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Preformulation studies

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Pre-formulation studies
Pre-formulation studies • Evaluation of drug prior to formulation development → pre- formulation studies. Why pre-formulation studies required? • Drug discovery and development → complex, lengthy process • Failure of a molecule during development stage • Reasons →poor pharmacokinetics, lack of efficacy, and/or toxicity
Significance of pre-formulation studies • Understanding the physical and chemical properties of a drug helps to formulate the crude drug into a suitable dosage form/ various dosage regimens etc. • Lead to simple and elegant formulations/ successful commercial products Provides the scientific basis for formulation development Classification of pre-formulation studies (i) Fundamental properties →specific to drug, chemical structure (ii) Derived properties→ related to development of specific dosage form
Preliminary pre-formulation study and molecular optimization Active pharmacological compound invention Preliminary studies on suspected problem area Development into its optimum molecular state Stability and solubility→ molecular modification E.g. salts, pro-drug, solvates, polymorphs, or even new analogs
Salt approach • Solubility problem is resolved by converting into salt form • Compound having ionisable group are converted into salt • Ephedrine →Ephedrine hydrochloride, ↑solubility/ dissolution/ bioavailability Pro-Drug approach • Prodrugs are synthetic derivatives (esters, amides) → transformation in vivo to liberate the active drug molecule. • Erythromycin is water soluble, has a bitter taste, and is rapidly hydrolyzed in gastric acid • Erythromycin estolate, the lipophilic ester prodrug , absorbed 4 times more efficiently, but hydrolyzed only 24% in serum.
Initial / preliminary solubility investigation Total solubility (cs) • Total solubility (Cs) is solubility of ionized + unionized form of the drug • Method→ Equilibrium solubility method • Procedure: Excess solute + solvent → agitate at constant temperature until equilibrium, chemical analysis of drug Intrinsic solubility (Co) • Intrinsic Solubility (Co) is solubility of only unionized form of the compound. • The solubility obtained in acid (0.1 N Hcl) for a weak acid • The solubility obtained in alkali (0.1 N NaOH) for a weak base • Unit →the number of moles of solute per litre that dissolves into solution at 25oc.
Effect of pH on solubility of drug • Weak acid solubility increases with increase in pH • Weak base solubility increases with decrease in pH • Amphoteric drug solubility increases with increase/ decrease in pH • Neutral drug no change in the solubility with change in pH The solubility should ideally be measured at two temperatures Max. density of water is at 4 o C – to check mini. aqueous solubility. 37 o C to support biopharmaceutical evaluation.
Solubility in various pH Every new drug must be determined as a function of pH ,why? • Over the physiological pH range of 1-8. • For relatively insoluble drugs , rate of dissolution depends on its solubility which can influence its biological absorption. • Stability during processing Henderson -Hassel Bach equation to find ratio of ionised/unionised drug • pH = pKa + log [(un-ionized drug) / (ionized drug)]→basic drug • pH = pKa + log [(ionized drug) / (un-ionized drug)]→acidic drug
Stability studies (i)Solid state stability, (ii)Solution phase stability → ICH guidelines Solid state stability Physical stability Polymorphism, hygroscopicity Factors influencing physical stability Solubility, pKa, melting point, crystal structure , equilibrium moisture content Chemical stability Degradation, hydrolysis, oxidation, photo-degradation…. Factors influencing chemical stability → heat, light, moisture, oxygen
Effect of temperature on stability • Elevated temperatures like 400C, 500 and 600 etc. / ambient humidity • Are compared with a control for any physical /chemical change. • The data obtained may be extrapolated by Arrhenius treatment • The degradation rate at a lower temperature is determined ICH guidelines Long term→ 25± 2°C/60% ± 5% RH or 30 ± 2°C/65RH ± 5% RH for 12 months Intermediate→ 30 ± 2°C/65% ± 5% RH for 6 months Accelerated → 40 ± 2°C/75% ± 5% RH for 6 months
Stability studies under high humidity conditions The presence of high humidity conditions some drugs tend to hydrolyse Some tend to react with other excipients Some drugs tend to oxidize. • During stability study the drug is exposed to different relative humidity conditions • Controlled humidity conditions may be obtained by using laboratory desiccators. Application To find the material is to be protected/ stored in a controlled low humidity environment  Formulation planning Eg. An aqueous based granulation system is to be avoided or not.
