drug manufacturing notes on drying procedure. UST 3rd year BS Pharma.
Preparations 1-6Full description
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Descripción: Pre informe laboratorio química 4 5 6
Descripción: procesos administrativos
For those taking the IB diploma, Engilsh lang and lit , IOC for the great gatsby. These are some really good notes and will help you on a whole in understanding the book.Full description
Descripción: For those taking the IB diploma, Engilsh lang and lit , IOC for the great gatsby. These are some really good notes and will help you on a whole in understanding the book.
manuf lab
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Laboratorio Cisco Exploration 6.4.6 en españolDescripción completa
Case Notes - Topic 6
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CPA Study Notes - FARFull description
EGR
MANUF LAB (PRELIMS) PREPARATION 4,5,6 POWDERS mixture of finely divided drugs &/or chemicals in drug form may be finely subdivided, coarsely comminuted product or product of intermediate particle size used internally or externally Advantages: flexibility of compounding good chemical stability rapid dispersion of ingredients Disadvantages Time consuming inaccuracy of dose unsuitability for many unpleasant tasting, hygroscopic and deliquescent drugs Packaging & Dispensing Bulk Powder Divided Powder
Sieve Size: All Particles Pass Through
Very Coarse (No. 8)
20
Coarse (No.20)
20
Moderately (No.40)
Coarse
USP Descriptive Terms
Sieve Size: All Particles Pass Through
20
Coarse (No.20) Moderately (No.40)
Coarse
40
Fineness Nmt 60% through a no.40 sieve Nmt 60% through a no.60 sieve
Characteristics Homogenously blended Methods of Blending a.) Small Scale Spatulation Trituration Geometric dilution Sifting b) Large Scale Tumbling Must be of the most advantageous particle size Comminution techniques a) Small Scale Trituration Levigation Pulverization by intervention b) Large Scale Various mills Pulverizers USP Standards for Powders of Animal & Vegetable drugs USP Descriptive Terms
USP Standards for Powder of Chemicals
40
Fine (No.60)
60
Very Fine (No.80)
80
NaCl......................................... 1.6 g KCl............................................ 1.5 g ` NaHCO3................................... 1.5 g Anhydrous Glucose............. 36.4 g For 1 L soln *Each subgroup prepared for 200 mL soln Guidelines in labeling Electrolytes for ORT must be expressed in mEq Quantities of electrolytes administered to patients Prep of Label ORAL REHYDRATION SALTS Provides 200 mL Soln Sodium.................................................... ___meq Potassium.............................................. ___meq Chloride................................................. ___meq Bicarbonate........................................... ___meq Anhydrous Glucose............................ ___meq
Fineness
Not more than (nmt) 20% through a no.60 sieve
Nmt 40% through a no.80 sieve Nmt 40% through a no.80 sieve Nmt 40% through a no.100 sieve No limit to greater fineness
Direction for reconstitution must be indicated in the labelling materials Dispensing: Each dose should be dissolved in sufficient, freshly boiled and cooled water to make 200 mL solution taking hygiene and precaution. Storage: Powders: ______________ After reconstitution: Unused soln must be discarded after 1 hour Refrigerated: may be kept for 12 - 24 hrs
2 SUSPENSION Preparation containing finely divided drug particles distributed uniformly throughout a vehicle 2 phase systems dispersed medium can be oily or aqueous dispersed phase is usually greater than 0.5 Preparation = GELOMAMI Purpose: Sustaining Effect Stability Taste Base Solubility Properties of Ideal Suspension uniform particle size no particle interaction no sedimentation or slow sedimentation rate other properties: redisposable, chemically stable, acceptable to consume Components Active Ingredient Wetting Agt -make them more soluble to solvent -Alcohol, PPG, Sorbitol, Surfactant Floculating Agt -avoid aggregates -electrolytes < 1% of KCl & NaCl Viscosity Agt -increases viscosity, hydrophillic colloids -clays, gums Buffer Preservative Flavorant Colorant Solvent 2 Forms of Suspension Ready to use - oral suspension - no reconstitution needed Dry Powders/ Dry Granules for Oral Suspension -reconstitution required -contains "for oral suspension" PREPARATION 5: Aluminum Magnesium Hydroxide Al(OH)3......................................................7% (Active Ing) Mg(OH)2....................................................3% (Active Ing) CMC Na....................................................2.5 % (Viscosity Agt) Peppermint................................................0.1% (Flavorant) Na Saccharin..............................................0.1% (Sweetener) Na Benzoate...............................................0.1% (Preservative) Sorbitol Soln...............................................20% (Wetting Agt) Purified H2O qs ad.....................................100%
Procedures: Place Mg(OH)2 in a blender Add Sorbitol Soln Add purified water (1/3) Blend the mixture 5 mins Add Al(OH)3 gel blend for 5 mins Place CMC in a mortar & triturate with 50 mL water until paste is formed Add CMC paste to the blender In a separate container, heat water to 500C & dissolve saccharin solution & Sodium benzoate. Cool the soln to 400C. Charge into blender & blend for 10 mins Add Peppermint oil Homogenize the suspension QS H2O. Blend for 1-2 mins GRANULES Prepared agglomerates of smaller particles Irregularly shaped and behave as single larger particles uses sieve #4 -12 for particles size classification Granulation Pharmaceutical process that attempts to convert produced materials into aggregates Large Scale - granulating machine on granulation Small Scale powder + water => moist mass =>sieve #4-12 =>net granules =>(drying) Dry granules Advantages flow well composed to powder more stable physically and chemically than powders Easily wetted PREPARATION 6: Phenoxymethyl Penicillin Phenoxymethyl Penicillin............................ 25g CMC................................................................ 25g Sucrose............................................................125g Na benzoate...................................................9 g Citric Acid......................................................5g Cone strawberry powder ..........................1g Lactose...........................................................30g
EGR
3 Procedures: Mix the powders & blend for 15 mins using titration Prepare 20 mL colorant solution & spray into powder mixtures with continuous trituration until a moist mass is formed Pass the moist mass through sieves #12 & receive net granules in a tray Oven dry granules a temp not exceeding 400C -1 hour Dry the granules until 1 nmt 2% moisture is present. Check the moisture content every 30 mins weigh & pack the divided granules
