1 / 39

Training Workshop on Pharmaceutical Development with focus on Paediatric Formulations Protea Hotel Victoria Junction, Wa

Pharmaceutical Development. Training Workshop on Pharmaceutical Development with focus on Paediatric Formulations Protea Hotel Victoria Junction, Waterfront Cape Town, South Africa Date: 16 to 20 April 2007. Physicochemical Properties of APIs and their relevance to formulation.

powa
Télécharger la présentation

Training Workshop on Pharmaceutical Development with focus on Paediatric Formulations Protea Hotel Victoria Junction, Wa

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Pharmaceutical Development Training Workshop on Pharmaceutical Development with focus on Paediatric Formulations Protea Hotel Victoria Junction, Waterfront Cape Town, South Africa Date: 16 to 20 April 2007

  2. Physicochemical Properties of APIsand their relevance to formulation Presenter: Peter York Professor of Physical Pharmaceutics Institute of Pharmaceutical Innovation (IPI), University of Bradford, UK (www.ipi.ac.uk) (p.york@bradford.ac.uk)

  3. Physicochemical Properties of APIs and their relevance to formulation Outline of presentation • Assurance of quality and safety of APIs • Spectrum of tests and criteria for specifications for APIs • Inter-dependency between ‘categories’ of properties • ‘Functionality’ testing related to formulation design • Summary of ‘challenges’ in API procurement and in evaluating APIs for formulation design

  4. Sources of APIs - Procurement • Patented compounds – from originators or their licenced suppliers • Non-patented APIs and generic APIs - transition from traditional supplying countries to other emerging nations eg India, China - consistency between ‘tender’ samples and following supplies from chosen supplier - pressure regarding CoG issues; no compromise with APIs for quality and safety

  5. Specifications and Standards for APIs • API suppliers – for patented compounds • Likely to be ‘licenced’ manufacturing agreement with originator, according to originator’s documentation • ‘Drug Master File’ (submitted to registration authorities) containing full details regarding synthesis, testing and analytical procedures, impurities (sources and limits), storage requirements; drug source will be originator or their licenced toll manufacturer • ‘Certificate of Analysis’ provided by API supplier; details results of routine tests applied to specified batches

  6. Specifications and Standards for APIs • Specific pharmacopoeial monographs for off-patent/generic APIs • Pharmacopoeias (eg BP) initiate new monographs for APIs approaching end of patent life, with support/dialogue with originator companies • USP, EP, Int Ph, and national pharmacopoeia (eg JP, BP) • Additional general guidance chapters and information provided in pharmacopoeias (eg testing methods…..)

  7. Generalised Content of API Monographs • Objective – to provide the standards required to ensure the quality and safety of API compounds; appropriate limitation of potential impurities rather than provide against all possible impurities • Monographs generally focus on chemical identification and purity assessment • Chemical properties – - structure, molecular weight and chemical formula, melting point, moisture content - identification tests - solubility in common solvents - impurities, related substances (resulting from synthesis, and potential of degredants from storage during shelf life of API), and limits for their contents - assay

  8. Generalised Content of API Monographs • Increasing awareness of need to monitor physical, crystallographic and ‘functional’ properties – some testing required by pharmacopoeial monographs • Such information can provide valuable aid to formulation design • Physical properties - moisture content - solid state/crystallography (eg polymorphism, level of solvation, crystalline/amorphous character) - particle properties (eg particle size) • Storage recommendations • NB indication of availability of reference standards provided

  9. Pharmacopoeial Monographs for APIs • Nomenclature/structure - follow international agreed systems (eg rINN, BAN; CASRN)) • Identification – means of verifying identity of API is as stated on the label - often two tests detailed –(for EP first is used in all circumstances, second if API complies with all other aspects of monograph) • Impurities/related substances - specific, discriminating analytic methods - substances controlled related to synthetic route (eg reagents, catalysts) - limits imposed by monographs (and general guidelines) - additional limits for known degredation products if API unstable on storage

  10. Pharmacopoeial Monographs for APIs • Assay - often a precise, non-specific (eg volumetric assay) test detailed - can use alternative assay method if known that alternative method will give a result of equivalent accuracy - purity figure related to reference substance - local reference material can be used if calibrated against official reference material - limits (range) based on data obtained in normal analytical practice, taking into account normal analytical errors, and acceptance of some variation in material eg aspirin – 99.5 – 101.5% (EP) eg erythromycin – sum of the contents of erythromycin A, B and C- 93.0 to 102%, with erythromycin B - maximum 5%, erythromycin C - maximum 5% (EP)

