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Polymorphism in Organic Chemistry: Methods and Applications

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bharath krishna

Polymorphism is the ability of a solid material to exist in two or more crystalline forms. The document discusses the different types of polymorphism, factors that influence polymorphism, and methods to identify and produce polymorphs. It also outlines several applications of polymorphism in pharmaceuticals and organic chemistry. Specifically, selecting the right polymorph is important for drug stability, solubility, and bioavailability.

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Polymorphism in organic chemistry
CONTENT 6. Methods to identify polymorphism 5.methods of polymorphism 9. Conclusion 10. Reference 8.Pharmacetiucal application 2. Need to study polymorphism 1. Intro 4.types of polymorphism 3.Properties of polymorphism 8. Polymorphism of organic chemistry 7. Applications
Introduction The term polymorph has been derived from Greek word "poly" which means "many" and "morph" implying "form". Hence, polymorphism refers to different structural forms of a chemical substance. It is defind as the ability of a solid material to exist in two or more crystalline forms with different arrangements or conformations in the crystal lattice. Polymorphism can potentially be found in any crystalline material including polymers, minerals, and metals, and is related to allotropy, which refers to chemical elements. The complete morphology of a material is described by polymorphism and other variables such as crystal habit, amorphous fraction or crystallographic defects. Polymorphism is relevant to the fields of pharmaceutics. agrochemicals, pigments, dyestuffs, foods and explosives.
More than 50% of active pharmaceutical ingredients (APIs) are estimated to have more than one polymorphic form. Polymorphism and pseudomorphism are very common amongst drugs and are responsible for differences in many properties. The first observation of polymorphism is attributed to Friedrich Wohler and Justus Von Liebig, in 1832. He was examining a boiling solution of organic solid benzamide. During cooling, initially the benzamide is crystallized in the form of silky needles but on standing they were slowly transformed or replaced into another form like rhombic crystals. The different crystal types are the result of hydration or salvation, in pseudo polymorphism. Glycine is example for organic polymorph and is able to form mono clinic and hexagonal crystals
Silica is the example for polymorphism and it forms many polymorphs such as a quartz, ß-quartz, tridymite, cristobalite, coesite, and stishovite. A classic example for polymorph are the minerals calcite and agagonite, both forms of calcium carbonate. Polymorphism is exhibited in diamonds and graphite. Both diamond and graphite are polymorphs of the same element carbon. Both the elements entirely consist of carbon but they have different crystalline structures and physical properties, since the structure determines the properties of the compounds
Need to study polymorphism  Depending upon their relative stability, one of the several polymorphic form will be physically more stable than others.  Stable polymorph represents the lowest energy state, has highest melting point and least aqueous solubility.  Metastable form represent the higher energy state, have lower melting point and high aqueous solubility.  Metastable form converted to the stable form due to their higher energy state.  Metastable form shows better bioavailability and therefore preferred in formulations.
 Only 10% of the pharmaceuticals are present in their metastable form.  The effect of polymorphism on bioavilability is the most important consequencefor drug substaces if the bioavailability is mediated via dissolution.  The example is chloramphenicol palmitate. Other like novobiocin, griseofulvine, carbanazepine, aspirin and ampiciline.  The polymorphism of the excipients may also play an important role in bioavailability.  latest example: HYDOISOINDOLIN
Stability characteristics  Stable form  Meta form  Solubility ratio- solubility of metastable form/ solubility of stable form  Stable form having least aqueous solubility.  Meta form having high aqueous solubility. Depending upon relative stability there are two form of polymorphs::
Dissolution behavior of polymorphs  Order of dissolution rate: amorphous>metastab le>stable.  As the thermodynamic activity of polymorph is lower there is lower apparent solubility and thus absorption is also less. Among which dissolution rate is one of the most important. The abosrption rate and bioavailability of drug administered orally is controlled by many factor. Behaviour
Polymorphs shows the same properties in the liquid or gaseous state but they behave differently in solid state.  Vapour pressure  Solubility and dissolution rate  Hygroscopicity  Stability  Cryastal habit  Optical and electrical property  Melting and sublimation temperature Properties of polymorphism
Types of polymorphism 02  Enantiotropic polymorph  Eg:Sulfur 01  Monotropic polymorph  Eg:Glyceryl stearate  Monotrophs only one polymorph is stable at all temperature below the melting point, with all other polymorph being unstable.  Enantitrophs: if one form stable over certain pressure and temperature range. while the other polymorph is stable over different pressure and temperature range.
