufacturing process or during stability • Drug product containing DS with multiple polymorphs having different bioavailabilty

6. Things to Consider • How close is solution dosage form to saturation solubility for least soluble polymorph • If an amorphous DS is considered for development an EOP2 meeting is important to discuss data. • Decision tree 4 in polymorphism • How different is “different” • “Change” includes DP manufacture and stability

7. Common Thoughts • Do we need more dialog to enable FDA and industry to understand what is needed to establish tests and acceptance criteria? • Case studies • From joint Industry/Agency group • Is there negative impact from providing additional data and rationale the FDA seems to be asking of Industry?