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Edit Comment Close Premium member Presentation Transcript PILOT PLANT STUDY FOR LIQUID ORALS: 1 PILOT PLANT STUDY FOR LIQUID ORALS HARISH DHANASHREE I M PHARMA DEPT OF PHARMACEUTICSIntroduction:: 2 Introduction : Pilot plant is a processing system used to generate the information about behavior of the system that can be used in designing large scale unit Intermediate to laboratory and production plantPowerPoint Presentation: 3 Process scale up is an increase in batch size or production capacity, usually in response to increased product demand, concerns about high production costs, or an increased need for clinical research supplies.LIQUIDS ORALS: 4 LIQUIDS ORALS Liquid pharmaceuticals encountered in the pilot plant are defined as non sterile solutions, suspensions or emulsions. Scale of each of these present a different set of processing concerns that must be considered Liquid orals are the liquid dosage formulations containing one (or) more active ingredients with (or) without additives dissolved in a suitable vehicle, meant for oral administrationPowerPoint Presentation: 5 The physical form of a drug product that is pourable displays Newtonian or pseudoplastic flow behaviour and conforms to it’s container at room temperature. Liquid dosage forms may be dispersed systems or solutions . In dispersed systems there are two or more phases, where one phase is distributed in another. A solution refers two or more substances mixed homogeneously.TYPES OF ORAL LIQUIDS: 6 TYPES OF ORAL LIQUIDS SOLUTIONS EMULSION SUSPENSIONOBJECTIVE: 7 OBJECTIVE A formula is transformed into a viable robust product using reliable and practical method of manufacture that effects the orderly transition from lab to routine processing in a full-scale productionSTEPS INVOLVED IN PILOT PLANT FOR LIQUID ORAL: 8 STEPS INVOLVED IN PILOT PLANT FOR LIQUID ORAL Reporting responsibility Personal requirements Space requirements Review of the formula Raw materials Relevant processing equipments Production rates Process evaluation GMP consideration Transfer of analytic method to quality assuranceA pilot plant layout.: 9 A pilot plant layout.PowerPoint Presentation: 10 Raw materials Weighing & Measuring Mixing Distilled water Filling Packing Finished Product storage Quality Assurance Pilot Plant Scale-Up Techniques for liquid oralsGeneral Consideration: I. Reporting responsibilities:: 11 General Consideration: I. Reporting responsibilities: The goal of pilot plant scale is to facilitate the transfer of a product from the laboratory in to production. The formulators continue to provide support to the production even after the transition in to production has been completed. There must be good relation between pilot plant and other departments.II. Personnel requirements:: 12 II. Personnel requirements: Have good theoretic knowledge of pharmaceutics. Practical experience in liquid orals manufacturing industry. Chemical, physical, biochemical and medical properties of drugs. Have the knowledge of computer, electronics.III. Space requirements:: 13 III. Space requirements : Administration and information processing area Physical testing area Standard pilot plant equipment floor space Storage areaAdministration and information processing area: 14 Administration and information processing areaPhysical testing area: 15 Physical testing areaStandard pilot plant equipment floor space: 16 Standard pilot plant equipment floor spaceStorage area : 17 Storage areaIV Review of formula:: 18 IV Review of formula: A thorough review of each and every steps of formulation is important The purpose of each ingredient and its contribution to the final product should be studied If any modification in formula, it should be done as soon as possible in phase III trials to allow time to generate meaningful long term stability in a support of a proposed new drug applicationV. Raw materials:: 19 V. Raw materials : One responsibility of pilot plant function is the approval and validation of the active ingredient and excipients raw materials used in the pharmaceutical products. The quality of the active ingredients needs to be verified.Formulation consideration:: 20 Formulation consideration : Solvents Preservatives Antioxidants Solubilizers Organoleptic agents etc.SOLVENTS: 21 SOLVENTS Water Alcohol Glycerol Polyethylene glycol Propylene glycol.Water: 22 Water Compared to ordinary drinking water , purified water USP is more free of solid impurities. When evaporated to dryness, it must not yield greater than 0.001% of residue. Purified water is obtained by distillation, ion-exchange treatment, reverse osmosis and other relevant methodPRESERVATIVES: 23 PRESERVATIVES Preservatives are added to prevent the microbial growth Preservative are necessary due to chances of microbial growth Raw material, processing containers & equipments, the manufacturing environment, operators, packing materials & the user . Phenol, chlorocresol, benzoic acid, etc.PowerPoint Presentation: 24 Antioxidants: ascorbic acid, sodium thiosulphate, sodium metabisulphate. Solubilizers: co-solvents and surface active agents Organoleptic agents etc: colour, flavor, sweetening agentsVI. Relevant processing equipment:: 25 VI. Relevant