Photolytic stability • Many drug will fade / darken on exposure to light. • The extent of degradation depends on the exposed surface area • Can be overcome→ protection of the drug using an amber coloured container / a photo stable dye in the system/dark place/physical barriers • For confirmatory studies, • Samples are exposed to light providing an overall illumination of • Not less than 1.2 million lux hours and an integrated near ultraviolet energy of not less than 200 watt hours/square meter . • Samples may be exposed side-by-side with a validated chemical actinometric system.
Stability to oxidation • Testing its stability in an atmosphere of high oxygen tension usually at 40% oxygen atmosphere. • Results are compared against a standard stored under the inert or ambient conditions. Application of test for Sensitivity to oxygen • To decide atmospheric conditions for product packing • To Include an anti-oxidant in the formulation Stability to pH • The pH stability profile data helps in predicting solid state stability of a drug in the presence of acidic and basic impurities.
SOLUTION PHASE STABILITY • Why solution phase stability is required ? Stability of the drug from pH ranging from 1 to 8 is to be investigated To assure that the substance does not degrade when exposed to GI fluids. It is important for the selection of granulation solvent and the drying conditions.
Developing a Profile of the Active Pharmaceutical Ingredient When preliminary pre-formulation study assures the solubility/ stability of compound The best (optimum) molecular form of a drug has been selected Physicochemical characterization begins Following parameters are to be studied further Fundamental Properties • Physical description/Organoleptic properties • Analytical methods, Purity • Partition coefficient, ionization constant • Crystal properties and polymorphism • Dissolution, Permeation across the membrane Derived Properties Compatibility Studies : Stability in the presence of excipients
PHYSICAL DESCRIPTION/ORGANOLEPTIC PROPERTIES Colour, physical appearance, taste and odour The colour • attributes of a drug substance will be indicative of stability problems, • May indicate the necessity of improving the appearance by including a dye in the body or the coating of the final product. Taste • May indicate palatability problems • Excipients and flavours may also be used to obtain desired taste. Odour • Is indicative of degradation products ( Aspirin hydrolysis imparts odour of acetic acid). • Also may indicate the need of flavours and excipients in the formulations for required odour.
ANALYTICAL METHODS: UV SPECTROSCOPY • The first requirement , the development of a simple analytical method for quantitative estimation in subsequent steps. • Most of drugs have aromatic rings and/or double bonds as part of their structure and absorb light in UV range. • UV spectroscopy being a fairly accurate and simple estimation technique • The absorption Co-efficient (E) of the drug can be determined by the formula: E = AF / X A=Absorbance, F = dilution factor, X = weight of drug (mg) • It is now possible to determine concentration of drug in any solution by measuring absorbance C = AF/E mg/ ml
Purity • The determination of the purity and the data will help further studies to be carried out safely. • All the impurities present in the compound should be within the range specified. • Impurities may affect the stability of the compound and also the appearance of the compound. • Some impurities may make the compounds toxic. • The techniques used in the purity studies are TLC, HPTLC, paper chromatography, HPLC, XRD and GC.
Dissolution • Dissolution precedes absorption • The dissolution behaviour should be investigated • To make necessary changes to enhance the dissolution rate /to select an optimum form for its development.
Dissolution rate and Noyes-Nernst equation dW/dt = dissolution rate A = surface area of the dissolving solid D=diffusion coefficient V= volume of the medium, h = thickness of the diffusion layer Cs =concentration of solute in diffusion layer, C =solute concentration in the bulk medium
Factors affecting dissolution rate Physicochemical properties like • Crystal habit, • Particle size, • Surface area, • Solubility, • Wetting properties, • Hydration/solvation Extrinsic factors like • Test apparatus, • rpm, • Viscosity, • pH, • Flow rate, • Temperature
The intrinsic dissolution rate (IDR) • The dissolution rate of a pure active substance, where the conditions of surface area, temperature, agitation, and medium pH and ionic strength are all constant. • Using a specific device for this purpose, where the compressed drug is exposed in a dissolution medium over a constant surface area, and its value is expressed in mg cm-2 s-1. • IDR data helps to obtain the chemical purity and equivalence of drugs from different sources.
