DISPERESE SYSTEM - Ease of swallowing

- Flexibility of doses
TYPES OF LIQUID DOSAGE FORM
SOLUTION Properties desired in pharmaceutical suspension
- 1 phase - Settle slowly and should be readily redispersed upon
- Solute, solvent gentle shaking
- Completely soluble - particles size should remain fairly constant
DISPERSED SYSTEM throughout long periods of undisturbed standing
- suspension and emulsions - Pour readily and evenly from its container
- 2 phases - Container: Wide-mouth Amber Bottle
- Not completely miscible
- SOLUTE (Dispersed phase, discontinuous phase or Sedimentation and Stoke’s Law
internal phase) - A flocculated suspension sediments faster and is
- SOLVENT (dispersing medium, continuous phase or easy to redisperse, whereas a deflocculated
external phase) suspension sediments slowly and is difficult to
redisperse. The rate of sedimentation of particles
Disperse System can be determined by Stoke’s law.
- Consists of dispersed phase and dispersion medium - Increase in particle size also increases velocity
- Particles of dispersed phase vary in size - Particle size
- 0.5µm to 10 µm fine dispersion: aerosols, inhalants - Density of the particle
- 1nm - 0.5µm colloidal dispersion: magmas, gels - Density of the medium
- 0.5 µm coarse dispersion (usually 10-50µm - Viscometer
suspension and emulsion) - Viscosity of the medium

SUSPENSION

- Refers to a two-phase system consisting of a finely

divided solid dispersed (suspended) in a liquid (the
dispersing medium)
- Preparations containing finely divided drug particles
(the suspensoid) distributed somewhat uniformly
throughout a vehicle in which the drug exhibits a
minimum degree of solubility
- Bentonite magma: common suspending agent
- It is a disperse system in which solid, vehicle-
insoluble particles (internal phase) are uniformly
suspended by mechanical agitation and formulation
design throughout the liquid vehicle (external phase)
- The solid particles are greater than 1um
- best pharmaceutical suspensions = 1 to 50 µm
Classification of Suspension
- According to route of administration
- Oral suspensions
- Topical/External suspensions
- Parenteral suspension
Advantages
- Provide palatable mixtures of an insoluble derivative
of a drug that in its soluble form has a highly
unpleasant taste
- Prolongs the action of drug
- Chemical stability
Dispersed phase
- Particle size is considered - between 1 - 50µm
- Reduction is accomplished by the use of dry milling,
micropulverization (10-50 um)
- Finer: < 10 um by fluid energy grinding – Jet milling
(micronizing)
o For parenteral or ophthalmic suspension
- Spray drying – extremely small dimensions
- Small particles reduce sedimentation rate but may
pose a problem on forming hard sediment
Flocs
- AKA floccules
- an aggregation of particles
- Form loose aggregate
- Rate of sedimentation is high
- Sedimentation volume is high somewhat unsightly
- Sediment is formed rapidly
- Sediment is loosely packed –AVOIDS the problem of
CAKING
Deflocculated Suspensions
- In this system, solids as present as individual
particles. They also exhibit aggregation but
comparatively low than flocculated.
- Pleasant appearance because of uniform dispersion
of particles
- Particles exhibit repulsive forces
- Particles settle independently
Flocculated Suspensions
- Solids are aggregate by forming chemical bridges
- A slightly sediment and supernatant layer is formed
- Particles exhibit attractive forces
- They settle flocs
Flocculating agents
- Bentonite, MC, sodium alginate, tragacanth,
- pH adjustment
- Electrolytes
- Surfactants
Dispersion medium (Criteria)
- Density of the suspensoid
- If suspensoid is flocculated
- Amount of the suspensoid
Use of suspending agents
- (Methyl Cellulose, CarboxyMethyl Cellulose,
MicroCrystalline Cellulose,PVP, xanthan gum and
bentonite) at concentrations of 0.5% to 5
Apply Rheology
- study of flow and formation of matter
- addresses the viscosity characteristics of powder and
fluid
Newtonian flow
- constant viscosity (e.g solutions)
Non-newtonian flow
- change in viscosity upon increasing the shear rates
(e.g., dispersed system)
- Plastic, Pseudoplastic, dilatant flow
- Plastic: viscosity decrease upon applying sheer rate
(ketchup) ―yield value
- Pseudoplastic flow: the substances begin to flow
after sheering stress is applied
- Dilatant flow: the materials increase in volume when
sheered; viscosity increases as shear rate increase
(whip cream)
Components of a suspension
Flocculating agents or suspending agents - enhance
particle ―Dispersability‖
Viscosity enhancers- reduce sedimentation rate in the
flocculated suspension (Hydroxypropylcellulose,
Hydroxypropylmethylcellulose)
Preservatives - prevents the growth of microorganisms
(Benzoic acid, Methyl Paraben)
Stabilizers - any additive used in substance and
compounds to keep them stable, retard deterioration
Wetting agents - increases penetration by the dispersion
medium (Alcohol, glycerin, propylene glycol, and other
hygroscopic liquids
Preparation of suspension
- Wet the powders using wetting agents like alcohol,
glycerin, propylene glycol and other hygroscopic
agents
- Use colloid mills or mortar and pestle to effect
thorough mixing
- Add the dispersion medium to which other soluble
components are dissolve
Extemporaneous preparation
- Capsules or tablets are place in mortar and pestle
- Vehicle is added and mixed thoroughly to create a
paste
- Diluted to volume using desired vehicle
- Caution on the use of alcohol, Benzyl alcohol and
Propylene glycol on neonates and geriatric patients
- International Journal of Pharmaceutical
Compounding
Packaging and storage
- Wide-mouth amber color bottles
- Tight containers
- Protected from freezing, excessive heat and light
- Shake well instruction – Antacid oral suspensions,
antibacterial, antiprotozoal and anti-inflammatory
OTHER EXAMPLES
Rectal suspensions
- Barium sulfate for suspension, Mesalamine, Colocort
- Barium sulfate: employed or administered orally or
rectally; used as diagnosis for diagnostic agents for
visualization of gastrointestinal tract
- Mesalamine: aka 5-aminosalicylic acid; used as
treatment for Crohn’s Disease; for protitis
- Colocort: cortico streiods used for ulcerative colitis;
antiinflamatory
Dry powders for suspension
- for oral suspension
 EMULSIONS
- A thermodynamically unstable two-phase system
consisting of at least two immiscible liquids, one of
which is dispersed in the form of small droplets
throughout the other, and an emulsifying agent.