Factors affecting polymorphism  Effect of sovent  gamma-unstable  Effect of grinding  Photostability  Temperature and humidity  Effect of tablet compression
METHOD OF POLYMORPH PREPARATION  Solvent evaporation method  Slow cooling approach  Vapour diffusion method  Solvent diffusion technique  Vaccum sublimation
1. Solvent evaporation method (Rota Evaporation) : In this approach, the saturated solution of the drug is prepared in an appropriate solvent and the solvent is removed by rotatory evaporation. Air drying at various temperatures, can also be employed to obtain different potential polymorphs. 2. Slow cooling approach: This technique is frequently employed for the polymorphic forms of less soluble drugs in the solvent systems having boiling point range of 30 to 90°C. In brief, the solute is heated in the solvent just above the boiling point of the latter to produce the saturated solution. This solution is transferred to a stoppered tube and is connected to a Dewar flask containing water at a temperature just below the boiling point of the solvent. The Dewar flask is left in these conditions for several days. This technique may further be improved to obtain better crystal forms using different solvent mixtures of different polarities. Variation in the solvent composition may inhibit or promote growth of particular crystal faces and hence, can yield crystals of the desired morphology. This approach is also called the solution growth approach. 3. Solvent diffusion technique : This method is employed when the amount of drug available is less, and the drug is sensitive to air and/or solvent(s). In this option, the solution is placed in a sample tube; subsequently a less dense solvent is carefully dripped down the sides of the tube using either a pipette or a syringe to form a discreet layer.
4. Vapor diffusion method : This method is analogous to the previous one and is also applicable for the less quantities of the sample. In this case, the concentrated drug solution (0.5 µL to approximately 20 µL) is placed as a drop hanging on the underside of a microscope cover slip. The cover slip with the hanging drop is sealed with silicon oil over a solution (approx. 1 mL; reservoir) containing high concentration of precipitant. Due to higher precipitant concentration, the latter has lower vapor pressure than the drug solution. This results in diffusion of the solvent from the drop towards the reservoir and subsequent crystallization of the API within hours to weeks.
Methods to identify polymorphism Hot stage microscopy Optical crystallography Differential thermal analysis (DTB) X-ray diffraction method Differential scanning calorimetric (DSC) Thermo gravimetric analysis (TGA)
 Used in the identification of polymorphs crystal exist in isotropic and anisotropic form.  Isotropic examine the velocity of light is same in all direction.  Anisotropic crystal have 2 or 3 different light velocity or refractive indices.  Video recording system and polarizing microscope fitted during according to heating and cooling stage for investigating polymorph. Hot stage microscopy  Fluid stage transformation as a function of temperature is observed.  Silicon oil stage microscopy is used for detection of pseudopolymorph X-ray diffraction method  It provide the most complete information about solid state.  This method is based on the scattering of x-ray by crystal. Optical crystallography
Thermo gravimetric analysis  Is a type of testing that is performed on samples to determine changes in weight in relation to change in temperature.  Such analysis relies on a high degree of precision in measurements; weight and temperature changes.  As many weight loss similar, the weight loss curve may require transformation before results may be interpreted.
Applications  The knowledge of solid-state properties in an early stage of development helps to avoid manufacturing problems, to fine tune the performance of drugs and provides space for innovations.  E,g.- Famotidine which is an excellent histamine  H2 receptor antagonist is also found to exist in two different polymorphic forms, metastable polymorph B and stable polymorph A.  For improvement of therapeutic activity of drug.  To prevent loss of raw material.  • For better bioavailability of drug.