processing equipment : Almost all formulation development work is carried out on small, relatively simple laboratory equipment. The equipment that is most economical, the simplest, the most efficient should be selected Liquid pharmaceutical processing tanks, kettles, pipes, mills, filter housings, and so forth are most frequently fabricated from stainless steel. Of the three types commonly used in the industry (304, 308, and 316), type 316 is most often used because it is the least reactive. Ease of cleaning should be considered, if multiple products are to be manufacture in the same equipment.Stages of operations: 1.Tank selection: 26 Stages of operations: 1.Tank selection Material of the tank must not be additive to the product The shape and size of equipment must be selected according to the batch size The tanks are usually constructed of polished stainless steel of different grades Teflon and glass lined tank. Adequate clean-up procedures developed.2.Mixing: 27 2.Mixing Simple mixing is essential to increase flow of liquids. If the liquid is of high viscosity, high electrical stirrer may be used. Addition of ingredients in proper order have vital important. At high viscosity the chance of air entrapment .Air entrapment Minimize:-: 28 Air entrapment Minimize :- By reducing agitator speed By caring out the mixing procedure in enclosed tank under vacuum The alternative procedure to the all is versatorVersator: 29 Versator3. Dispersion: 30 3. Dispersion Suspensions and emulsions require considerably greater shear forces Laboratory formulation is difficult to duplicate at large scale Dispersion produced by colloidal mill or an immersion homogenizer Variety of equipment should evaluated for better results. Homogenizer Colloidal mill4. Filtration and clarification—: 31 4. Filtration and clarification — Filtration procedure, requires careful evaluation to ensure that pilot scale-ups will exhibit the same degree of clarity as their laboratory counterparts. During the pilot run the clarity of the filtrate should be checked periodically, in order to establish schedule for changing pads, cake, or cartridges, depending on the type of filtration employed. In filtration, filter pads are used which is made up of asbestos and cellulose. Selection of filtration depends on The product viscosity Volumes Rate requirement 5. Transfer and filling: 32 5. Transfer and filling Filling – important parameter in the transfer of liquids from tank to tank and into containers. New batches should not be started until the previous batches are completely filled and the tanks are emptied. Bins and PipingMethods for filling of liquids:-: 33 Methods for filling of liquids:- The selection of equipment depends on characteristic of liquid such as, viscosity, type of packaging, surface tension. Gravimetric (specific weight) Volumetric (specific volume) Constant volume filling Gravimetric VolumetricContainers and closures: : 34 Containers and closures: Glass Plastic It is more important to store the final product in container until its expiration. Most oral liquids are packed in either amber or flint glass containers with plastic or metal caps.VII. Production rates:-: 35 VII. Production rates :- The immediate and future market requirements -estimating the production rates, selecting the type and the size of the equipment needed. Determining the product loss in the equipment during manufacture. The time required to clean the equipment between batches. The number of batches that will need to be tested for release.VIII. Process evaluation:-: 36 VIII. Process evaluation :- Items that should be examined include the following- Mixing speed Mixing time Rate of addition of solvents, solutions of drug, slurries etc Heating and cooling rates Filter sizes Filling IX. Preparation of manufacturing procedures:-: 37 IX. Preparation of manufacturing procedures :- The processing directions should be precise and explicit. The batch records should include addition rates, mixing times, mixing speeds heating and cooling rates and temperature should be given. Finished product specification and release specification are set; they should be take into consideration.X. GMP considerations:-: 38 X. GMP considerations :- A check list of GMP items Equipment qualification Process validation Regular process review and revalidation Relevant written SOP Adequate provision for training of personnel A well defined technology transfer system An orderly arrangement of equipmentsXI. Transfer of analytic method to quality assurance:-: 39 XI . Transfer of analytic method to quality assurance :- During the scale up new product the analytic test methods transferred to the quality department. The quality assurance staff should review the process to make sure that the proper analysis instrumentation is available and that personnel are trained to perform tests.Viscosity-: 40 Viscosity- It is the internal resistance (or) friction to the movement of molecules to “FLOW”. Agents which control viscosity E.g. Polyvinylpyrolidine, alginates, carbomers, and various cellulose derivatives. .PowerPoint Presentation: 41 Purpose to control Viscosity - 1. Improve pour ability. 2. Improve acceptability. 