  11. Aspirin Molecule - Structure

  12. Erythromycin Molecules- Structure

  13. Pharmacopoeial Monographs for APIs • Storage recommendations - to avoid/minimise degradation for sensitive materials - to avoid/minimise any contamination - possible vectors leading to degradation - elevated temperatures, light, oxygen (free radicals), moisture/high humidity, microorganisms eg aspirin – store in an air tight container (EP) eg erythromycin- protect from light (EP)

  14. API Routine Testing – ‘Good Practice’ • Provide assurance of quality and safety • Verification of CoA and magnitude of testing programme • Sampling programme/isolated quarantine storage areas • Retention/storage of batch samples • Training programmes for staff, SOPs, GLP and validation of methods • ‘Confidence’ in consistent quality of supply from chosen suppliers

  15. API Properties – Formulation Design and Processing • 50% of new APIs, and many others, have very low aqueous solubility which can constrain drug dissolution (ie rate of solution) and thereby limit bioavailability • Many APIs exhibit polymorphism (also solvation – hydration) – alternative molecular packing of the same chemical in crystalline material leading to different properties such as dissolution rate) • Moisture content control – hygroscopic material often difficult to process (eg tabletting); change in hydration state (eg during wet granulation) • Respiratory drug delivery – DPIs and suspension MDIs require drug particle size (aerodynamic) of 1 – 5 microns • All above are also examples of QUALITY issues when formulating and processing APIs; may require additional testing and/or control procedures

  16. API Properties – Formulation Designand Processing • Additional tests (sometimes specified in monograph, or testing methods detailed in pharmacopoeias)- • Examples – - solubility/dissolution (ie rate of solution) - polymorphism (eg IR analysis) - chirality (pure chiral API compared with racemate – HPLC with chiral colomn, capillary electrophoresis (CE)) - particle sizing (eg microscopy, sieves) or particle surface area (eg gas adsorption, permeability) - particle sizing for inhalation products (eg cascade impactors for aerodynamic particle size measurement

  17. API Properties - Solubility • Descriptive solubilities • General rules – • Polar solutes dissolve in polar solvents • Non-polar solutes dissolve in non-polar solvents

  18. API Properties - Solubility • Many drugs are weak acids or weak bases • Dissociation (ionisation) constants and pea • Formulation and drug delivery issues • pKa of aspirin (weak acid) = 3.5 Change in degree of ionisation and relative solubility of weakly acidic and weakly basic drugs as a function of pH

  19. API Properties - Polymorphism • e.g carbamazepine, ritonavir Representation of two polymorphic forms of a crystal consisting of a molecule represented by a ‘hockey-stick’ shape

  20. API Properties – Crystallinity The disruption of a crystal (represented as a brick wall), giving the possibility for water vapour absorption in the amorphous region

  21. API Properties – Crystallinity • API pretreatment effects on crystallinity The amorphous content of a model drug substance following milling in a ball mill and a micronizer (Ahmed et al 1996).

  22. API Properties – Formulation Design and Processing • Alternative pre-treatment and processing of APIs (eg alternative final solvent used during final crystallisation step during synthesis of API; use of crystallisation rather than milling process for particle size reduction ) can lead to different surface properties of particles, such as interparticle cohesion and surface ‘charge’ • These phenomena can lead to different secondary processing behaviour and potentially variation in product performance

  23. API Properties – Particle Size Analysis • Microscopy – equivalent diameters Different equivalent diameters constructed around the same particle.

  24. API Properties – Particle Size Analysis • - eye-piece graticule: circles with diameters in progression • - particle size distribution (number basis) over range 2 – 200 microns Frequency distribution curves corresponding to (a) a normal distribution, (b) a positively skewed distribution and (c) a bimodal distribution.