Parameters Affecting Absorption The absorption of drugs consists of 2 processes; The dissolution of the drug molecules Its transport across the GI/biological membrane into the systemic circulation. For the relatively soluble compounds, the rate determining step is the permeation across the membrane For the relatively insoluble compounds, the rate determining step is the rate of dissolution. The three main parameters that influence the rate of absorption are partition coefficient, ionization constant and the permeation across the membrane.
Partition coefficient • Partition coefficient→ the ratio of the concentration of the drug in the oil phase to that in the aqueous phase. • n-octanol is used as the oil phase / water as the aqueous phase • Other organic solvents→ chloroform, ether, amyl acetate etc. Method • Known amount of drug + two phases → equilibrating, separation of the phases, analysis of drug
Partition coefficient Partition Coefficient(P) = [Organic] / [Aqueous] • Log P= log10 (Partition Coefficient) Log P = 1 → 10:1 Organic: Aqueous Log P = 0 → 1:1 Organic: Aqueous Log P = -1 → 1:10 Organic: Aqueous
Ionization constant • Most drugs are weak acids or bases , • They exist as ionized or unionized species based on the pH of the medium. • Unionized species are easily absorbed as they are lipid soluble. The pH partition theory includes three principles 1. The pH as the site of absorption, 2. Ionization constant 3. Lipid solubility of the drug
The relative concentration of the ionized and the unionized form Henderson Hassel Bach equation pH = pKa + log [unionized form] / [Ionized form] FOR BASES pH = pKa + log [ionized form]/ [unionized form] FOR ACIDS Ratio can be determined • Potentiometric pH-Titration, • pH-Spectrophotometry Method, • pH-Solubility Analysis.
Permeation across the membrane • in vitro experiments using biological membranes. • The method used is the everted rat gut method. • This technique determines the degree & rate of passage of drug through the membrane sac by passive & active transport.
Crystal properties and polymorphism • Drug can exist in more than one crystalline from with different space lattice arrangements → Polymorphism • Pre-formulation activity → Study on Crystal structure, polymorphism, and solvate form Changes in crystal characteristics can influence bioavailability chemical and physical stability in dosage form process functions like flow and compaction behaviours in tablet dosage form Techniques are used to determine crystal properties • Hot stage microscopy, thermal analysis, infrared spectroscopy, and X- ray diffraction.
Derived Properties • Derived pre-formulation properties are carried out • to learn about the issues related to development of a particular dosage form • like solid oral, liquid oral or parenteral.
Derived properties for solid dosage form • Particle size, shape and surface area • Powder Flow Properties • Density • Hygroscopicity • Compactibilty and compressibility • Wettability (for Suspension also)
Excipient selection • Chemical structure of the API • Its physicochemical characteristics • The type of delivery system required • The proposed manufacturing process.
Compatibility studies • Compatibility studies are usually the last activity • Studying the interactions of drug substance with other excipients Need of compatibility study • for careful selection of the excipients • To facilitate administration • To promote the consistent release and Bioavailability of the drug • To protect it from degradation.
Methods used to study DEC • DSC- Differential Scanning Calorimetry • DTA- Differential Thermal Analysis, • FT-IR Spectroscopy, • DRS-Diffuse Reflectance Spectroscopy, • TLC-Thin Layer Chromatography, • HPLC-High Pressure Liquid Chromatography, • XRD
Characteristics of Powder XRD and its interpretations • Results of the PXRD procedure are commonly presented as • Peak positions at 2θ and X-ray counts (intensity) • in the form of a table or a x-y plot, • known as diffractogram.
Characteristics of Powder XRD and its interpretations • It is reliable and powerful tool for crystalline sample identification. • It is a non-destructive technique. • Each crystalline substance has a unique X-ray diffraction pattern.
Crystal structure • Crystal structure is a description of the ordered arrangement of atoms, ions or molecules in a crystalline material. • Crystal lattice is the periodic and systematic arrangement of atoms. • The smallest portion of a crystal lattice is called Unit Cell.