 Pharmaceutical application of polymorphs  Suspension : In preparation of suspension use of a wrong polymorph of a drug, a phase conversion from the metastable to stable polymorph may occur. This results in crystal growth and caking of suspension. Eg: cortisone acetate was one of the most difficult polymorphic problems to solve. Macek obtained the first patent on stable noncaking aqueous suspension of cortisone acetate and methods of preparing the same. He describe the early attempts to obtain a stable aqueous suspension, where cortisone acetate, in the form of crystals stable in the dry state, was suspended in the aqueous medium and allowed to remain in the medium for a few hours. It was observed that crystals growth of the cortisone acetate invariably occurred with subsequent caking and sedimentation. A physically stable aqueous suspension was obtained by ball-milling cortisone acetate powder, in the aqueous vehicle where a polymorphic phase transition occurred. In a later patent, Magerlein described two new polymorphs of cortisone acetate, Form A ,which is not stable in the dry state, and Form B, which is stable in the dry state. Both crystal forms when used in aqueous suspensions gave physically stable, noncaking aqueous suspension.
Creams: When creams are prepared with the active ingredient suspended in the cream base. use of the wrong polymorph can result in a phase inversion to a more stable phase. As a consequence, crystal growth can occur in the vehicle yielding gritty, cosmetically unacceptable creams or products in which the active ingredient is unevenly distributed. During the preparation of a topical cream it is necessary to select the correct polymorph of the active ingredient, which when suspended is least susceptible to growth in the cream base. Solution: Flynn has reported some problem in the formulation of a parenteral solution of a drug. In this instance, determination of the water solubility of the compound indicated the drug to be adequately soluble for the concentration required in the formulation. Stability studies on the formulation quickly turned up the presence of a precipitate. An investigation of the problem showed the precipitate to consist of a less soluble polymorph of the compound. The problem was solved by formulating the product a vehicle containing sufficient cosolvent to solubilize the less soluble polymorphic form.
 Polymorphism in organic chemistry Active pharmaceutical ingredients (APIS), frequently delivered to the patient in the solid-state as part of an approved dosage form, can exist in such diverse solid forms as polymorphs, pseudopolymorphs, salts, co-crystals and amorphous solids. Various solid forms often display different mechanical, thermal, physical and chemical properties that can remarkably influence the bioavailability, hygroscopicity, stability and other performance characteristics of the drug. Hence, a thorough understanding of the relationship between the particular solid form of an active pharmaceutical ingredient (API) and its functional properties is important in selecting the most suitable form of the API for development into a drug product. In past decades, there have been significant efforts on the discovery, selection and control of the solid forms of APIs and bulk drugs. This contribution discusses the thermodynamics and kinetics of polymorphic systems, the characterization of polymorphs, and the transformation between polymorphs.
 Conclusion  In the present era of evolving understanding, it is accepted that not merely chemical purity/integrity of the API is the sole dependable and formulation influential parameter. The physical arrangements of the constituents in the crystal lattice have immense potential to influence the physicochemical properties of the drugs and subsequently the therapeutic outcomes. Therefore, the study of polymorphic forms has become as important as any other branch of pharmaceutical sciences, as the former helps to embark upon the proper API/excipient form selection.  with the foregoing discussion, it is clear that probably every organic medicinal can exist in different polymorphs and the choice of the proper polymorph will determine if a pharmaceutical preparation will be chemically or physically stable, or if a powder will tablet or not tablet well, or if the blood level obtained will be the therapeutic level to give the pharmacologic response desired. Thus, it is time that pharmaceutical companies, as a part of their pre- formulation studies, identify and study the stability of different polymorphs of each potential new drug, as they do the melting points or other physical characteristics.
 REFERENCES  Karpinski PH. Polymorphism of active pharmaceutical ingredients. ChemEng Technol. 2006; doi: 10.1002/ceat.200500397.  Chawla G, Bansal AK. Challenges in polymorphism of pharmaceuticals. CRIPS. 2004. . The theory and practice of industrial pharmacy by - Leon Lechman, Joseph L Kanig.  Biopharmaceutics and pharmacokinetics by- DM Bhramankar, Sunil Jaiswal.  Physical pharmacy by- Alfred Martine. Sun C. Grant DJW. Influence of crystal structure on the tableting properties of sulfamerazine polymorphs. Pharm Res. 2001; 18(3):274-80.  Eyjolfsson R. Enalapril maleate polymorphs: instability of form II in a blet formulation. Phamazie. 2002; 57(5):347–48.  Schmidt AC, Senfter N, Griesser UJ. Crystal polymorphism of local anaesthetic drugs. J Therm Anal Calorim. 2003: 73:397-404.