- Micro-emulsions: Thermodynamically stable
- a dispersed system containing at least two
immiscible liquid phases. The majority of
conventional emulsions in pharmaceutical use have
dispersed particles ranging in diameter from 0.1 to
100 um.
Phases of Emulsion
- The dispersed liquid - internal or discontinuous
phase
- The dispersion medium - external or continuous
phase
Types of Emulsion
1. OIL-IN-WATER (O/W) EMULSIONS
- oils, petroleum hydrocarbons, and / or waxes are the
dispersed phase, and water or an aqueous solution is
the continuous phase
- Oil is dispersed as droplets in an aqueous medium.
- formed if the aqueous phase constitutes >45% of the
total weight and hydrophilic emulsifier is used
- O/W emulsions are used topically, orally, or
parenterally.
2. WATER-IN-OIL (W/O) EMULSION
- Water is dispersed as droplets in an oil or oleaginous
medium
- Used for external preparations when emollient,
lubricating, or protective properties are desired.
3. MULTIPLE EMULSIONS O/W/O OR W/O/W
4. MICROEMULSION - appear as translucent or
transparent and have droplet diameter in the
nanometer range
Advantages:
- dosage form of oral, rectal and topical administration
of oils and oil-soluble drugs
- enhances palatability of oils when given orally
- increases absorption of oils and oil-soluble drugs
through intestinal walls
- dosage form for IM administered (vegetable oils) and
some water-soluble vaccines
- dosage form for Parenteral Nutrition
THEORIES OF EMULSIFICATION
- surface tension theory – tension lowering substances
or wetting agent
- oriented-wedge theory
- plastic or interfacial film theory
SURFACE TENSION THEORY
- tension lowering substances or wetting agent or
surfactant
- The use of these substances that used as emulsifiers
or stabilizers to lower the interfacial tension to
penetrate the dispersing medium
- Reduce the repellent forces between the liquids and
diminishing the liquid extraction for its own molecule
- Facilitate the breaking of large globules
ORIENTED-WEDGE THEORY
- assumes the monomolecular layers of emulsifying
agents curved around a droplet of the internal phase
- Certain emulsifying agents orients themselves about
and within manner of their solubility
PLASTIC OR INTERFACIAL FILM THEORY
- Places the emulsifying agent interface between the
oil and water surrounding the droplets of the internal
phase as the thin layer of film absorbed on the
surface
Preparing an emulsion: Select the suitable emulsifier
- Compatible with the other ingredients
- table and do not deteriorate
- Nontoxic
- Little odor, taste or color
- Capable of emulsifying
Emulsifying agents
1. Natural emulsifying agents
- substances derived either form animal or plant
sources
- Example: gelatin, casein, egg yolk, wool fat,
cholesterol, acacia, tragacanth, pectin, alginates,
starch
2. High–molecular-weight alcohols
- Stearyl alcohol, cetyl alcohol, and glyceryl
monostearate
- Employed primarily as thickening agents and
stabilizers for o/w emulsions of certain lotions and
ointments used externally.
3. Finely divided solids
- substances adsorbed in the water interface to form
a coherent film. (Volcanic origin)
- Example: Bentonite, veegum, magnesium hydroxide,
aluminum hydroxide and magnesium trisilicate
4. Synthetic emulsifying agents
- or surface-active agents, they contain both the
lipophilic and hydrophilic groups.
- Anionic agents
o these are organic salts which are ionized in the
presence of water.
 o They are widely used in external preparations as
o/w emulsifying agents
o Ex. Sodium lauryl sulfate
- Cationic surfactants
o these are quaternary ammonium compounds,
which are inactivated by the presence of soaps.
o Emulsions which used this type are generally
stable at acidic pH
o Ex. Benzalkonium chloride
- Non-ionic surfactants
o these are the polysorbates and sorbitan series
which tend to be of low order toxicity,
nonirritating, tasteless and chemically stable
and are compatible with ionic, anionic and non-
ionic drugs or adjuvant
o Ex. PEG 400, SPANS (sorbitan), TWEENS
(polyoxyethylene derivatives)
HLB VALUES
- The type of emulsion formed is based on the
hydrophiliclipophilic balance (HLB).
- HLB system – logical means of selecting emulsifying
agents based on balance between the hydrophilic
and lipophilic portions of an emulsifying agent.
- HLB number usually between 1 and 20 are used as
emulsifying agents
- with values 8 –18 indicates hydrophilic molecule and
will produce o/w type of emulsion
- lower numbers in the range of 3 to 6 indicates
lipophilic molecules and will produce w/o emulsions
Methods of Preparation
1. Continental or dry gum method.
- “4:2:1”method
- O+G+W
2. English or wet gum method
- same proportions of oil, water, and gum but the
order of mixing is different.