Crystal structure and X-RAY diffraction pattern • The crystallographic planes are geometric planes linking atoms/ions/molecules in crystal lattice. • Given any plane in a lattice, there is an infinite set of parallel lattice planes (family of planes) that are equally spaced (d value) from each other. • More the number of planes in given family greater is the intensity of peaks
X-Ray diffraction pattern • Higher the intensity greater the crystallinity • Their widths are rather dependent on particle size (overly small particles will result in line broadening) i.e. broad nature of peak indicates higher degree of amorphousness or less crystalline in comparison with other samples • The number of observed peaks is related to the symmetry of the unit cell (higher symmetry generally means fewer peaks).
DIFFERENTIAL SCANNING CALORIMETRY (DSC) • DSC is a technique in which the difference in energy inputs into a substance and a reference material is measured as a function of temperature while the substance and reference material are subjected to a controlled temperature program. • The graph of heat flow in mJ/s on the Y-axis plotted versus temperature at a fixed rate of change of temperature in °C on the X-axis shows the output of the DSC.
Application and Interpretation of DSC curves • To check the Purity , • For polymorph identification, • To check decomposition
• Determination of melting point • The enthalpy (Heat of fusion)
• Drug-excipient compatibility
FTIR spectra • The Functional Group Region (4000-1500 cm-1) • The Fingerprint Region (1500-400 cm-1)
Characteristics of IR spectra and its interpretation • Used as a supplementary technique to investigate the DEC and to confirm the results obtained by the thermal analysis. • The appearances of new absorption band, broadening of band, and alteration in intensity are the main characteristics to evidence DEC. • IR is most useful in providing information about the presence or absence of specific functional groups. • Different bonds have diff. frequencies Eg; C-C, C=C, C ≡ C, C-O, O-H, N-H • IR does not provide detailed information or proof of molecular formula or structure. • Hydrogen bonding (Physical interaction) and shift in IR peaks: The number and strength of hydrogen bonds differs with chemical environment. The force constant varies and the wavenumber differs at which these molecules absorb infrared light. The number and strength of intermolecular interactions varies greatly within the sample, causing the bands in these samples to be particularly broad.

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Preformulation studies

  • 2. Pre-formulation studies • Evaluation of drug prior to formulation development → pre- formulation studies. Why pre-formulation studies required? • Drug discovery and development → complex, lengthy process • Failure of a molecule during development stage • Reasons →poor pharmacokinetics, lack of efficacy, and/or toxicity
  • 3. Significance of pre-formulation studies • Understanding the physical and chemical properties of a drug helps to formulate the crude drug into a suitable dosage form/ various dosage regimens etc. • Lead to simple and elegant formulations/ successful commercial products Provides the scientific basis for formulation development Classification of pre-formulation studies (i) Fundamental properties →specific to drug, chemical structure (ii) Derived properties→ related to development of specific dosage form
  • 4. Preliminary pre-formulation study and molecular optimization Active pharmacological compound invention Preliminary studies on suspected problem area Development into its optimum molecular state Stability and solubility→ molecular modification E.g. salts, pro-drug, solvates, polymorphs, or even new analogs
  • 5. Salt approach • Solubility problem is resolved by converting into salt form • Compound having ionisable group are converted into salt • Ephedrine →Ephedrine hydrochloride, ↑solubility/ dissolution/ bioavailability Pro-Drug approach • Prodrugs are synthetic derivatives (esters, amides) → transformation in vivo to liberate the active drug molecule. • Erythromycin is water soluble, has a bitter taste, and is rapidly hydrolyzed in gastric acid • Erythromycin estolate, the lipophilic ester prodrug , absorbed 4 times more efficiently, but hydrolyzed only 24% in serum.
  • 6. Initial / preliminary solubility investigation Total solubility (cs) • Total solubility (Cs) is solubility of ionized + unionized form of the drug • Method→ Equilibrium solubility method • Procedure: Excess solute + solvent → agitate at constant temperature until equilibrium, chemical analysis of drug Intrinsic solubility (Co) • Intrinsic Solubility (Co) is solubility of only unionized form of the compound. • The solubility obtained in acid (0.1 N Hcl) for a weak acid • The solubility obtained in alkali (0.1 N NaOH) for a weak base • Unit →the number of moles of solute per litre that dissolves into solution at 25oc.