3. Improve palatability. Equipment used for this purpose are as followed- By OSTWALD VISCOMETER (Or) BY FALLING SPHERE VISCOMETER. OSTWALD VISCOMETER FALLING SPHERE VISCOMETERPreservative evaluation: 42 Preservative evaluation Preservative evaluation – should be done in addition to physical and chemical tests. Depending on the nature of the product and degree of protection required the surface of the product can be over lapped during filling or holding stages with carbon dioxide or nitrogen. Bacteriological testing should be done, to know if the concentration of preservative is to be increased in the formulationStability studies:-: 43 Stability studies:- Physical: Physical instability of liquid formulations involves the formation of precipitates, less-soluble polymorphs, and adsorption of the drug substances onto container surfaces, changes in product appearance. Chemical : Chemical instability of liquid formulation is mainly due to interaction between additives, oxidation or some due to interaction with containers. Microbiological : It is the most favorable condition for the growth of microorganism. So studies must me conducted for different microbiological test. Different preservatives are used to make product more stable.Type of changes:: 44 Type of changes: Contents : Viscosity, Texture, Color, Odour, pH Containers : a) Leakage, b) Corrosion, c) Stress d) cracking Glass container Plastic or metal capREFERENCES:: 45 REFERENCES: Leon Lachman, Liberman & Joseph.L, The theory & practice of industrial pharmacy. 3rd Ed., Vargese publishing house-1991, 466-75,681-84,703-706. James Swarbrick, encyclopedia of pharmaceutical technology Third Edition volume 5. Herbert A. Lieberman, Martin M. Rieger and Gilbert S. Banker, pharmaceutical dosage forms: Disperse system vol 1. Howard C. Ansel Introduction to pharmaceutical dosage forms, 4th edition. www.google.comPowerPoint Presentation: 46PowerPoint Presentation: 47 You do not have the permission to view this presentation. In order to view it, please contact the author of the presentation.
pilot plant scale up technique for Liquid Orals. harish_pharma Download Post to : URL : Related Presentations : Share Add to Flag Embed Email Send to Blogs and Networks Add to Channel Uploaded from authorPOINT lite Insert YouTube videos in PowerPont slides with aS Desktop Copy embed code: (To copy code, click on the text box) Embed: URL: Thumbnail: WordPress Embed Customize Embed The presentation is successfully added In Your Favorites. Views: 464 Category: Entertainment License: All Rights Reserved Like it (0) Dislike it (0) Added: November 11, 2011 This Presentation is Public Favorites: 2 Presentation Description No description available. Comments Posting comment... By: preethidevarapalli (2 month(s) ago) please send it to my id preethidevarapalli@gmail.com by tomorrow urgent pls Saving..... Post Reply Close Saving..... Edit Comment Close By: martin789 (6 month(s) ago) sir i am one of the user of this author stream,but ur ppt is not showing any download option.......................................... Saving..... Post Reply Close By: harish_pharma (6 month(s) ago) u can download it now... Saving..... Edit Comment Close By: martin789 (6 month(s) ago) how can i copy this ppt sir........................ Saving..... Post Reply Close Saving..... Edit Comment Close By: martin789 (6 month(s) ago) how can i download this ppt sir................... it is very necessary for me Saving..... Post Reply Close Saving..... Edit Comment Close Premium member Presentation Transcript PILOT PLANT STUDY FOR LIQUID ORALS: 1 PILOT PLANT STUDY FOR LIQUID ORALS HARISH DHANASHREE I M PHARMA DEPT OF PHARMACEUTICSIntroduction:: 2 Introduction : Pilot plant is a processing system used to generate the information about behavior of the system that can be used in designing large scale unit Intermediate to laboratory and production plantPowerPoint Presentation: 3 Process scale up is an increase in batch size or production capacity, usually in response to increased product demand, concerns about high production costs, or an increased need for clinical research supplies.LIQUIDS ORALS: 4 LIQUIDS ORALS Liquid pharmaceuticals encountered in the pilot plant are defined as non sterile solutions, suspensions or emulsions. Scale of each of these present a different set of processing concerns that must be considered Liquid orals are the liquid dosage formulations containing one (or) more active ingredients with (or) without additives dissolved in a suitable vehicle, meant for oral administrationPowerPoint Presentation: 5 The physical form of a drug product that is pourable displays Newtonian or pseudoplastic flow behaviour and conforms to it’s container at room temperature. Liquid dosage forms may be dispersed systems or solutions . In dispersed systems there are two or more phases, where one phase is distributed in another. A solution refers two or more substances mixed homogeneously.TYPES OF ORAL LIQUIDS: 6 TYPES OF ORAL LIQUIDS SOLUTIONS EMULSION SUSPENSIONOBJECTIVE: 7 OBJECTIVE A formula is transformed into a viable robust product using reliable and practical method of manufacture that effects the orderly transition from lab to routine processing in a full-scale productionSTEPS INVOLVED IN PILOT PLANT FOR LIQUID ORAL: 8 STEPS INVOLVED IN