- Mucilage is prepared
- G+W+O
3. Bottle or Forbes bottle method
- For the extemporaneous preparation of emulsions
from volatile oils or oleaginous substances of low
viscosities
- 3:2:1 or 2:2:1
4. Auxiliary Methods
- An emulsion prepared by either the wet gum or the
dry gum methods using hand homogenizer to
facilitate emulsification
- The hand homogenizer is less efficient in reducing
the particle size of very thick emulsions, and it should
not be employed for emulsions containing a high
proportion of solid matter because of possible
damage to the valve
5. In situ soap method
- The two types of soaps developed by this method are
calcium soaps and soft soaps. Calcium soaps are
water-in-oil emulsions, which contain certain
vegetable oils, e.g., oleic acid, in combination with
limewater, and are prepared simply by mixing equal
volumes of the oil and limewater
Factors that determine emulsion type
1. Emulsifier
- Some emulsifiers form either w/o or o/w emulsion,
others form only one type
2. Phase ratio
- Phase present in greater concentration tends to be
external phase
3. Order of mixing
- The phase that is being added by portions tends to
be the internal phase
Identification of emulsion type
O/W and W/O
- Miscibility test
- Conductivity test
- Dye-solubility test
o Oil soluble - Scarlet red C or Sudan III
o Water soluble - Amaranth
- Fluorescence test
o Oil fluoresces, when the whole field fluoresce –
w/o
Microemulsion
- Thermodynamically stable, optically transparent
isotropic mixtures of biphasic o/w system stabilized
with surfactants
- With droplets having the size of 100Å - 1000Å
(angstron)
- Use for more rapid and efficient delivery of drugs
following oral or transdermal drug delivery system
Phenomena associated with the physical stability are:
CREAMING
- Creaming is the upward movement of dispersed
droplets relative to the continuous phase
- Downward creaming
- These phenomena are based on the densities of the
dispersed and continuous phase
AGGREGATION AND COALESCENCE
- Aggregation (flocculation) is the coming together of
the dispersed droplets which results to creaming.
- Coalescence is the complete fusion of droplets.
Aggregation precedes coalescence
CRACKING
- Irreversible
- The coalescence of droplets results to separation of
the dispersed phase as a separate layer
- Causes of emulsion to crack or cream
o Incorporation of excess dispersed phase
o Globule size – the smaller the better
o Storage temperature
o Potential for globule coalescence
o Changes which affect the interfacial film formed
by the emulsifying agent
PHASE INVERSION
- when an emulsion changes from o/w to w/o.
- the most stable range of dispersed phase
concentration is 30% to 60%.
- If the amount of the dispersed phase approaches or
exceeds a theoretical maximum of 74% of the total
volume, then phase inversion may occur.
Dispensing of emulsion
- Emulsions can be extemporaneously prepared on a
small scale using mortar and pestle in such cases,
proper labeling should be observed during
dispensing.
- Emulsions are packed using tight, ambercolored
containers, preferably wide mouth for easy pouring.
- Emulsions should be stored at room temperature,
special labeling such as ―shake well before use‖
should be attached to the container
- Emulsions are affected by heat, cold, light, air and
microorganisms
GELS
- Sometimes called jellies.
- Semisolid system consisting of either suspension
made up of small inorganic particles or large organic
molecules interpenetrated by a liquid.
- Single-phase - macromolecules are distributed so
that no apparent boundaries exist
- Two-phase system – small distinct particles or
MAGMAS
- Transparent or translucent semi-solid or solid
preparation, consisting of solution or dispersions of
one or more active ingredients in suitable hydrophilic
or hydrophobic bases.
- It is non-greasy and generally applied externally.
- The gel contains small discrete particles - the gel is
called a two-phase system.
- If it does not appear to have discrete particles it is
called as a one-phase system.
- Two-phase systems are thixotropic
o e.g., they are semi-solid on standing but liquefy
when shaken.
o Pseudoplastic
Advantages
- As a vehicle for the presentation of water-soluble
medicaments, it is ideal because of their high-water
content.
- Products tend to be smooth.
- GELS are colloidal dispersion – 1 nm – 0.5 micron
Terminologies
- Sol – general term that refers to the dispersion of
solid substance to liquid, solid or gas; solid liquid
dispersed system
- Tyndall effect – scattering of lights
- Lyophilic – solvent loving
- Lyophobic – solvent fearing
- Imbibition – taking up of certain amount of liquid
without increase in volume
- Swelling- taking up liquid then increase in volume
- Syneresis – interaction between particles of the
dispersed phase becomes, it forms an unstable
aqueous gel there will be shrinkage
- Thixotropy- the progressive decrease in viscosity
with time for a constant applied shear stress,
followed by a gradual recovery when the stress is
removed
- Xerogel – framework; liquid is removed from the gel
and only the framework remains (e.g., tragacanth,
acacia)
Types
- Inorganic hydrogels
- Organic
- Hydrogels
- Organogels
Method of preparation: Fusion and Dispersion
Gelling agents - 6 – 10% propellant, 35-55 psig
- acacia, alginic acid, bentonite, CARBOMER, CMC - Pet products and food products
sodium, cetostearyl alcohol, colloidal silicon dioxide,
ethylcellulose, gelatin, guar gum, hydroxy Advantages
ethylcellulose, hydroxypropyl cellulose, HPMC, - Minimum contamination
magnesium aluminum silicate, maltodextrin, MC, - Maximum stability
PVA, povidone, propylene carbonate, propylene - Reduces the irritation and provides cooling effect
glycol alginate, sodium alginate, sodium starch - Easy to control physical form: particles size and form
glycolate, starch, tragacanth, and xanthan gum, - A clean process requiring no wash-up
POLOXAMERS
Principle
MAGMAS AND MILKS - Product concentrate
- Propellant
- Aqueous suspensions of insoluble, inorganic drugs - Valve assembly
and differ from gels mainly in that the suspended - pressure of the propellant forces the liquid phase up
particles are larger the tube and out in the atmosphere →propellants
