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MALLA REDDY COLLEGE OF PHARMACY Maisammaguda, Dhulapally (post via Hakimpet), Sec-bad-14 SSOOLLIIDD DDIISSPPEERRSSIIOONN && CCOOMMPPLLEEXXAATTIIOONN Presented by J.Jagan (256213886013) Guided by Dr. Yasmin Begum H.O.D. Dept. of Pharmaceutics Malla Reddy College of Pharmacy
Contents * Solubility * Advantages * Importance * Solid dispersion * Types of solid Dispersion * Preparation Techniques * Complexation
Solubility * Solubility is the property of a solids, liquid or gaseous chemical substance called solute to dissolve in a solid, liquid or gaseous solvent to form a homogenous solution of the solute in the solvent. * The solubility term is defined as maximum amount of solute that can be dissolved in a given amount of solvent. The solubility of a substance fundamentally depends on the solvent used as well as temperature & pressure.
Advantages * Increased bioavailability * Fast absorption * Patient compliance * No shaking * No gritty particles are observed.
Importance * Selection of solvent for dosage form. * Information about the structure, inter molecular forces. * Selection of dissolution medium. * Separation of mixtures. * Separation of optical isomers.
Solid dispersion * The term solid dispersion refers to a group of solid products consisting of atleast two different components, generally a hydrophilic matrix and hydrophobic drug.
Introduction * The concept of solid dispersion was originally proposed by Sekiguchi & obi. * Solid dispersion represents a useful pharmaceutical technique for increasing the dissolution, absorption & therapeutic efficacy of drugs in dosage forms. * The solubility of celecoxib, halofantrine, ritonavir can be improved by solid dispersion using suitable hydrophilic carriers
Types of solid dispersion * Solid eutectic mixture. * Solid solutions. * Glass solutions & suspension. * Amorphous precipitations in crystalline carriers.
Solid Eutectic mixture * A simple eutectic mixture consists of two components which are completely miscible in liquid state but to a limited extend in solid state. * These are prepared by rapid solidification of fused melt of two components. * When a mixture of poor water soluble drug & water soluble carrier is dissolved in aqueous medium, the carrier is dissolved rapidly, releasing very fine crystal of drug.
Glass solution & suspension * A glass is a homogenous glassy system in which solute dissolves in the glassy system. * A glass suspension refers to a mixture in which precipitated particles are suspended in a glassy solvent. * Characterization of glassy state is transparency & brittleness below the glass transition temperature.
Solid solution * In a solid solution, the two components crystallize together in a homogenous one phase system. * In continuous solid solution, the two components are miscible in the solid state in all proportions. * In discontinuous solid solutions, the solubility of each of the components in the other component is limited.
Amorphous precipitations in crystalline carrier * In the group of dispersions drug is precipitated out in amorphous form while in simple eutectic mixture is in crystalline form. * Example : sulphathiazole in crystalline urea.
Preparation techniques * Holt-melt method (fusion method ) * Solvent evaporation method * Holt melt extrusion * Kneading method
Hot melt method * In this method, the physical mixture of a drug & water soluble carrier was heated directly until it melted. * The melted mixture was the cooled & solidified rapidly in an ice-bath under vigorous stirring.. * The final solid mass was crushed, pulverized & sieved, which can be compressed into tablets with the help of tableting agents. * Advantages: Simplicity economy
Solvent evaporation method * Tachibana & Nakumara were the first to dissolve both the drug & the carrier in a common solvent and then evaporate the solvent under vacuum to produce a solid solution. * This enabled them to produce a solid solution of the highly lipophillic β-carotene in the highly water soluble carrier polyvinylpyrolidone. Advantages: * Thermal decomposition of drugs are carriers can be prevented because of the low temperature required for the evaporation of organic solvents. Disadvantage: * High cost of preparation * Difficulty in completely removing liquid solvent
Hot-melt extrusion * Holt-melt extrusion is essentially the same as the fusion method except that intense mixing of the components is induced by extruder. * Just like in the traditional fusion process, miscibility of drug and matrix can be a problem. * High shear forces resulting in high local temperature in the extruder is a problem for heat sensitive materials.
