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MANUFACTURING TECHNIQUES, PROCESSES, AND TECHNOLOGIES OF LARGE AND SMALL VOLUME PARENTRAL PRODUCTION
outline
introduction
Parenteral products-for use by injection under or through one or more layers of the skin or mucous membranes They are most frequently
solutions suspensions but may even be solid pellets for tissue implantation
microbial contamination and from toxic components as well as possess an exceptionally high level of purity
introduction
These characteristics are the principal qualities that distinguish parenteral products from other types of pharmaceutical dosage forms. in the preparation of these products all components and all processes must be selected and designed to eliminate contamination of all types, whether of physical, chemical, or microbiological origin The preparation of sterile superior level of
The standards established, the attitude of personnel, and the process control.
Formulation Ingredients
Antimicrobial preservative Agents required in preparations intended for multiple dosing from the same container
Cont
Prevent oxidization by being oxidized faster than the drug or by blocking oxidization Water soluble Oil-soluble
Buffers
Production
The production process included all of the steps from the accumulation and combining of the ingredient of the formula to the inclosing of the product individual container for distribution
Production
All equipment and supplies introduced into the aseptic filling area should be sterile
having come directly from the sterilization process, preferably through autoclaves, ovens and UV-light
WFI
WFI is stored and delivered at elevated temperatures from a 20,000-L tank to various locations in the manufacturing clean
the clean steam generator, WFI still, CIP skids and wash-up areas.
The AWFI loops have an automated procedure to sanitize the circuits as required
Mixing
a.
Efficient mixing, homogenizing and volume dispersing of powders in liquid media, Important when effective solid wetting and fine dispersion are required at comparatively low energy input levels.
Mixing
Vertical mixer / homogenizer type VRM
Suitable for the mixing and homogenizing of freeflowing products with different particle sizes and bulk densities. The design of the VRM mixer is based on the principle of creating multiple mass flows within the mixing vessel. The products to be mixed are first conveyed upward by a screw mounted in a central mixing tube. The tube is fitted with one or more mixing heads. At each mixing head and at the top of the mixing tube the product is partially discharged into the descending product flow. Capacities from 500 up to 100,000 liters.
Mixing
Vertical conical screw mixer type CRM
The conical mixer is suitable for the mixing of viscous products. The conical mixer can be supplied in any required material. Capacities from 100 up to 5,000 liters.
Filtration
Filtration is a unit operation process in which particles are separated from a liquid through a permeable material
Bulk drug sterilization is accomplished by filtration, normally a depth filter.
The drugs can be pre-sterile filtered (e.g. .45 micron), followed by a series of at least two sterile filters at .22 micron.
The best-in-class for sterile filtration is a closed system that extends from the nonsterile bulk to the aseptic filling equipment.
Filter types
Sartobran P 523 Sterilizing grade pharmaceutical filter cartridge for low unspecific adsorption all applications that require highest product recovery rates Biological Fluids, Bacterial and Viral Vaccines Sartopore 2 544 Sterilizing grade pharmaceutical filter cartridge with broad chemical compatibility Typical applications include sterilizing grade filtration of: SVPs, LVPs Antibiotics Biological Fluids Ophthalmic
Filter types
Sartolon 510
Sterilizing grade pharmaceutical filter cartridge with reinforced Nylon membrane for broad solvent compatibility
sterilizing grade filtration of: Solvents, Antibiotics, Bulk Pharmaceutical Chemicals, LVP Pharmaceutical grade hydrophobic PTFE membrane filter cartridge Sterile air filtration for filling equipment Fermentation air filtration Sterile filtration of gases
Filtration
Consideration should be given to complementing the filtration process with some degree of heat treatment Such filters can remove most bacteria and moulds, but not all viruses or mycoplasmas The time taken to filter a known volume of bulk solution and the pressure difference to be used across the filter should be determined during validation The Sterile bulk is then transferred to the aseptic fill and aseptically connected to the fill equipment.
Filling
filling lines are designed for filling operations under aseptic and sterile conditions.