- USP indicates that the term MILK is sometimes used meet the air → evaporates due to drop in pressure
for suspension in aqueous vehicles intended for oral → leaving the product concentrate as airborne liquid
administration as compared to MAGMA, which is droplets or dry particles, as in powders 🡪 equilibrium
often used to describe suspensions of inorganic acids is reestablished
such as clay in water
Pressure
AEROSOLS - is controlled by a) type and amount of propellant b)
nature and amount of product concentrate
- pressurized dosage forms that upon actuation emit a
fine dispersion of a liquid and /or solid materials Aerosol system
containing one or more active ingredients in a - Propellants
gaseous medium. - Amount
- Designed to deliver drug systemically or topically - Reactivity - Trichloromonofluoromethane→ free HCl
with the aid of liquefied or propelled gas - Physiologic effect
- Colloidal system of very finely subdivided liquid or - Environmentally safe
solid particles dispersed in and surrounded by a gas - A ban was implemented (Montreal Protocol)
regarding the use of CFCs because of the negative
Classification impact to the ozone layer, temporary exceptions for
- Formulation of the product - Systemic or local effects CFCs in metered dose inhalers were granted and the
- Type of the valve assembly - Metered dose, dry use of acceptable hydrofluorocarbons
powder
Types of propellants
Space sprays Liquefiable gases
- Finely divided spray with particles not larger than 50 - include the saturated hydrocarbons,
um chlorofluorocarbons, hydroflurocarbons and
- 85% of propellant, 30- 45 psig (pound per square in dimethyl ether
gage) - CFCs - Propellant 114, 12, 11
- Insecticides, disinfectants, air deodorizer - HFCs – 134a, 152b
- Inhalational therapy: particles less than 6 µm or less
than 2 µm Compressed gases
Surface coating - include carbon dioxide, nitrogen, nitrous oxide
- Larger particles- coarse spray - higher initial pressures are used with compressed
- 30 – 70% of propellant, 25- 55 psig gas-based systems as compressed gas tends to lose
- Cosmetic/dermatological preparations, household pressure over time as the product is dispensed
products resulting to the drop in pressure
Foam spray/ Aerated spray - Nitrogen: Inert, tasteless, odorless, insoluble
- Foams, paste and creams - Carbon dioxide, nitrous oxide: Slightly soluble
Aerosol system
Two-phase
- Liquid phase
- Vapor phase
Three-phase
- Water-immiscible propellant
- Product concentrate
- Vapor phase
Container valve assembly
- Pressurized container – tin-plated, aluminum,
stainless steel, glass or plastic
- Valve – expels the contents from the container in the
desired form at the desired rate
- Actuator – button that activates the system,
contributes in the discharged product’s physical form
- Stem – supports the actuator and delivers the
formulation in the proper form to the chamber of the
actuator
- Gasket –prevents the leakage when the valve is
closed
- Spring – holds the gasket in place and the mechanism
by which the actuator retracts when pressure is
released 🡪 valve in close position
- Mounting cup – holds the valve in place
- Housing – links the dip tube, the stem and the
actuator
- Dip tube – the tube that delivers the content
Inhalation Devices
METERED DOSE INHALER
- metering valves are used for potent medication is
required in inhalation therapy.
- In this device the amount of material discharged is
regulated by an auxiliary valve chamber by virtue of
its capacity or dimension
- Controlled by dual valve mechanism
DUAL VALVE MECHANISM
- Actuator is closed 🡪 chamber is sealed from
atmosphere but open to the container to be filled
with the contents 🡪 Press the actuator 🡪 the chamber
closes from the contents in the container and
releases its pre-filled content
NEBULIZER
DRY POWDERED INHALER
MDI vs DPI
- MDI’s energy for generating a dose relies on the
device, DPI relies on energy provided by the patient’s
inspiratory effort
Filling Methods
COLD FILLING
- Both the product concentrate and the propellant
must be cooled to temperatures of -34.5°C and -40°C
o Gas is liquefied
- Metered into the cold container
- Not suitable for aqueous systems
o Ice
PRESSURE FILLING
- Product concentrate is placed in the container and
the propellant, liquefied gases, is metered into the
valve stem.
- This is the method commonly used in pharmaceutical
aerosols
- Less danger of moisture contamination
- Less propellant is lost
Tests
- Tests for leaks and weakness at 130 F
- Proper functioning of the valve
- Particles size distribution
- Accuracy and reproducibility using metered valve
Packaging and Labeling
- Packaging is part of the manufacturing process
- Labeling uses the shrink wrap labels or peelaway
labels
- Use warning labels whenever required
- ‘Avoid inhaling except for preparations intended for
inhaling
- Do not puncture of incinerate container
- Storage condition: 15 and 30°C
- Shake before use and proper angle and distance for
use are also included in the label
Why a Curved Bottom?
- The shape strengthens the structure of the can
- The shape makes it easier to use up all the product
 STERILE DOSAGE FORMS AND DELIVERY SYSTEMS
- Parenterals: outside the intestine
- Biologicals
- STERILE: free from pyrogens (fever causing bacteria),
endotoxin
PARENTERAL PREPARATION
- pharmaceutical dosage forms that are injected
through one or more layers of skin.
- Sterile preparation: pure, free from toxicity and free
from contamination
- Pyrogen-free
Advantages
- Immediate action is provided
- Modification of the formulation allowing the drug to
be administered slowly or with prolong duration of
action
- Therapeutic response is more readily controlled
- When administered by a professional can provide
actual and accurate dose
- For drugs which cannot be administered or taken
orally
Disadvantages
- Requires aseptic technique
- Results to psychological pain factor
- Requires a professionally trained person to
administer
PARENTERAL ROUTES OF ADMINISTRATION
Injection dependent routes (Sterility Demanding Route)
- limited to solutions, suspensions, and emulsions
- limited volumes of formulation that can be injected
- excessive injection volumes will cause pain and cell
necrosis.