  25. API Properties – Particle Size Analysis • Sieve analysis – equivalent diameters • - ‘stack’ of sieves • - particle size distribution (weight basis) over range 50 – 1000 microns Sieve diameter ds for various shaped particles

  26. API Properties Particle size, drug dissolution and bioavailability • Dissolution is measure of rate of solution • Dissolution related to particle size and particle surface area (smaller particle size, larger surface area, faster dissolution) = dissolution rate, A = surface area of solid, k = dissolution rate constant, Cs = saturation of drug, C = concentration of drug in solution)

  27. API Properties – Particle Size Reduction • Examples of drugs where a reduction in particle size has led to improvements in bioavailability

  28. API Properties – Biopharmaceutical Classification Scheme • Valuable classification system to guide formulators in requirements for ‘particle engineering’ of APIs • Consider aqueous solubility and permeability via oral route of delivery • Class I – high solubility, high permeability - rapid absorption, good bioavailability - eg propanolol, metaprolol • Class II – low solubility, high permeability - API controls absorption; potential for particle size effects on bioavailability - eg ketoprofen, carbamazepine

  29. API Properties – Biopharmaceutical Classification Scheme • Class III high solubility, low permeability - APIs dissolve rapidly and poorly absorbed - require fast API dissolution to maximise absorption - potential benefits from particle size reduction eg ranitidine, atenolol • Class IV low solubility, low permeability - challenging molecules, likely to exhibit low bioavailability eg hydrochlorothiazide, furosemide, - option to increase permeability - modify APIs as ‘prodrugs’

  30. API Properties – Prodrugs with modified permeability and absorption • Examples of prodrugs with improved permeability and oral absorption

  31. API Properties and Design of Medicines • Wide range of dosage forms - liquids, semi-solids, solids • Range of administration routes • Medicines containing more than one API • Single unit dosage and multi unit dose systems • Device, administration and compliance issues • All these are issues that can impose requirements for ‘desired’ API properties, in addition to chemical quality and safety assurance

  32. API Properties – Characteristicsto be considered when formulating medicines

  33. API Property Classification – inter-dependencies between ‘groupings’

  34. API Properties – Formulation Design and Processing • Formulation design – dosage form and delivery route issues, and ‘functionality’ tests for guiding choice of processing route and conditions • API stability, solubility (dissolution) and particle size are key properties for effective formulation design • For preparation of solutions, suspensions, granules for reconstitution - NB attention to stability (chemical and physical) and storage requirements • For solid dosage forms – eg tablets and capsules - NB biopharmaceutics classification - potential for increasing drug dissolution rate - potential for modifying drug solubility/permability (eg salts, prodrugs)

  35. API Properties – Formulation Designand Processing • Additional tests being considered for including in pharmacopoeias as tests for APIs (and solid particle excipients) - these include ‘functionality’ based (to standardise ‘performance’ of API in formulation and secondary processing) - characterisation of crystalline and partially crystalline solids (by X-ray powder diffraction) - porosity and pore size distribution of solids (by mercury porosimetry) - water-solid interactions (by sorption isotherms, hygroscopicity, water activity) - particle size analysis (by laser light diffraction) - calorimetric and thermal behaviour of powders

  36. ‘Life-Time’ of APIs • Appropriate specifications must be met throughout ‘life-time’ of API to ensure quality and safety • Life-time = from - isolation of API - API received by product manufacturer from supplier - API processed into pharmaceutical product - storage period of product (shelf life limit) to - end of period of administration of product to patient NB Alternative specifications will apply at the different stages

  37. Challenges for API Procurement and Evaluation • Compliance with CoA, and/or pharmacopoeial monograph • Consistency within/between batches, sampling issues • Alternative suppliers and CoG issues • Building confidence in supplying agencies • Quality and safety, quality and safety, quality and safety!!

  38. Challenges for API Formulation and Processing • Identify critical chemical, physical and ‘functional’ properties which are crucial for specific formulation requirements • Awareness of stability of API as pure substance, during formulation and processing, and through ‘shelf life’ of product • This information needs to be linked to the type of dosage form required, route of administration and desired ‘shelf life’ of product under ‘anticipated’ storage conditions

  39. Physicochemical Properties of APIs their relevance to formulation Summary and conclusion • Assurance of quality and safety of APIs • Spectrum of tests and specifications of criteria for APIs • Interdependency between ‘categories’ of API properties • ‘Functionality’ testing related to formulation design (and processing route and conditions) • Summary of ‘challenges’ in API procurement and in evaluating APIs for formulation design

More Related