Kneading method * Drug & carrier weighed , they are mixed together, use motor & pestle to reduce the size of the both drug & carrier. * Water-methanol mixture 3:1 ratio was added to the above mixture . The solution was mixed well and slurry was collected by filtration and dried in hot-air oven for 2hrs at 500C * Then dried mass was collected further dried in desiccated for 12hrs. * Then the solid dispersion passed to sieve no:80 to obtained uniform particle size.
Complexation * The complex may be considered as a species of definite substrate to ligand stoichiometry which can be formed in an equilibrium process in solution and also may exists in solid state. Advantages: * To enhance the aqueous solubility * Drug stability
Inclusion complexes * Lipophilic drug –cyclodextrin complexes, commonly known as inclusion complexes. * It can be formed simply by adding the drug and excipient together, resulting in enhanced drug solubilization. * Cyclodextrins are a group of structurally related cyclic oligosaccharides that have a polar cavity and hydrophilic external surface.
* Hydrophilic cyclodextrins are non toxic in normal doses while lipophilic ones may be toxic * Hence methyl, hydroxyl propyl, sulphoalkylated and sulphated derivatives of natural cyclodextrins that posses improved aqueous are preferred for pharmacy use * Cyclodextrins an also used as membrane permeability enhancer and stabilizing agents.
Conclusion * For orally administered drugs solubility is one of the rate limiting parameter to achieve their desired concentration in systemic circulation of pharmaceutical response. * Problem of solubility is a major challenge for formulation scientist. * Increasing number of poorly water soluble drug candidates as well as improvements in solid dispersion manufacturing methods strongly favor the roll of solid dispersion in solubility enhancement of poorly water soluble drugs.
Reference: * International Journal of Pharmaceutical sciences review and Research * Remington the science and practice of pharmacy * Text book of essentials of physical pharmacy by C.V.S. Subhramanyam * www.ncbi.nlm.nih.gov
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solid dispersion

  • 1. MALLA REDDY COLLEGE OF PHARMACY Maisammaguda, Dhulapally (post via Hakimpet), Sec-bad-14 SSOOLLIIDD DDIISSPPEERRSSIIOONN && CCOOMMPPLLEEXXAATTIIOONN Presented by J.Jagan (256213886013) Guided by Dr. Yasmin Begum H.O.D. Dept. of Pharmaceutics Malla Reddy College of Pharmacy
  • 2. Contents * Solubility * Advantages * Importance * Solid dispersion * Types of solid Dispersion * Preparation Techniques * Complexation
  • 3. Solubility * Solubility is the property of a solids, liquid or gaseous chemical substance called solute to dissolve in a solid, liquid or gaseous solvent to form a homogenous solution of the solute in the solvent. * The solubility term is defined as maximum amount of solute that can be dissolved in a given amount of solvent. The solubility of a substance fundamentally depends on the solvent used as well as temperature & pressure.
  • 4. Advantages * Increased bioavailability * Fast absorption * Patient compliance * No shaking * No gritty particles are observed.
  • 5. Importance * Selection of solvent for dosage form. * Information about the structure, inter molecular forces. * Selection of dissolution medium. * Separation of mixtures. * Separation of optical isomers.
  • 6. Solid dispersion * The term solid dispersion refers to a group of solid products consisting of atleast two different components, generally a hydrophilic matrix and hydrophobic drug.
  • 7. Introduction * The concept of solid dispersion was originally proposed by Sekiguchi & obi. * Solid dispersion represents a useful pharmaceutical technique for increasing the dissolution, absorption & therapeutic efficacy of drugs in dosage forms. * The solubility of celecoxib, halofantrine, ritonavir can be improved by solid dispersion using suitable hydrophilic carriers
  • 8. Types of solid dispersion * Solid eutectic mixture. * Solid solutions. * Glass solutions & suspension. * Amorphous precipitations in crystalline carriers.
  • 9. Solid Eutectic mixture * A simple eutectic mixture consists of two components which are completely miscible in liquid state but to a limited extend in solid state. * These are prepared by rapid solidification of fused melt of two components. * When a mixture of poor water soluble drug & water soluble carrier is dissolved in aqueous medium, the carrier is dissolved rapidly, releasing very fine crystal of drug.