PILOT PLANT FOR LIQUID ORAL Reporting responsibility Personal requirements Space requirements Review of the formula Raw materials Relevant processing equipments Production rates Process evaluation GMP consideration Transfer of analytic method to quality assuranceA pilot plant layout.: 9 A pilot plant layout.PowerPoint Presentation: 10 Raw materials Weighing & Measuring Mixing Distilled water Filling Packing Finished Product storage Quality Assurance Pilot Plant Scale-Up Techniques for liquid oralsGeneral Consideration: I. Reporting responsibilities:: 11 General Consideration: I. Reporting responsibilities: The goal of pilot plant scale is to facilitate the transfer of a product from the laboratory in to production. The formulators continue to provide support to the production even after the transition in to production has been completed. There must be good relation between pilot plant and other departments.II. Personnel requirements:: 12 II. Personnel requirements: Have good theoretic knowledge of pharmaceutics. Practical experience in liquid orals manufacturing industry. Chemical, physical, biochemical and medical properties of drugs. Have the knowledge of computer, electronics.III. Space requirements:: 13 III. Space requirements : Administration and information processing area Physical testing area Standard pilot plant equipment floor space Storage areaAdministration and information processing area: 14 Administration and information processing areaPhysical testing area: 15 Physical testing areaStandard pilot plant equipment floor space: 16 Standard pilot plant equipment floor spaceStorage area : 17 Storage areaIV Review of formula:: 18 IV Review of formula: A thorough review of each and every steps of formulation is important The purpose of each ingredient and its contribution to the final product should be studied If any modification in formula, it should be done as soon as possible in phase III trials to allow time to generate meaningful long term stability in a support of a proposed new drug applicationV. Raw materials:: 19 V. Raw materials : One responsibility of pilot plant function is the approval and validation of the active ingredient and excipients raw materials used in the pharmaceutical products. The quality of the active ingredients needs to be verified.Formulation consideration:: 20 Formulation consideration : Solvents Preservatives Antioxidants Solubilizers Organoleptic agents etc.SOLVENTS: 21 SOLVENTS Water Alcohol Glycerol Polyethylene glycol Propylene glycol.Water: 22 Water Compared to ordinary drinking water , purified water USP is more free of solid impurities. When evaporated to dryness, it must not yield greater than 0.001% of residue. Purified water is obtained by distillation, ion-exchange treatment, reverse osmosis and other relevant methodPRESERVATIVES: 23 PRESERVATIVES Preservatives are added to prevent the microbial growth Preservative are necessary due to chances of microbial growth Raw material, processing containers & equipments, the manufacturing environment, operators, packing materials & the user . Phenol, chlorocresol, benzoic acid, etc.PowerPoint Presentation: 24 Antioxidants: ascorbic acid, sodium thiosulphate, sodium metabisulphate. Solubilizers: co-solvents and surface active agents Organoleptic agents etc: colour, flavor, sweetening agentsVI. Relevant processing equipment:: 25 VI. Relevant processing equipment : Almost all formulation development work is carried out on small, relatively simple laboratory equipment. The equipment that is most economical, the simplest, the most efficient should be selected Liquid pharmaceutical processing tanks, kettles, pipes, mills, filter housings, and so forth are most frequently fabricated from stainless steel. Of the three types commonly used in the industry (304, 308, and 316), type 316 is most often used because it is the least reactive. Ease of cleaning should be considered, if multiple products are to be manufacture in the same equipment.Stages of operations: 1.Tank selection: 26 Stages of operations: 1.Tank selection Material of the tank must not be additive to the product The shape and size of equipment must be selected according to the batch size The tanks are usually constructed of polished stainless steel of different grades Teflon and glass lined tank. Adequate clean-up procedures developed.2.Mixing: 27 2.Mixing Simple mixing is essential to increase flow of liquids. If the liquid is of high viscosity, high electrical stirrer may be used. Addition of ingredients in proper order have vital important. At high viscosity the chance of air entrapment .Air entrapment Minimize:-: 28 Air entrapment Minimize :- By reducing agitator speed By caring out the mixing procedure in enclosed tank under vacuum The alternative procedure to the all is versatorVersator: 29 Versator3. Dispersion: 30 3. Dispersion Suspensions and emulsions require considerably greater shear forces Laboratory formulation is difficult to duplicate at large scale Dispersion produced by colloidal mill or an immersion homogenizer Variety of equipment should evaluated for better results. Homogenizer Colloidal mill4. Filtration and clarification—: 31 4. Filtration and clarification — Filtration procedure, requires careful