  • 7. Effect of pH on solubility of drug • Weak acid solubility increases with increase in pH • Weak base solubility increases with decrease in pH • Amphoteric drug solubility increases with increase/ decrease in pH • Neutral drug no change in the solubility with change in pH The solubility should ideally be measured at two temperatures Max. density of water is at 4 o C – to check mini. aqueous solubility. 37 o C to support biopharmaceutical evaluation.
  • 8. Solubility in various pH Every new drug must be determined as a function of pH ,why? • Over the physiological pH range of 1-8. • For relatively insoluble drugs , rate of dissolution depends on its solubility which can influence its biological absorption. • Stability during processing Henderson -Hassel Bach equation to find ratio of ionised/unionised drug • pH = pKa + log [(un-ionized drug) / (ionized drug)]→basic drug • pH = pKa + log [(ionized drug) / (un-ionized drug)]→acidic drug
  • 9. Stability studies (i)Solid state stability, (ii)Solution phase stability → ICH guidelines Solid state stability Physical stability Polymorphism, hygroscopicity Factors influencing physical stability Solubility, pKa, melting point, crystal structure , equilibrium moisture content Chemical stability Degradation, hydrolysis, oxidation, photo-degradation…. Factors influencing chemical stability → heat, light, moisture, oxygen
  • 10. Effect of temperature on stability • Elevated temperatures like 400C, 500 and 600 etc. / ambient humidity • Are compared with a control for any physical /chemical change. • The data obtained may be extrapolated by Arrhenius treatment • The degradation rate at a lower temperature is determined ICH guidelines Long term→ 25± 2°C/60% ± 5% RH or 30 ± 2°C/65RH ± 5% RH for 12 months Intermediate→ 30 ± 2°C/65% ± 5% RH for 6 months Accelerated → 40 ± 2°C/75% ± 5% RH for 6 months
  • 11. Stability studies under high humidity conditions The presence of high humidity conditions some drugs tend to hydrolyse Some tend to react with other excipients Some drugs tend to oxidize. • During stability study the drug is exposed to different relative humidity conditions • Controlled humidity conditions may be obtained by using laboratory desiccators. Application To find the material is to be protected/ stored in a controlled low humidity environment  Formulation planning Eg. An aqueous based granulation system is to be avoided or not.
  • 12. Photolytic stability • Many drug will fade / darken on exposure to light. • The extent of degradation depends on the exposed surface area • Can be overcome→ protection of the drug using an amber coloured container / a photo stable dye in the system/dark place/physical barriers • For confirmatory studies, • Samples are exposed to light providing an overall illumination of • Not less than 1.2 million lux hours and an integrated near ultraviolet energy of not less than 200 watt hours/square meter . • Samples may be exposed side-by-side with a validated chemical actinometric system.
  • 13. Stability to oxidation • Testing its stability in an atmosphere of high oxygen tension usually at 40% oxygen atmosphere. • Results are compared against a standard stored under the inert or ambient conditions. Application of test for Sensitivity to oxygen • To decide atmospheric conditions for product packing • To Include an anti-oxidant in the formulation Stability to pH • The pH stability profile data helps in predicting solid state stability of a drug in the presence of acidic and basic impurities.
  • 14. SOLUTION PHASE STABILITY • Why solution phase stability is required ? Stability of the drug from pH ranging from 1 to 8 is to be investigated To assure that the substance does not degrade when exposed to GI fluids. It is important for the selection of granulation solvent and the drying conditions.
  • 15. Developing a Profile of the Active Pharmaceutical Ingredient When preliminary pre-formulation study assures the solubility/ stability of compound The best (optimum) molecular form of a drug has been selected Physicochemical characterization begins Following parameters are to be studied further Fundamental Properties • Physical description/Organoleptic properties • Analytical methods, Purity • Partition coefficient, ionization constant • Crystal properties and polymorphism • Dissolution, Permeation across the membrane Derived Properties Compatibility Studies : Stability in the presence of excipients
  • 16. PHYSICAL DESCRIPTION/ORGANOLEPTIC PROPERTIES Colour, physical appearance, taste and odour The colour • attributes of a drug substance will be indicative of stability problems, • May indicate the necessity of improving the appearance by including a dye in the body or the coating of the final product. Taste • May indicate palatability problems • Excipients and flavours may also be used to obtain desired taste. Odour • Is indicative of degradation products ( Aspirin hydrolysis imparts odour of acetic acid). • Also may indicate the need of flavours and excipients in the formulations for required odour.