  • 10. Glass solution & suspension * A glass is a homogenous glassy system in which solute dissolves in the glassy system. * A glass suspension refers to a mixture in which precipitated particles are suspended in a glassy solvent. * Characterization of glassy state is transparency & brittleness below the glass transition temperature.
  • 11. Solid solution * In a solid solution, the two components crystallize together in a homogenous one phase system. * In continuous solid solution, the two components are miscible in the solid state in all proportions. * In discontinuous solid solutions, the solubility of each of the components in the other component is limited.
  • 12. Amorphous precipitations in crystalline carrier * In the group of dispersions drug is precipitated out in amorphous form while in simple eutectic mixture is in crystalline form. * Example : sulphathiazole in crystalline urea.
  • 13. Preparation techniques * Holt-melt method (fusion method ) * Solvent evaporation method * Holt melt extrusion * Kneading method
  • 14. Hot melt method * In this method, the physical mixture of a drug & water soluble carrier was heated directly until it melted. * The melted mixture was the cooled & solidified rapidly in an ice-bath under vigorous stirring.. * The final solid mass was crushed, pulverized & sieved, which can be compressed into tablets with the help of tableting agents. * Advantages: Simplicity economy
  • 15. Solvent evaporation method * Tachibana & Nakumara were the first to dissolve both the drug & the carrier in a common solvent and then evaporate the solvent under vacuum to produce a solid solution. * This enabled them to produce a solid solution of the highly lipophillic β-carotene in the highly water soluble carrier polyvinylpyrolidone. Advantages: * Thermal decomposition of drugs are carriers can be prevented because of the low temperature required for the evaporation of organic solvents. Disadvantage: * High cost of preparation * Difficulty in completely removing liquid solvent
  • 16. Hot-melt extrusion * Holt-melt extrusion is essentially the same as the fusion method except that intense mixing of the components is induced by extruder. * Just like in the traditional fusion process, miscibility of drug and matrix can be a problem. * High shear forces resulting in high local temperature in the extruder is a problem for heat sensitive materials.
  • 17. Kneading method * Drug & carrier weighed , they are mixed together, use motor & pestle to reduce the size of the both drug & carrier. * Water-methanol mixture 3:1 ratio was added to the above mixture . The solution was mixed well and slurry was collected by filtration and dried in hot-air oven for 2hrs at 500C * Then dried mass was collected further dried in desiccated for 12hrs. * Then the solid dispersion passed to sieve no:80 to obtained uniform particle size.
  • 18. Complexation * The complex may be considered as a species of definite substrate to ligand stoichiometry which can be formed in an equilibrium process in solution and also may exists in solid state. Advantages: * To enhance the aqueous solubility * Drug stability
  • 19. Inclusion complexes * Lipophilic drug –cyclodextrin complexes, commonly known as inclusion complexes. * It can be formed simply by adding the drug and excipient together, resulting in enhanced drug solubilization. * Cyclodextrins are a group of structurally related cyclic oligosaccharides that have a polar cavity and hydrophilic external surface.
  • 20. * Hydrophilic cyclodextrins are non toxic in normal doses while lipophilic ones may be toxic * Hence methyl, hydroxyl propyl, sulphoalkylated and sulphated derivatives of natural cyclodextrins that posses improved aqueous are preferred for pharmacy use * Cyclodextrins an also used as membrane permeability enhancer and stabilizing agents.
  • 21. Conclusion * For orally administered drugs solubility is one of the rate limiting parameter to achieve their desired concentration in systemic circulation of pharmaceutical response. * Problem of solubility is a major challenge for formulation scientist. * Increasing number of poorly water soluble drug candidates as well as improvements in solid dispersion manufacturing methods strongly favor the roll of solid dispersion in solubility enhancement of poorly water soluble drugs.
  • 22. Reference: * International Journal of Pharmaceutical sciences review and Research * Remington the science and practice of pharmacy * Text book of essentials of physical pharmacy by C.V.S. Subhramanyam * www.ncbi.nlm.nih.gov