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Polymorphism in Organic Chemistry: Methods and Applications

  • 2. CONTENT 6. Methods to identify polymorphism 5.methods of polymorphism 9. Conclusion 10. Reference 8.Pharmacetiucal application 2. Need to study polymorphism 1. Intro 4.types of polymorphism 3.Properties of polymorphism 8. Polymorphism of organic chemistry 7. Applications
  • 3. Introduction The term polymorph has been derived from Greek word "poly" which means "many" and "morph" implying "form". Hence, polymorphism refers to different structural forms of a chemical substance. It is defind as the ability of a solid material to exist in two or more crystalline forms with different arrangements or conformations in the crystal lattice. Polymorphism can potentially be found in any crystalline material including polymers, minerals, and metals, and is related to allotropy, which refers to chemical elements. The complete morphology of a material is described by polymorphism and other variables such as crystal habit, amorphous fraction or crystallographic defects. Polymorphism is relevant to the fields of pharmaceutics. agrochemicals, pigments, dyestuffs, foods and explosives.
  • 4. More than 50% of active pharmaceutical ingredients (APIs) are estimated to have more than one polymorphic form. Polymorphism and pseudomorphism are very common amongst drugs and are responsible for differences in many properties. The first observation of polymorphism is attributed to Friedrich Wohler and Justus Von Liebig, in 1832. He was examining a boiling solution of organic solid benzamide. During cooling, initially the benzamide is crystallized in the form of silky needles but on standing they were slowly transformed or replaced into another form like rhombic crystals. The different crystal types are the result of hydration or salvation, in pseudo polymorphism. Glycine is example for organic polymorph and is able to form mono clinic and hexagonal crystals
  • 5. Silica is the example for polymorphism and it forms many polymorphs such as a quartz, ß-quartz, tridymite, cristobalite, coesite, and stishovite. A classic example for polymorph are the minerals calcite and agagonite, both forms of calcium carbonate. Polymorphism is exhibited in diamonds and graphite. Both diamond and graphite are polymorphs of the same element carbon. Both the elements entirely consist of carbon but they have different crystalline structures and physical properties, since the structure determines the properties of the compounds
  • 6. Need to study polymorphism  Depending upon their relative stability, one of the several polymorphic form will be physically more stable than others.  Stable polymorph represents the lowest energy state, has highest melting point and least aqueous solubility.  Metastable form represent the higher energy state, have lower melting point and high aqueous solubility.  Metastable form converted to the stable form due to their higher energy state.  Metastable form shows better bioavailability and therefore preferred in formulations.
  • 7.  Only 10% of the pharmaceuticals are present in their metastable form.  The effect of polymorphism on bioavilability is the most important consequencefor drug substaces if the bioavailability is mediated via dissolution.  The example is chloramphenicol palmitate. Other like novobiocin, griseofulvine, carbanazepine, aspirin and ampiciline.  The polymorphism of the excipients may also play an important role in bioavailability.  latest example: HYDOISOINDOLIN
  • 8. Stability characteristics  Stable form  Meta form  Solubility ratio- solubility of metastable form/ solubility of stable form  Stable form having least aqueous solubility.  Meta form having high aqueous solubility. Depending upon relative stability there are two form of polymorphs::
  • 9. Dissolution behavior of polymorphs  Order of dissolution rate: amorphous>metastab le>stable.  As the thermodynamic activity of polymorph is lower there is lower apparent solubility and thus absorption is also less. Among which dissolution rate is one of the most important. The abosrption rate and bioavailability of drug administered orally is controlled by many factor. Behaviour
  • 10. Polymorphs shows the same properties in the liquid or gaseous state but they behave differently in solid state.  Vapour pressure  Solubility and dissolution rate  Hygroscopicity  Stability  Cryastal habit  Optical and electrical property  Melting and sublimation temperature Properties of polymorphism
  • 11. Types of polymorphism 02  Enantiotropic polymorph  Eg:Sulfur 01  Monotropic polymorph  Eg:Glyceryl stearate  Monotrophs only one polymorph is stable at all temperature below the melting point, with all other polymorph being unstable.  Enantitrophs: if one form stable over certain pressure and temperature range. while the other polymorph is stable over different pressure and temperature range.