Filling
A measured volume of liquid through the orifice of a delivery tube designed to enter the constricted opening of a container. The size of the delivery tube is governed by the opening in the container to be used, the viscosity and density of the liquid, and
the speed of delivery desired. The tube must freely enter the neck of the container and deliver the liquid deep enough to permit air to escape
Filling
To reduce the resistance to the flow of the liquid, the tube should have the maximum possible diameter.
Excessive delivery force causes splashing of the liquid and troublesome foaming, if the liquid has a low surface tension
A drop of liquid normally hangs at the tip of the tube after a delivery. retraction device is designed as a part of most filling machines. Filling machines demounted for cleaning and sterilization. constructed of non reactive materials such as borosilicate glass or stainless steel.
Filling
The specific method used for filling a pharmaceutical liquid varies greatly depending on the characteristics of the liquid viscosity, surface tension, foam-producing qualities, and compatibility with the materials used in the construction of the filling machine) the type of package into which the liquid is placed, the required production output.
Filling
Three basic filling methods that are used for most liquid filling operations gravimetric, volumetric, and vacuum The latter two methods are used most frequently in the filling of pharmaceutical liquids.
Blow/fill/seal technology
Blow/fill/seal units are purpose built machines in which, in one continuous operation, containers are formed from a thermoplastic granulate, filled and then sealed, all by the one automatic machine
The plastic used to make the container is normally low, medium or high-density polyethylene or polypropylene, depending on the desired container properties
Blow/fill/seal
The plastic is obtained as small granules and, prior to use, kept in large bulk containers in a room adjacent to the BFS machine. When required, the plastic granules are transported to the BFS machine where they are melted in a high-pressure extruder to produce a tube, called the parison, of sterile, molten plastic.
Extruding : The plastic parison, extruded from polymer, is accepted by the opened blow mould and cut below the die of the parison head. Blowing : The main mould closes and simultaneously seals the bottom. The special mandrel unit settles into the neck area and forms the parison into a container using compressed air. Small containers are formed by vacuum.
Filling : By way of the special mandrel unit, the product, measured precisely by the dosing unit, is filled into the container
Sealing : After the special mandrel unit retracts, the head mould closes and forms the required seal by vacuum.
Mould Opening: With the opening of the blow mould, the container exits from the machine and the cycle repeats itself. Transfer for further processing is achieved by means of a conveying system.
Cleaning and sterilizations of prefabricated containers and closures is not required. A clean, sterile container is made within the BFS machine as it is required for filling The cost of material transport, storage and inventory control is reduced. Validation requirements are reduced A single compact BFS machine takes the place of several conventional machines, saving floor space In addition, zones for transport to successive filling and closing procedures are not required because these operations all take place in the BFS machine itself The operation of BFS machines is less labor-intensive than conventional aseptic filling
Cont
The ampoules / vials can be fed passing under a shower head, immersed in the heated ultrasonic bath. Pushed into and then fed directly on to the jetting needles to the jetting stations in the upper station. Blown of and lifted into the discharge tray Trayed or fed directly on to the conveyor belt of the sterilizing tunnel
sterilization
In case of steam sterilization up to 1210C, 2 bars for 30minutes, only bags with suitable fitments and films for this particular system must be used
liquid filling
Automatic Ampoule Filling Machine under a Class 100 Laminar Airflow Workstation. Product physical characteristics may suggest selection of one type of filling machine over another Low density liquid can be achieved with light-duty machinery, Viscous , sticky, or high-density liquids require much more rugged machines to withstand the pressure required to dispense them. Solution are usually filled by gravity, pressure, or vacuum filling devices
Solid Filling
are more difficult to subdivide accurately and precisely into individual dose containers than are liquids
rate of flow of solid material tends to be slow and irregular, particularly if finely powdered. Small, granular particles flow most evenly.
stratification of particles due to varying particles size, the development of electrostatic charge the formation of air pockets and an even flow due to clumping of the particles
Stoppering
Stoppering of the vial will be done after filling Stopper size will need to match the finish of the selected vial. Vibratory stopper bowl is used to orient vial stoppers so that they can be fed into automated placement equipment.