- Injection independent
- intranasal, inhalation, and ophthalmic routes
PARENTERAL ROUTES
INTRAVENOUS
- the veins of the antecubital area, and some of the
larger veins in the foot
- Provide the most rapid onset of action of any
parenteral route
- Johann Daniel Major in 1662
- Highest bioavailability
- Drugs that are too irritating for intramuscular or
subcutaneous administration (e.g., chemotherapy
agents) can be given by this route.
- Placement of these devices is crucial to avoid
problems of extravasation or infiltration.
Complications
- Extravasation – pass out of vessel into the tissue,
blood, lymph
- Infiltration – into a substance, cell or tissue
- VESICANTS: blistering
Thrombosis
- Clotting within a blood vessel
- Caused by factors: extremes in solution pH,
particulate material, irritant properties of the drug,
needle or catheter trauma, and selection of too small
of a vein for the volume of solution injected
Phlebitis
- inflammation of the vein
- Caused by the same factors that cause thrombosis.
Air emboli
- air is introduced into the vein
- a good practice is to purge all air bubbles from the
formulation and administration sets before use.
INTRAMUSCULAR
- The mid-deltoid area and gluteus medius are
common injection sites.
- No more than 5 ml of a solution should be injected
by this route.
- Drugs intended for prolonged or delayed absorption
commonly are administered intramuscularly.
- Patients generally experience more pain via IM
administration compared to intravenous
administration.
- Considered less hazardous and easier to use than the
intravenous route.
- The onset of action is typically longer than with IV
administration, but shorter than with subcutaneous
administration.
- Needles used for the injections are generally 2 inch
to 3 inches long and are generally 20 to 22 gauge in
size.
- The size of the needle must be chosen based on the
patient's deposits of fat.
- Maximum amount that can be used is 5 ml in gluteal
region, 2 ml in the deltoid of the arm
Complication INTRATHECAL
Abscesses - administration is injection into the spinal fluid; it
- is a collection of pus that has built up within the sometimes is used for antibiotics.
tissue of the body Needle Gauge
Cysts - the higher the gauge number, the smaller the
- sac-like structures, typically filled with liquid, diameter of the needle
semisolid, or gaseous material, very much like a - the higher the viscosity of the liquid, the lower the
blister. gauge size
- Other Complications: Embolism, Hematoma, Skin - the lower the gauge number, the stronger the
sloughing, Scar formation needle, resulting in less chance of bending or
breaking
SUBCUTANEOUS - the higher gauge number, the less pain or bruising
- beneath the skin layers-usually of the arm or thigh. experienced by patients
- it can be used for both short term and very long term
therapies Official Types of Injections
- loose interstitial tissues of the upper arm, the - Solutions ready for injection
anterior surface of the thigh, the lower portion of the - Dry, soluble product ready to be combined with a
abdomen vehicle just prior to use
- The site of injection is usually rotated when - Suspensions ready for injection
injections are frequently given. - Dry, insoluble products ready to be combined with a
- The maximum amount of medication that can be vehicle just prior to use
subcutaneously injected is about 1.3 mL. - Emulsions for injection
- Needles are generally 3/8 to 1 inch in length and 24
to 26 gauge. Parenteral solutions and suspensions
- Solvents or vehicles
INTRADERMAL - Added substances
- The usual site for intradermal injections is the - Specifications or standards
anterior surface of the forearm. - Production (facilities, areas)
- Needles are generally 3/8 inches long and 23 to 26 - Containers
gauge. - Labeling
- Drugs that are intradermally injected are agents for - Powders for reconstitution
diagnostic determinations, desensitization, or
immunization COMPONENTS
- 0.1 mL of solution is the maximum volume that can
be administered VEHICLES
INTRACARDIAC WATER
- administration is injection of a drug directly into the - is the vehicle of the greatest importance for sterile
heart. products and especially, for parenterals since it is the
HYPODERMOCLYSIS vehicle for all natural fluids
- refers to injection of large volumes of a solution into - It must meet the requirements for water for
subcutaneous tissue to provide a continuous, injection, USP.
abundant drug supply. - Water of highest quality is prepared distillation or by
- This route occasionally is used for antibiotic reverse osmosis.
administration in children WATER FOR INJECTION
INTRASPINAL - Meets requirements for Purified Water USP plus the
- administration refers to injection into the spinal USP "Pyrogen Test"
column. - Total dissolved solid nmt 1mg/100ml
INTRA-ARTICULAR - pH 5-7
- administration means injection into a joint space. - Contain no additives
INTRASYNOVIAL - Not necessarily sterile
- administration refers to injection into the joint fluid. - Used to prepare parenteral products which are then
sterilized after preparation (used within 24 hrs)
STERILE WATER FOR INJECTION
- Meets requirements for Water for Injection USP plus
passes the USP "Sterility Test"
- Contains no additives
- Used to prepare parenterals - no further sterilization
needed
- Packaged in single dose containers (Packaged in
container not larger than 1 L)
BACTERIOSTATIC WATER FOR INJECTION
- Sterile water with antimicrobialagents
- Packaged in container not more 30 mL
- For multiple dosepreparation
- Use for preparations administered in small doses
- Not to exceed 5ml
- NOT USE FORNEONATES
SODIUM CHLORIDE INJECTION
- sterile, isotonic
- No antimicrobial agents
- Approximately 154 mEq of Na and Cl per L solution
BACTERIOSTATIC SODIUM CHLORIDE
- Contains 1 or more antimicrobials
- nmt 30 mL
- Not for use in neonates
RINGER’S INJECTION
- NaCl, KCl, CaCl2
- Sodium lactate (Lactated Ringer’s)
NON-AQUEOUS SOLVENTS
- must not be toxic, irritating or sensitizing and must
not exert adverse effect on the ingredients of the
formulation.