evaluation to ensure that pilot scale-ups will exhibit the same degree of clarity as their laboratory counterparts. During the pilot run the clarity of the filtrate should be checked periodically, in order to establish schedule for changing pads, cake, or cartridges, depending on the type of filtration employed. In filtration, filter pads are used which is made up of asbestos and cellulose. Selection of filtration depends on The product viscosity Volumes Rate requirement 5. Transfer and filling: 32 5. Transfer and filling Filling – important parameter in the transfer of liquids from tank to tank and into containers. New batches should not be started until the previous batches are completely filled and the tanks are emptied. Bins and PipingMethods for filling of liquids:-: 33 Methods for filling of liquids:- The selection of equipment depends on characteristic of liquid such as, viscosity, type of packaging, surface tension. Gravimetric (specific weight) Volumetric (specific volume) Constant volume filling Gravimetric VolumetricContainers and closures: : 34 Containers and closures: Glass Plastic It is more important to store the final product in container until its expiration. Most oral liquids are packed in either amber or flint glass containers with plastic or metal caps.VII. Production rates:-: 35 VII. Production rates :- The immediate and future market requirements -estimating the production rates, selecting the type and the size of the equipment needed. Determining the product loss in the equipment during manufacture. The time required to clean the equipment between batches. The number of batches that will need to be tested for release.VIII. Process evaluation:-: 36 VIII. Process evaluation :- Items that should be examined include the following- Mixing speed Mixing time Rate of addition of solvents, solutions of drug, slurries etc Heating and cooling rates Filter sizes Filling IX. Preparation of manufacturing procedures:-: 37 IX. Preparation of manufacturing procedures :- The processing directions should be precise and explicit. The batch records should include addition rates, mixing times, mixing speeds heating and cooling rates and temperature should be given. Finished product specification and release specification are set; they should be take into consideration.X. GMP considerations:-: 38 X. GMP considerations :- A check list of GMP items Equipment qualification Process validation Regular process review and revalidation Relevant written SOP Adequate provision for training of personnel A well defined technology transfer system An orderly arrangement of equipmentsXI. Transfer of analytic method to quality assurance:-: 39 XI . Transfer of analytic method to quality assurance :- During the scale up new product the analytic test methods transferred to the quality department. The quality assurance staff should review the process to make sure that the proper analysis instrumentation is available and that personnel are trained to perform tests.Viscosity-: 40 Viscosity- It is the internal resistance (or) friction to the movement of molecules to “FLOW”. Agents which control viscosity E.g. Polyvinylpyrolidine, alginates, carbomers, and various cellulose derivatives. .PowerPoint Presentation: 41 Purpose to control Viscosity - 1. Improve pour ability. 2. Improve acceptability. 3. Improve palatability. Equipment used for this purpose are as followed- By OSTWALD VISCOMETER (Or) BY FALLING SPHERE VISCOMETER. OSTWALD VISCOMETER FALLING SPHERE VISCOMETERPreservative evaluation: 42 Preservative evaluation Preservative evaluation – should be done in addition to physical and chemical tests. Depending on the nature of the product and degree of protection required the surface of the product can be over lapped during filling or holding stages with carbon dioxide or nitrogen. Bacteriological testing should be done, to know if the concentration of preservative is to be increased in the formulationStability studies:-: 43 Stability studies:- Physical: Physical instability of liquid formulations involves the formation of precipitates, less-soluble polymorphs, and adsorption of the drug substances onto container surfaces, changes in product appearance. Chemical : Chemical instability of liquid formulation is mainly due to interaction between additives, oxidation or some due to interaction with containers. Microbiological : It is the most favorable condition for the growth of microorganism. So studies must me conducted for different microbiological test. Different preservatives are used to make product more stable.Type of changes:: 44 Type of changes: Contents : Viscosity, Texture, Color, Odour, pH Containers : a) Leakage, b) Corrosion, c) Stress d) cracking Glass container Plastic or metal capREFERENCES:: 45 REFERENCES: Leon Lachman, Liberman & Joseph.L, The theory & practice of industrial pharmacy. 3rd Ed., Vargese publishing house-1991, 466-75,681-84,703-706. James Swarbrick, encyclopedia of pharmaceutical technology Third Edition volume 5. Herbert A. Lieberman, Martin M. Rieger and Gilbert S. Banker, pharmaceutical dosage forms: Disperse system vol 1. Howard C. Ansel Introduction to pharmaceutical dosage forms, 4th edition. www.google.comPowerPoint Presentation: 46PowerPoint Presentation: 47