Stoppering
Compatibility of the product with the stoppers rubber formulation will dictate the stoppers physical characteristics.
A mineral-oilbased product will be incompatible with a butyl rubber stopper; a neoprene stopper is a better choice
Lyophilization
Lyophilization, commonly referred to as freeze drying, is the process of removing water from a product by sublimation and desorption. This process is performed in Lyophilization equipment which consists of
a drying chamber with temperature controlled shelves, a condenser a cooling system a vacuum system
For pharmaceutical compounds that undergo hydraulic degradation, Lyophilization offers a means of improving their stability and shelf life
Lyophilization
Many parenteral medications such as vaccines, proteins, peptides, and antibiotics have been successfully lyophilized Lyophilization cycles consist of three phases: Freezing, primary drying, and secondary drying During the freezing phase, the goal is to freeze the mobile water of the product. The rate of cooling will influence the structure of the frozen matrix If the water freezes quickly, the ice crystals will be small. This may cause a finer pore structure in the product with higher resistance to flow of water vapor and longer primary drying time If freezing is slower, ice crystals will grow from the cooling surface and may be larger. The resultant product may have coarser pore structure and perhaps a shorter primary drying time
Lyophilization
In the primary drying phase, the chamber pressure is reduced, and heat is applied to the product to cause the frozen mobile water to sublime. The water vapor is collected on the surface of a condenser It is important to control the heating rate during this phase
If the product is heated too rapidly, it will melt or collapse degradation of the product, and will change the physical characteristics of the dried material,
making it harder to reconstitute and
visually unappealing
Lyophilization
To improve the heat transfer mechanism, inert gas such as nitrogen may be introduced into the drying chamber at a controlled rate. The presence of these gas molecules facilitates heating of the walls of the container in addition to conduction through the bottom of the container, thereby increasing the amount of heat being supplied to the product per unit time During secondary drying temperature is increased to desorb bound water such as water of crystallization until the residual water content falls to the range required for optimum product stability
Lyophilization equipment
SEALING
Containers should be sealed in the aseptic area immediately adjacent to the filling machine a sterile container that has been opened no longer be considered to be sterile. temper proof sealing is essential. Ampoules bead seals (tip-seals) or pull-seals Sealing vials Rubber closures must fit the opening of the container snugly enough to produce a seal Aluminum caps are used to hold rubber closure in places
Quality control
Pyrogen tests traditional test uses rabbits, solution injected into the ear vein using sterile device measure body temperature a temperature elevation will occur within 3 hours Many imitative medical agents will also cause a fever limulus amebocyte lysate(LAL) tests A test sample is incubated with amebocyte lysate from the blood of the horseshoe crab, Limulus polyphemus. A pyrogenic substance will cause a gel to form clottable protein from the amebocyte cells reacting with the endotoxins This test is more sensitive, more rapid, and easier to perform than the rabbit test
Leaker Test
microorganisms or other dangerous contaminates may enter the ampoule, or the contents may leak to the outside and spoil the appearance of the package
Changes in temperature during storage cause expansion and contraction of the ampoule and contents accentuating interchange if an opening exists
Tip-sealed ampoules are more likely to be incompletely sealed than are those that have been pull-sealed
Leaker Test
submerged ampoules in a deeply colored dye solution (usually 0.5-10% methyleneblue) Subsequent atmospheric pressure then causes the dye to penetrate an opening visible after the ampul has been washed externally to clear it of dye
Clarity Test
every unit of product is perfectly free from visible particulate matters it is the responsibility of the quality control department to detect and discard individual containers of product that the ultimate user would consider unclear
packaging
packaging is an essential part of the parenteral formulation . providing long-term protection and maintenance of physical and chemical stability The main types of packaging systems
Summary
Parenteral production requires aseptic environment and strict follow-up of the different unit operations. Hence, use of recent technologies like Blow-fill-seal Machines could be invaluable.