- most frequently used non-aqueous solvents are
glycerin, polyethylene glycol, propylene glycol, ethyl
oleate, isopropyl myristate, dimethylacetamide, and
fixed oils.
- FIXED OILS are NOT used for IV route
- USED for IM to reduce irritation, produce longer DOA
- Stability, pH, viscosity, fluidity, boiling point,
miscibility, vapor pressure, purity
- Fixed oils
o they must remain clear when cooled to 10°C
(50°F).
o They must not contain mineral oil or paraffin –
The fluidity of a vegetable oil
o They must meet stated requirements of iodine
number and saponification number.
ADDED SUBSTANCES
- solubilizers, antioxidants, chelating agents, buffers,
antimicrobial agents, tonicity contributors,
hydrolysis inhibitors, antifoaming agents
Characteristics
- Perform its function throughout the useful life of the
product
- Must be non-toxic and non-irritating
- Must not exert any adverse effect on the products,
i.e., must be compatible with all the components of
the formulation
- must not interfere with: Therapeutic efficacy, Assay
of the active therapeutic compound
ANTIBACTERIAL/ANTIFUNGAL AGENTS
- The USP states that antimicrobial agents in
bacteriostatic or fungi static concentrations must be
added to preparation contained in multiple dose
containers.
- They must be present in adequate concentration at
the time of use to prevent the multiplication of
microorganism inadvertently introduced into
preparation while with drawing portion of the
contents with a hypodermic needle and syringe.
- The most commonly used agents include:
phenylmercuric nitrate and thimerosal (0.01%),
phenol, benzyl alcohol and chlorobutanol, cresol
(0.5%), sulfite, bisulfite or metabisulfite (0.2%)
ANTIOXIDANTS
- Oxidation is the primary pathway of degradation of
which can be accelerated during thermal
sterilization.
- To protect a therapeutic agent susceptible to this
reaction, antioxidants are required.
- Inert gas
- Antioxidants
- Antioxidants used in sterile products are classified
into:
- Reducing agents- antioxidants which function by
being preferentially oxidized; e.g.: ascorbic acid,
sodium bisulfite, and metabisulfite, sodium
formaldehyde sulfoxylate, thiourea.
- Blocking agents- antioxidants which block an
oxidative chain reaction in which they are not usually
consumed; e.g.: ascorbic acid esters, butyl
hydroxytoluene(BHT) and tocopherols.
- Synergist- compounds increase the effectiveness of
antioxidants, particularly those blocking oxidative
reactions; e.g.: ascorbic acid, citric acid, citraconic
acid, phosphoric acid and tartaric acid.
- Chelating agents- those that complex with catalysts
which otherwise would accelerate the oxidative
reactions; e.g. ethylenediaminetetraacetic acid salts.
- Inert gases like nitrogen and carbon dioxide have
been used to displace oxygen from solution and
 reduced the possibility of the oxidative changes in
the formulation
BUFFERS
- Buffers are added to maintain the required pH for
many products; a change in pH may cause significant
alterations in the rate of degradation reactions
- Changes in pH may occur during storage as a result
of:
- Dissolving of glass constituents in the products.
- Release of constituents from rubber closures or
plastic components in contact with the product.
- Dissolving of gases and vapors from the air spaces in
the container or by diffusion through the rubber or
plastic component.
- Reactions within the product.
- The principal buffer systems used to stabilize pH are
the acetates, citrates and phosphates.
TONICITY CONTRIBUTORS
- Compounds contributing to the isotonicity of a
product reduced the pain of injection in the areas
with nerve endings. Buffers may serve as tonicity
contributors as well as stabilizers for the pH.
STERILIZATION
- Thermal – Moist and Dry heat
- Chemical
- Radioactive
- Mechanical
Steam Sterilization (Moist heat)
- Steam under pressure
- Denaturation and coagulation
- Temperature and time
- 10 lb pressure for 30 mins (115.5 C)
- 15 lb pressure for 20 mins (121.5 C)
- 20 lb pressure for 15 mins (126.5 C)
Moist heat Sterilization
- Moist heat sterilization is the most widely used and
reliable sterilization method.
- Microorganisms are destroyed by cellular protein
coagulation.
- The objects to be sterilized are exposed to saturated
steam under pressure at a minimum temperature of
121°C for at least 15 minutes.
- Because it does not require as high a temperature,
moist heat sterilization causes less product damage
compared to dry heat sterilization.
- Autoclave -commonly is used for moist heat
sterilization.
- Exposure time must consider the penetration of
moist heat into the load
- Used for heat-stable materials
o Bulk solutions
o Glassware
o Medical devices
o Surgical dressing
o Not for oils, fats, oleaginous preparations
Dry heat sterilization
- Dry heat
- 150 – 170 C, not less than 2 hours
- Dehydration followed by oxidation
- Temperature and time
- Objects are subjected to a temperature of at least
160°C for 120 minutes (if higher temperatures can be
used, less exposure time is required).
- Oven
- Used for heat-stable materials which cannot be
sterilized by moist heat
o Fixed oils
o Glassware
o Medical devices, instruments
Sterilization by Filtration
- Non thermal method based on the removal of
microorganisms by adsorption on filter medium
- Filters with varying pore size
- Millipore filter – 14 t0 0.025 um
- 6.5 um RBC
- 0.2 um Bacteria
- 0. 025 um poliovirus
Depth filter
- usually consist of fritted glass or unglazed porcelain-
substances that trap particles in channels.