  • 12.
  • 13. Factors affecting polymorphism  Effect of sovent  gamma-unstable  Effect of grinding  Photostability  Temperature and humidity  Effect of tablet compression
  • 14. METHOD OF POLYMORPH PREPARATION  Solvent evaporation method  Slow cooling approach  Vapour diffusion method  Solvent diffusion technique  Vaccum sublimation
  • 15. 1. Solvent evaporation method (Rota Evaporation) : In this approach, the saturated solution of the drug is prepared in an appropriate solvent and the solvent is removed by rotatory evaporation. Air drying at various temperatures, can also be employed to obtain different potential polymorphs. 2. Slow cooling approach: This technique is frequently employed for the polymorphic forms of less soluble drugs in the solvent systems having boiling point range of 30 to 90°C. In brief, the solute is heated in the solvent just above the boiling point of the latter to produce the saturated solution. This solution is transferred to a stoppered tube and is connected to a Dewar flask containing water at a temperature just below the boiling point of the solvent. The Dewar flask is left in these conditions for several days. This technique may further be improved to obtain better crystal forms using different solvent mixtures of different polarities. Variation in the solvent composition may inhibit or promote growth of particular crystal faces and hence, can yield crystals of the desired morphology. This approach is also called the solution growth approach. 3. Solvent diffusion technique : This method is employed when the amount of drug available is less, and the drug is sensitive to air and/or solvent(s). In this option, the solution is placed in a sample tube; subsequently a less dense solvent is carefully dripped down the sides of the tube using either a pipette or a syringe to form a discreet layer.
  • 16. 4. Vapor diffusion method : This method is analogous to the previous one and is also applicable for the less quantities of the sample. In this case, the concentrated drug solution (0.5 µL to approximately 20 µL) is placed as a drop hanging on the underside of a microscope cover slip. The cover slip with the hanging drop is sealed with silicon oil over a solution (approx. 1 mL; reservoir) containing high concentration of precipitant. Due to higher precipitant concentration, the latter has lower vapor pressure than the drug solution. This results in diffusion of the solvent from the drop towards the reservoir and subsequent crystallization of the API within hours to weeks.
  • 17. Methods to identify polymorphism Hot stage microscopy Optical crystallography Differential thermal analysis (DTB) X-ray diffraction method Differential scanning calorimetric (DSC) Thermo gravimetric analysis (TGA)
  • 18.  Used in the identification of polymorphs crystal exist in isotropic and anisotropic form.  Isotropic examine the velocity of light is same in all direction.  Anisotropic crystal have 2 or 3 different light velocity or refractive indices.  Video recording system and polarizing microscope fitted during according to heating and cooling stage for investigating polymorph. Hot stage microscopy  Fluid stage transformation as a function of temperature is observed.  Silicon oil stage microscopy is used for detection of pseudopolymorph X-ray diffraction method  It provide the most complete information about solid state.  This method is based on the scattering of x-ray by crystal. Optical crystallography
  • 19. Thermo gravimetric analysis  Is a type of testing that is performed on samples to determine changes in weight in relation to change in temperature.  Such analysis relies on a high degree of precision in measurements; weight and temperature changes.  As many weight loss similar, the weight loss curve may require transformation before results may be interpreted.
  • 20. Applications  The knowledge of solid-state properties in an early stage of development helps to avoid manufacturing problems, to fine tune the performance of drugs and provides space for innovations.  E,g.- Famotidine which is an excellent histamine  H2 receptor antagonist is also found to exist in two different polymorphic forms, metastable polymorph B and stable polymorph A.  For improvement of therapeutic activity of drug.  To prevent loss of raw material.  • For better bioavailability of drug.
