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Excipient Composition and Performance-Related Properties of Excipients
Chris Moreton, Ph.D.FinnBrit Consulting
IPEC-Americas FDA Seminar, October 21, 2013
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Presentation Outline
• How excipient performance arises• Excipient composition• Excipient form• Excipient performance examples
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Excipient Performance• Most often we do not know just what correlates
with the performance of an excipient in a particular application (formulation).
• What we can say is that performance must arise from a combination of:– The chemical composition of the excipient
• The chemical nature of the nominal excipient• The composition profile of the excipient
– Including concomitant components!• Molecular weight distribution for polymers
– The physical properties of the excipient– The physical form of the excipient
• Excipient performance will change with the application (formulation).
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Excipient Composition
• What are excipients comprised of?– The nominal excipient– What else?
• It depends!– The source of the raw materials
(feedstock)– How the excipient is manufactured– How the excipient is processed– Are there any additives?
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Excipient Manufacturing: Sources of Excipient
Components
1. Concomitant components2. Residual solvents3. Residual catalysts4. By-products
Processing steps
Final isolation
PackagedExcipient
Processing aid
Additives
Starting material(s)
(Feedstock)
Co-processing component
Finishing
1. Residual solvents
Bulk finished excipient
Excipient composition1. ‘Nominal’ component(s)2. Additive(s)3. Processing aid(s)4. Concomitant components5. Residual processing aids6. Residual solvents7. Residual catalysts8. By products9. Unreacted starting materials10. Starting material components
Co-processing component
1. Concomitant components2. Unreacted starting material3. Other components from starting
materials4. Starting material impurities
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Chemical Composition of the Excipient
• Nominal chemical– Polymer molecular weight distribution
• Concomitant components– Reaction by-products– Residual starting materials and reagents– Processing aids
• Undesirable components– Potentially toxic components, e.g. monomer residues in
some polymers• Residual solvents• Elemental residues• Water• Additives
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Physical Properties of the Excipient
• Molecular properties– UV absorption– Optical rotation
• Aggregate properties (molecular interactions)– Melting behavior
• Bulk properties– Powder flow– Bulk and tapped densities
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The Physical Form of the Excipient
• Polymorphism• Particle size distribution• Particle morphology
– Needle crystals– Plate crystals– Dendritic crystals
• Particle structure– Total surface area vs. ‘envelope’ surface
area8
Challenges in understanding the link between Excipient Composition and
Excipient Performance• We know what we know.• BUT we do not know how much we don’t know!• We can see the effects of poor understanding in
failed product batches:– But is it the API, the excipient, the process or a
combination of them?• We can sometimes link poor performance to a
particular material attribute, but only for a specific application:– We do not have a universal understanding of the link
between excipient composition and performance.• Is there one?
• We frequently do not properly understand what we need to measure, and we very often do not have adequate methods with which to measure.
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Excipient Performance
• Since excipient performance will vary from application to application, it follows that we can only truly assess performance in the actual application (formulation).
• We need surrogates for excipient performance:– USP-NF <1059> Excipient Performance– Ph.Eur – Functionality-related Characteristics
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Examples
1. Microcrystalline Cellulose2. Dibasic Calcium Phosphate,
Dihydrate
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Cellulose structure
Courtesy JRS
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Microcrystalline Cellulose
Courtesy JRS Pharma
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Microcrystalline Cellulose
• Microcrystalline cellulose (MCC) contains:– Cellulose-I (-cellulose)– Cellulose-II (β-cellulose)– Hemicelluloses– Ammonia residues– Formic acid/formaldehyde– Sugar residues (intrinsic aldehyde type
reactions)• Very ‘pure’ -cellulose does not perform as
well as MCC• BUT what are the components to control?• What method(s)?
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MAIN GRADES OF MICROCRYSTALLINE
CELLULOSE Grade Size Characteristics
PH 101ca. 50 µmPH 102ca. 90 µmPH 103ca. 50 µm Moisture content < 3%PH 105< 20 µmPH 112ca. 90 µm Moisture content < 1.5%PH 113ca. 50 µm Moisture content < 1.5%PH 200ca. 180 µmPH 200 LM ca. 180 μm Moisture content <
3%PH 301ca. 50 µm Higher densityPH 302ca. 80 µm Higher density
Ceolus KG 802 ca. 50 µm Lower densityCeolus UF 711 ca. 50 μm Lower density, better flowCeolus KG 1000 ca. 50 μm Very low density
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Dibasic Calcium Phosphate Dihydrate
• CaHPO4.2H2O (DCP-D)• Deforms during tablet manufacture by
fragmentation (brittle fracture)• We can make very pure DCP-D using precipitated
calcium carbonate and so-called ‘green’ phosphoric acid.
• This very pure material does not perform well in compaction.
• The fragmentation appears to be due to dislocations in the DCP-D crystal lattice from the presence of foreign cations.
• The very ‘pure’ DCP-D appears not to have sufficient lattice dislocations, and thus does not fragment adequately to make strong enough compacts.
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Dibasic Calcium Phosphate Dihydrate
• So what do we need to control?• Do we have the methods?• Could this conflict with the proposed
limits for elemental impurities?
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Additives in Excipients• There is a lot of misunderstanding in the area:
– There are additives that have been present for many years, but have not been declared:
• Excipient manufacturers have been unaware of the requirements of USP-NF General Notices
• Intellectual property issues surrounding additives.– We need to be careful we do not inadvertently cause
excipient manufacturers to withdraw from servicing the pharmaceutical sector.
– Some so-called ‘additives’ are actually processing aids carried over from earlier stages in the processing or extraction of the excipient.
– IPEC-Americas has an active project in this area, and will be requesting a meeting with the FDA in 2014 to suggest a possible resolution.
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Conclusions
• We do not know enough about any excipient to state that we completely understand the link between excipient composition and form, and the performance of that excipient across different applications.
• Performance related surrogates will need to be specified on a case by case basis.– Between the User and the supplier.
• Excipient composition will continue to be an issue.
• Communication and acceptance of Additives in excipients is an issue that needs to be resolved.
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