Screen Filter
- Membrane filter: Cellulosic materials (acetate,
nitrates, fluorocarbonate, acrylic polymers,
polyester, PVC, vinyl, nylon, polytef)
- Particulate filter remove particles of glass, plastic,
rubber,and other contaminants
- Final Filter which may be either particulate or
microbial, arein-line filters used to remove
particulates or microorganisms from an intravenous
solution before infusion.
- Used for small quantity of solutions
- Inexpensive
- Allows removal of microorganisms
- Disadvantages include:
o Membrane tend to be fragile
o Requires validation of compatibility and
integrity
o Limited to small volumes
 o Nature of the filter
o Particle size of the drug
Gas sterilization
- In this method, ethylene oxide or propylene oxide is
generally used in combination with heat and
moisture
- used to sterilize surfaces and porous materials (e.g.,
surgical dressings) that other sterilization methods
may damage.
- Affected by time, temperature, gas concentration,
humidity
o Low temperature requires longer exposure
- Residual gas must be allowed to dissipate after
sterilization and before use of the sterile product
- Interference with bacterial cell metabolism
- Used in medical devices and supplies, heat-labile
enzyme preparations, antibiotics
Radioactive Sterilization
- Radioactive sterilization is suitable for the industrial
sterilization of contents in sealed packages that
cannot be exposed to heat (e.g., prepackaged
surgical components and some ophthalmic
ointments).
o This technique involves irradiation causing
cellular destruction
- Accelerated drug decomposition sometimes results.
Validation of sterility
- Media fills are growth medium which support the
growth of the contaminating microbe, and this
growth can be detected using a biologic indicator –
resistant
- B. stearothermophilus – steam and gas sterilization
- B. subtilis – dry heat
- B. stearothermophilus, subtilis and pumilus –
ionizing radiation
- P. diminuta – membrane filtration
- Thermal death time for thermal sterilization (F value)
o Time required to kill a particular organism under
specified conditions
PYROGEN Testing
- Pyrogens are lipid substances associated with a
carrier molecule, which is usually a
lipopolysaccharide but maybe a protein.
- product of a metabolism of microorganism such as
most bacteria, many molds and viruses.
- ENDOTOXINS – gram (-) bacteria
- Bacterial Endotoxin test
- This is a test for estimating the concentration of
bacterial endotoxins
- Endotoxins react with enzyme Limulus Amebocyte
Lysate (LAL) forming gel-clot formation
- LAL are obtained from aqueous extracts of the
circulating amebocytes of the horseshoe crab,
Limulus polyphemus
- The pyrogen test using rabbit is the Quantitative
Fever response test
o designed to limit to an acceptable level the risk
of febrile reaction in the patient to the
administration, any injection, of the product
concerned.
Rabbit Test
- Inject into an ear vein of each of three rabbits 10 mL
of the product per kilogram of bodyweight,
completing each injection within 10 minutes of the
start of administration. Record the temperature at
30-minute intervals 1 to 3 hours subsequent to the
injection.
- If no rabbit shows an individual rise in temperature
of 0.5°C or more, the product meets the
requirements for the absence of pyrogens.
- If any rabbit shows an individual temperature rise of
0.5°C or more, continue the test using five other
rabbits.
- If not more than three of the eight rabbits show
individual rises in temperature of 0.5°C or more and
if the sum of the eight individual maximum
temperature rises does not exceed 3.3°C, the
material under examination meets the requirements
for the absence of pyrogens.
Destroying pyrogens
- may be destroyed or eliminated through physical,
chemical or a combination of both means.
Depyrogenation methods are as follows:
- Adequate washing with detergent treatment
followed by dry heat sterilization.
- Distillation is the most reliable method of eliminating
pyrogens from water.
- Removal of pyrogens by selected adsorbents has
limited use because of the concurrent phenomenon
of adsorption of solute ions of molecules
- Use of oxidizing agents
General Process of parenteral production
- procurement and selection of the components
- production facilities and procedure
- quality control
- packaging handling
Parenteral solutions/ suspensions
- Solute → dissolved→ Filtration → packaged →
sterilization
- Particle size reduction → suspending the material →
sterilization → packaging
- Dry solids → sterilized → packaged
Production
- A cleanroom is to be a separate room that contains
laminar airflow hoods and meets certain standards
of airborne particle concentration.
Clean Room
- Positive pressure airflow, uniform velocity
- Counters as stainless steel
- Walls and floors are non-porous (epoxypainted), no
cracks, no crevice and with rounded corners
- Personnel wear special suit (cover-all gowns and
shoe cap, mask and gloves)
- Class 100 – less than 100 particles of 0.5 micron size
per cubic foot – (HEPA) filter – air is filtered through
a high efficiency particulate air filter, removing
99.97% of all particles 0.3 microns or larger
- DOP smoke test – efficiency of HEPA filters using
anemometer and particle counters
- Vertical and Horizontal Laminar Flow hood
Laminar flow hood
- Laminar flow hoods are used to control airborne
contamination of sterile products during their
extemporaneous preparation
Filtration and Filters
- Filtration is used to remove particles from solutions.
- Filtration is not a "terminal sterilization" procedure
as are steam (moist heat), dry heat, ionized radiation,
or gas sterilization.
- Filtration will sterilize the product, but after
filtration, the sterile product is then aseptically
combined with its packaging.