  • 21.  Pharmaceutical application of polymorphs  Suspension : In preparation of suspension use of a wrong polymorph of a drug, a phase conversion from the metastable to stable polymorph may occur. This results in crystal growth and caking of suspension. Eg: cortisone acetate was one of the most difficult polymorphic problems to solve. Macek obtained the first patent on stable noncaking aqueous suspension of cortisone acetate and methods of preparing the same. He describe the early attempts to obtain a stable aqueous suspension, where cortisone acetate, in the form of crystals stable in the dry state, was suspended in the aqueous medium and allowed to remain in the medium for a few hours. It was observed that crystals growth of the cortisone acetate invariably occurred with subsequent caking and sedimentation. A physically stable aqueous suspension was obtained by ball-milling cortisone acetate powder, in the aqueous vehicle where a polymorphic phase transition occurred. In a later patent, Magerlein described two new polymorphs of cortisone acetate, Form A ,which is not stable in the dry state, and Form B, which is stable in the dry state. Both crystal forms when used in aqueous suspensions gave physically stable, noncaking aqueous suspension.
  • 22. Creams: When creams are prepared with the active ingredient suspended in the cream base. use of the wrong polymorph can result in a phase inversion to a more stable phase. As a consequence, crystal growth can occur in the vehicle yielding gritty, cosmetically unacceptable creams or products in which the active ingredient is unevenly distributed. During the preparation of a topical cream it is necessary to select the correct polymorph of the active ingredient, which when suspended is least susceptible to growth in the cream base. Solution: Flynn has reported some problem in the formulation of a parenteral solution of a drug. In this instance, determination of the water solubility of the compound indicated the drug to be adequately soluble for the concentration required in the formulation. Stability studies on the formulation quickly turned up the presence of a precipitate. An investigation of the problem showed the precipitate to consist of a less soluble polymorph of the compound. The problem was solved by formulating the product a vehicle containing sufficient cosolvent to solubilize the less soluble polymorphic form.
  • 23.  Polymorphism in organic chemistry Active pharmaceutical ingredients (APIS), frequently delivered to the patient in the solid-state as part of an approved dosage form, can exist in such diverse solid forms as polymorphs, pseudopolymorphs, salts, co-crystals and amorphous solids. Various solid forms often display different mechanical, thermal, physical and chemical properties that can remarkably influence the bioavailability, hygroscopicity, stability and other performance characteristics of the drug. Hence, a thorough understanding of the relationship between the particular solid form of an active pharmaceutical ingredient (API) and its functional properties is important in selecting the most suitable form of the API for development into a drug product. In past decades, there have been significant efforts on the discovery, selection and control of the solid forms of APIs and bulk drugs. This contribution discusses the thermodynamics and kinetics of polymorphic systems, the characterization of polymorphs, and the transformation between polymorphs.
  • 24.  Conclusion  In the present era of evolving understanding, it is accepted that not merely chemical purity/integrity of the API is the sole dependable and formulation influential parameter. The physical arrangements of the constituents in the crystal lattice have immense potential to influence the physicochemical properties of the drugs and subsequently the therapeutic outcomes. Therefore, the study of polymorphic forms has become as important as any other branch of pharmaceutical sciences, as the former helps to embark upon the proper API/excipient form selection.  with the foregoing discussion, it is clear that probably every organic medicinal can exist in different polymorphs and the choice of the proper polymorph will determine if a pharmaceutical preparation will be chemically or physically stable, or if a powder will tablet or not tablet well, or if the blood level obtained will be the therapeutic level to give the pharmacologic response desired. Thus, it is time that pharmaceutical companies, as a part of their pre- formulation studies, identify and study the stability of different polymorphs of each potential new drug, as they do the melting points or other physical characteristics.
  • 25.  REFERENCES  Karpinski PH. Polymorphism of active pharmaceutical ingredients. ChemEng Technol. 2006; doi: 10.1002/ceat.200500397.  Chawla G, Bansal AK. Challenges in polymorphism of pharmaceuticals. CRIPS. 2004. . The theory and practice of industrial pharmacy by - Leon Lechman, Joseph L Kanig.  Biopharmaceutics and pharmacokinetics by- DM Bhramankar, Sunil Jaiswal.  Physical pharmacy by- Alfred Martine. Sun C. Grant DJW. Influence of crystal structure on the tableting properties of sulfamerazine polymorphs. Pharm Res. 2001; 18(3):274-80.  Eyjolfsson R. Enalapril maleate polymorphs: instability of form II in a blet formulation. Phamazie. 2002; 57(5):347–48.  Schmidt AC, Senfter N, Griesser UJ. Crystal polymorphism of local anaesthetic drugs. J Therm Anal Calorim. 2003: 73:397-404.