  • 17. ANALYTICAL METHODS: UV SPECTROSCOPY • The first requirement , the development of a simple analytical method for quantitative estimation in subsequent steps. • Most of drugs have aromatic rings and/or double bonds as part of their structure and absorb light in UV range. • UV spectroscopy being a fairly accurate and simple estimation technique • The absorption Co-efficient (E) of the drug can be determined by the formula: E = AF / X A=Absorbance, F = dilution factor, X = weight of drug (mg) • It is now possible to determine concentration of drug in any solution by measuring absorbance C = AF/E mg/ ml
  • 18. Purity • The determination of the purity and the data will help further studies to be carried out safely. • All the impurities present in the compound should be within the range specified. • Impurities may affect the stability of the compound and also the appearance of the compound. • Some impurities may make the compounds toxic. • The techniques used in the purity studies are TLC, HPTLC, paper chromatography, HPLC, XRD and GC.
  • 19. Dissolution • Dissolution precedes absorption • The dissolution behaviour should be investigated • To make necessary changes to enhance the dissolution rate /to select an optimum form for its development.
  • 20. Dissolution rate and Noyes-Nernst equation dW/dt = dissolution rate A = surface area of the dissolving solid D=diffusion coefficient V= volume of the medium, h = thickness of the diffusion layer Cs =concentration of solute in diffusion layer, C =solute concentration in the bulk medium
  • 21. Factors affecting dissolution rate Physicochemical properties like • Crystal habit, • Particle size, • Surface area, • Solubility, • Wetting properties, • Hydration/solvation Extrinsic factors like • Test apparatus, • rpm, • Viscosity, • pH, • Flow rate, • Temperature
  • 22. The intrinsic dissolution rate (IDR) • The dissolution rate of a pure active substance, where the conditions of surface area, temperature, agitation, and medium pH and ionic strength are all constant. • Using a specific device for this purpose, where the compressed drug is exposed in a dissolution medium over a constant surface area, and its value is expressed in mg cm-2 s-1. • IDR data helps to obtain the chemical purity and equivalence of drugs from different sources.
  • 23. Parameters Affecting Absorption The absorption of drugs consists of 2 processes; The dissolution of the drug molecules Its transport across the GI/biological membrane into the systemic circulation. For the relatively soluble compounds, the rate determining step is the permeation across the membrane For the relatively insoluble compounds, the rate determining step is the rate of dissolution. The three main parameters that influence the rate of absorption are partition coefficient, ionization constant and the permeation across the membrane.
  • 24. Partition coefficient • Partition coefficient→ the ratio of the concentration of the drug in the oil phase to that in the aqueous phase. • n-octanol is used as the oil phase / water as the aqueous phase • Other organic solvents→ chloroform, ether, amyl acetate etc. Method • Known amount of drug + two phases → equilibrating, separation of the phases, analysis of drug
  • 25. Partition coefficient Partition Coefficient(P) = [Organic] / [Aqueous] • Log P= log10 (Partition Coefficient) Log P = 1 → 10:1 Organic: Aqueous Log P = 0 → 1:1 Organic: Aqueous Log P = -1 → 1:10 Organic: Aqueous
  • 26. Ionization constant • Most drugs are weak acids or bases , • They exist as ionized or unionized species based on the pH of the medium. • Unionized species are easily absorbed as they are lipid soluble. The pH partition theory includes three principles 1. The pH as the site of absorption, 2. Ionization constant 3. Lipid solubility of the drug
  • 27. The relative concentration of the ionized and the unionized form Henderson Hassel Bach equation pH = pKa + log [unionized form] / [Ionized form] FOR BASES pH = pKa + log [ionized form]/ [unionized form] FOR ACIDS Ratio can be determined • Potentiometric pH-Titration, • pH-Spectrophotometry Method, • pH-Solubility Analysis.
  • 28. Permeation across the membrane • in vitro experiments using biological membranes. • The method used is the everted rat gut method. • This technique determines the degree & rate of passage of drug through the membrane sac by passive & active transport.
