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PREPARATION FOR INHALATION. Drugs under pressure. Drugs that are under pressure - preparation for inhalation Propellant Based-Metered Dose Inhalers. - PowerPoint PPT Presentation
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PREPARATION FOR INHALATION.
Drugs under pressure.
Drugs that are under pressure - preparation for inhalation
Propellant Based-Metered Dose Inhalers
this drug that are in special containers (canister) under the gas pressure and containing one or more active ingredients, as the solutions, emulsions or suspensions, which are released from canister in the aerosol, liquid or soft form due pressing on the valve .
Aerosol is a dispersion of solid or liquid particles of medicine substances in the gas, the size of which depends on the prescription.
Features of pMDI•The drug product consists of: container, actuator, formulation and protective packaging; dosing performance is highly dependent on the design of the device.
•The drug delivered to the patient consists of: API, excipients, propellant and/or solvent.
•Aerosolization of the formulation from the pressurized canister is highly transient, complex and rapid.
•The concept of classical bioequivalence and bioavailability is not usually applicable for inhalation aerosols.
The advantage of the preparation for inhalation:
• Ease of use, aesthetics, hygiene.• Availability of high efficiency at relatively low
cost drugs.• Use the metered device providing exact dosing.• Preparations for inhalation give rapid therapeutic
effect.• Canister is tightly closed, ensuring sterility and the
drug protecting from the impact of the external factors.
• When a large number of manipulations do not need a large number of staff.
Disadvantages of the drug under pressure:
relatively high cost;
possibility of explosion of the canister due impact or high temperature;
air pollution by drugs and propellants at the manipulation.
Classification of the drug under pressure
Pharmaceutical – are composed of the canister, valve-spray systems and content of different consistency, which are released from canister at the pressing on the valve due propellant. The structure of this product includes MS, auxiliary substances and propellants.
Medical – this means one or more MS in the form of solid or liquid particles, obtained by means of special stationary and intended primarily for inhalation administration.
1. inhalation,2. otolaryngology,3. dermatological,4. dental,5. proctologic et al.
Classification of the pharmaceutical drug under pressure by appointment:
Pharmaceutical drug under pressure
• topical (skin) therapy for local anaesthesia and cooling for
• sports injuries;• sub-lingual sprays for angina pectoris;• nasal sprays for allergic rhinitis and
sinusitis;• vaginal foams for contraception;• rectal foams for colitis.
FormulationActive Pharmaceutical Ingredients •Micronized•Spray Dried•Freeze Dried•Others
Excipients / Surfactants (improve valve lubrication, enhance API solubility and increase homogeneity of the suspension)
Propellants - HFA 134a and 227Solvents - ethanol (increase API solubility, increase miscibility of the surfactant and lower vapour pressure of propellant)
Principal Control Factors•Momentum (Particle/Droplet Size and Mass, Morphology, Shape and Velocity) •Particle Design•Formulation•Aerosol Generation•Plume Manipulation (delivery system specific)•Delivery Timing Relative to Aspiratory Cycle Synchronize propulsion and inhalation dynamics
Closure Container System/Primary Packaging
Container/canister (reservoir)• Coated (chemically or plasma)• Uncoated high grade aluminium Valve (seal and volume control)• Retention – Gaskets • need to prime• Non-retention• no need to primeNozzle (modify the rate of flow, speed, direction, mass,
shape, pressure of stream)Actuator/Mouthpiece(affect spray pattern and droplet/particle size)
Canisters and valve-spray devices1 - canister;2 - sprayer - mouthpiece;3 - metering valve;4 - siphon tube;5 - solution of MS;6 - a vapour of the
propellant;7 - propellant.Capacity from 3 ml to 3 litters.
a - two-phase system;b - three-phase system;
ba
Types
1. Two-phase system. (Gas & liquid)
2. Three-phase system. (Gas, liquid, solid/liquid).
Classification of canisters depend on material
1. Metal2. Glass3. Plastic4. Combined
Requirements to the glass canisters:
• should withstand the internal pressure (at least 2 MPa)
• should be resistant to impact• should be chemically and thermally stable• should not have internal stresses of glass• should have a uniform thickness of the• walls and bottom• should have a minimum flat surfaces
Requirements to the another canisters:
Plastics must be employed to coat the glassto improve safety characteristics or to coatmetal containers to improve corrosionresistance and enhances the stability offormulation. Suitable metals include stainless steel,
aluminium and tin-plated steel.
Classification of the metering valve depend on principle of
operation:
1. Spring in force when you click vertically down on the actuator;
2. Oscillated springless when you click by the side on the actuator;
3. Valves with screw valve.
Classification of the metering valve depend on the way of fixing to the
canister:
1. fixed by decompressing on the vertical walls;
2. by the process of rolling of the valve body on the special walls;
3. by screw metering valve on the neck canister.
Classification of the metering valve depend on appointment:
1. standard valves for liquid products,
2. for the foams;
3. for the viscous products;
4. for the powders and suspensions.
Types of the Nebulizers
• Conventional Tee Nebulizers• Standard jet nebs w/ reservoir tubing• Venturi nebulizers• Passive and Active venturi nebulizer• Breath actuated nebulizers• Ultrasonic nebulizers• Vibrating mesh
Types of the actuators:
1. for inhalation,2. for the treatment of
the asthma,3. for suspension,
4. for film forming composition;
5. nozzles dental, rectal, vaginal.
PropellantsFor pressurized metered dose inhalations
propellants perform the essential function of expelling the material from the container by supplying the necessary pressure within the aerosol system.
They are liquefied or compounded gases having vapor pressures exceeding employed to obtain the necessary delivery and spray characteristics of the aerosol.
The commonly used propellants in aerosolsystems are hydrocarbons, especially thefluorochloro derivatives of methane andethane (Table ), the butanes and pentanesand compressed gases are used.
Commonly used propellants in aerosol systems
Propellants Molecular weight Vapor pressure011(CCl3F) 137.4 13.4012(CCl2F2) 120.9 94.5 114(C2Cl2F4) 170.9 27.6 134(CH2FCF3) 102.0 96.0 227(CHF2C2F5) 170.0 72.6
Classification of the propellants depend on the vapor pressure:
1. The main, can create their own pressure not less than 0.2 MPa,
2. Auxiliary - propellants creating a pressure less than 0.1 MPa.
Classification of the propellants depend on the states of aggregation:1) Liquefied gases:
Freon , propane, butane, isobutane, vinyl and metylhloryd et al.
2) Compressed (difficulty liquefied) gases: nitrogen, nitrogen oxide, carbon dioxide;
3) easy volatile organic solvents:
metylenhloryd, ethylene chloride, etc.
Stages of the Drugs under pressure production:
1. Sanitary preparation of production2. Preparation of concentrate - MS solution3. Release him from insoluble impurities4. Packing in containers5. Sealing6. Filling propellant7. Check the strength and impermeability8. Standardization9. Design package for transportation
The advantages of the emulsion systems – foams:
- provides economical dosing- better contact with the mucous membrane,
provides long-acting of the MS ,- under the influence of body temperature they
increase in the volume, filling all vacancies and channels in the rectum or vagina
- can move in proximal direction, and during 4 hours provide a high concentration of MS.
Factors that affect on the stability of the foams:
• concentration of the foam agent,• presence of the electrolyte• pH,• viscosity of the solution• concentration and type of the propellant,• presence of the additives.
The indicators used to evaluate the foam:
• appearance• issuing its type of container (smooth, jerky, loud)• stability and lifetime,• elastic properties of the foam• drying as a percentage of the time,• wetting properties,• density,• viscosity,• dispersion.
Classification of the foams
Classes of the foams
Aqueous:aqueous phase,surface active
agents,propellant.
Aqueous alcohol:water
ethyl alcohol,foam,
propellant.
Nonaqueous :vegetable oil
or mineral oil, surface
active agentspropellant
Suspension under pressure - a heterogeneous dispersed systems are
characterized by the presence of th insoluble in liquid concentrate solid phase.
Classification by composition:
1. They propellant may be included in the soluble phase or dispersion medium.
2. The active substance is dispersed in non-volatile solvent.
The main factors affecting on the quality of suspensions:
1. physical and chemical properties of the substances;
2. correlation between the components of the filler;
3. features of the design and material of the packaging;
4. temperature conditions of the maintenances container.
Canisters Production:
Monoblock aluminium containers are made from flat pieces forming presses for impact type.
Glass containers are made of neutral borosilicate glass on the automatic glass forming machines by double firing in horizontal furnaces.
Plastic ones are made by vacuum forming or molding by pressure on the molding machines.
Methods of filling of the containers by propellants:
1. Filling pressure (primary)
2. Low-temperature method or "cold filling“
3. Method of filling by the compressed gases
4. Method of filling by the soluble compressed gases.
The steps of filling containers: A. Washing, rinsing and drying of the containers
2. Blowing of the containers with sterile air
3. Filling the container with solution of concentrates
4. Remove air from the container by th e drop of liquid propellant
5. Sealing of container by consolidation valve
6. Filling the propellant under pressure
7. Check for leaks and strength.
Storage:
• avoid impacts, direct sunlight,
high temperature.
Aerosol Testing Devices• Cascade Impactors-Provides aerodynamic particle sizing
and gives qty. of specific drug at a specific size- Anderson Cascade, Marple Miller and Next Generation
Impactor• Laser Diffraction Shines a laser beam through a particle
and measure the refraction of the laser light to determine the size of the particle. Converts particle size to an equivalent sphere.
- Malvern Mastersizer and Malvern Spraytech• Breath Simulation- Harvard Pump• Dose Assessment:- Filter Collection for weight analysis- Spectrophotometry / HPLC to assess drug presence
Aerosol TestingCascade Impactors AdvantagesProvides aerodynamic particle sizeProvides how much specific drug
at a specific sizeCascade Impactors
DisadvantagesContinuous flow rateLong test timesRequires testing to determine
amount of drug on each stageDuring nebulizer testing
(Specifically on Anderson impactor), drug may roll to the next stage if plate is overfilled
Evaporation during test understates particle size
Laser testing AdvantagesSpeed / Cost /Efficiency .Measures particle size in real timeLaser testing DisadvantagesCan only measure the particle size
distribution of solution based drugs . With a suspension, does not differentiate between the carrier and the drug
Does not take into account the aerodynamics of a particle (How does the particle look to a specific flow?)
Does not measure the quantity of drug in specific particle size ranges
Summary• Primary packaging design of an aerosol delivery
system is an integral part of its function
• Optimizing the principal design control factors of the drug product component will enhance the delivery efficiency and improve the consistency of the delivered dose
• Knowledge of optimizing these factors give us the edge on delivering innovative therapeutic agents