  • 29. Crystal properties and polymorphism • Drug can exist in more than one crystalline from with different space lattice arrangements → Polymorphism • Pre-formulation activity → Study on Crystal structure, polymorphism, and solvate form Changes in crystal characteristics can influence bioavailability chemical and physical stability in dosage form process functions like flow and compaction behaviours in tablet dosage form Techniques are used to determine crystal properties • Hot stage microscopy, thermal analysis, infrared spectroscopy, and X- ray diffraction.
  • 30. Derived Properties • Derived pre-formulation properties are carried out • to learn about the issues related to development of a particular dosage form • like solid oral, liquid oral or parenteral.
  • 31. Derived properties for solid dosage form • Particle size, shape and surface area • Powder Flow Properties • Density • Hygroscopicity • Compactibilty and compressibility • Wettability (for Suspension also)
  • 32. Excipient selection • Chemical structure of the API • Its physicochemical characteristics • The type of delivery system required • The proposed manufacturing process.
  • 33. Compatibility studies • Compatibility studies are usually the last activity • Studying the interactions of drug substance with other excipients Need of compatibility study • for careful selection of the excipients • To facilitate administration • To promote the consistent release and Bioavailability of the drug • To protect it from degradation.
  • 34. Methods used to study DEC • DSC- Differential Scanning Calorimetry • DTA- Differential Thermal Analysis, • FT-IR Spectroscopy, • DRS-Diffuse Reflectance Spectroscopy, • TLC-Thin Layer Chromatography, • HPLC-High Pressure Liquid Chromatography, • XRD
  • 35. Characteristics of Powder XRD and its interpretations • Results of the PXRD procedure are commonly presented as • Peak positions at 2θ and X-ray counts (intensity) • in the form of a table or a x-y plot, • known as diffractogram.
  • 36. Characteristics of Powder XRD and its interpretations • It is reliable and powerful tool for crystalline sample identification. • It is a non-destructive technique. • Each crystalline substance has a unique X-ray diffraction pattern.
  • 37. Crystal structure • Crystal structure is a description of the ordered arrangement of atoms, ions or molecules in a crystalline material. • Crystal lattice is the periodic and systematic arrangement of atoms. • The smallest portion of a crystal lattice is called Unit Cell.
  • 38. Crystal structure and X-RAY diffraction pattern • The crystallographic planes are geometric planes linking atoms/ions/molecules in crystal lattice. • Given any plane in a lattice, there is an infinite set of parallel lattice planes (family of planes) that are equally spaced (d value) from each other. • More the number of planes in given family greater is the intensity of peaks
  • 39. X-Ray diffraction pattern • Higher the intensity greater the crystallinity • Their widths are rather dependent on particle size (overly small particles will result in line broadening) i.e. broad nature of peak indicates higher degree of amorphousness or less crystalline in comparison with other samples • The number of observed peaks is related to the symmetry of the unit cell (higher symmetry generally means fewer peaks).
  • 40. DIFFERENTIAL SCANNING CALORIMETRY (DSC) • DSC is a technique in which the difference in energy inputs into a substance and a reference material is measured as a function of temperature while the substance and reference material are subjected to a controlled temperature program. • The graph of heat flow in mJ/s on the Y-axis plotted versus temperature at a fixed rate of change of temperature in °C on the X-axis shows the output of the DSC.
  • 41. Application and Interpretation of DSC curves • To check the Purity , • For polymorph identification, • To check decomposition
  • 42. • Determination of melting point • The enthalpy (Heat of fusion)
  • 44. FTIR spectra • The Functional Group Region (4000-1500 cm-1) • The Fingerprint Region (1500-400 cm-1)
  • 45. Characteristics of IR spectra and its interpretation • Used as a supplementary technique to investigate the DEC and to confirm the results obtained by the thermal analysis. • The appearances of new absorption band, broadening of band, and alteration in intensity are the main characteristics to evidence DEC. • IR is most useful in providing information about the presence or absence of specific functional groups. • Different bonds have diff. frequencies Eg; C-C, C=C, C ≡ C, C-O, O-H, N-H • IR does not provide detailed information or proof of molecular formula or structure. • Hydrogen bonding (Physical interaction) and shift in IR peaks: The number and strength of hydrogen bonds differs with chemical environment. The force constant varies and the wavenumber differs at which these molecules absorb infrared light. The number and strength of intermolecular interactions varies greatly within the sample, causing the bands in these samples to be particularly broad.