Sterilization by Filtration
- Depth Filter: matrix of randomly oriented fibers in a
maze of flow channels
- Screen Filter: rigid, uniforms continuous mesh of
polymeric material with pore size precisely
determined during manufacture
Packaging, labeling and storage
- Parenteral solutions are packaged as large volume
parenteral (LVP) solutions and small volume
parenteral (SVP) solutions
LVP
- Common uses: 1) correction of electrolyte and fluid
balance disturbances; 2) nutrition; and 3) vehicle for
administering other drug
- Large volume parenteral solutions are packaged in
containers holding 100 ml or more
- Packaged in glass bottles or plastic bags
Maintenance Therapy
- When patients are unable to take oral nutrition or
fluids for slightly longer periods,
- If oral feeding must be deferred for
- TPN or TNAs- carbohydrates, protein, fat,
electrolytes, trace elements—mixed in a single
plastic IV bag for convenient administration
Replacement Therapy
- Heavy loss of water and electrolytes due to severe
diarrhea, vomiting
- Chrohn’s disease, AIDS, burns or trauma
Electrolytes
- Potassium, the primary intracellular cation, is
particularly important for normal cardiac and
skeletal muscle function.
- The usual daily intake of potassium is about 100 mEq
and the usual daily loss is about 40 mEq
- Sodium, the principal extracellular cation, is vital to
maintain normal extracellular fluids.
- Average daily intake of sodium is 135 to 170 mEq (8
to 10 g)
- Chloride, the principal anion of the extracellular
fluid, is usually paired with sodium.
- Chloride is also important for muscle contraction,
balancing the fluid levels inside and outside the cells,
and maintaining the acid-base balance of the
extracellular fluid
- Caloric requirement: Generally, patients requiring
parenteral fluids are given 5% dextrose to reduce the
caloric deficit that usually occurs in patients
undergoing maintenance or replacement therapy
Plastic bags
Advantages over glass bottles:
- they do not break; they weigh less
- they take up less storage space
- they take up much less disposal space.
Disadvantages
- Adsorption of drugs into the plastic.
- Leaching of a plasticizer out of the plastic
- Plastic bags are available in different sizes. The most
common sizes are 250, 500, and 1,000 m
Glass bottles
- The major advantage of glass bottles is to administer
drugs that are incompatible with plastic bags.
- Glass intravenous bottles are packaged with a
vacuum, sealed with a solid rubber closure, and the
closure is held in place by an aluminum band
SVP
- Small volume parenteral (SVP) solutions are usually
100 ml or less and are packaged in different ways
depending on the intended use.
- If the SVP is a liquid that is used primarily to deliver
medications, it is packaged in a small plastic bag
called a minibag of 50 - 100 ml (minibags look like
small plastic LVP bags).
- SVPs can also be packaged as ampules, vials, and
prefilled syringes.
Ampule
- Ampules are sealed glass containers with an
elongated neck that must be broken off.
- Most ampules are weakened around the neck for
easy breaking or if not, it must first be scored with a
file
- Filtration is done when using solutions from ampule
- In addition, it is useful to wrap an alcohol wipe or
small piece of gauze around the top of the ampule
before breaking it.
- Types: Pull seal, Tip seal
- Disadvantages: Their unsuitability for multiple-dose
use, the need to filter solutions before use, and other
safety considerations have markedly reduced
ampule use.
Vials
- Vials are made of glass or plastic and are sealed with
a rubber stopper.
- Vials may be designated for single-dose or multidose
use.
- Advantages: Vials can be designed to hold multiple
doses (if prepared with a bacteriostatic agent). It is
easier to remove the product from vials than from
ampules. Vials eliminate the risk of glass particle
contamination during opening
- Disadvantages: The rubber stopper may become
cored causing a small bit of rubber to enter the
solution. Multiple withdrawals (as with multiple-
dose vials) may result in microbial contamination.
Some drugs that are unstable in solution are
packaged in vials unreconstituted and must be
reconstituted with sterile water or sterile sodium
chloride for injection before use.
Prefilled syringes
- A cartridge type package, is a single syringe and
needle unit which is to be placed in a special holder
before use. Once the syringe and needle unit is used,
they are discarded but the holder is used again with
a new unit.
- Glass tube closed at both ends with rubber stoppers.
The prefilled tube is placed into a specially designed
syringe that has a needle attached to it. After using
this type or prefilled syringe, all of the pieces are
discarded.
Ready-to-mix systems
- Mix – O – Vial (Pharmacia)
o Example: Solu-Medrol
- ADD Vantage System (Abbott)
QUALITY CONTROL
Aseptic technique - defined as the sum total of
methods and manipulations required to minimize the
contamination of sterile compounded formulations
- Conduct all manipulations inside a properly
maintained and certified laminar flow hood. Allow
the laminar flow hood to operate for at least 30
minutes before use in order to produce a particle
free environment. Maintain a designated "clean"
area around the hood.
- Remove all jewelry and scrub hands and arms to the
elbows with a suitable antibacterial agent. Sterile
gloves are worn in addition to scrubbing.
- Wear lint-free clothing or clothing covers, head and
facial hair covers, and a mask.
- Clean all flat surfaces of the hood with 70% isopropyl
alcohol, or other antibacterial scrub such as
benzalkonium chloride solution, working from top to
bottom, then from back to front.
Sterility Test
1. Sterility tests are intended primarily as a check test
on the probability that a previously validated
sterilization procedure has been repeated.
2. The USP provides two basic methods - direct
introduction method and membrane filtration
method.
3. A product is deemed to pass the sterility test if all
media vessels incubated with product sample reveal
no evidence of microbial growth (turbidity).
4. The time for incubation for sterility testing by
membrane filtration is 7 days, less than that for
testing by direct inoculation (14 days).

Pyrogen testing
1. Pyrogens, or bacterial endotoxins, are metabolic
products of living microorganisms, or the dead
Needles
microorganisms themselves, causing a specific
- A needle has three parts, the hub, the shaft, and the
pyretic response upon injection (chemically, they are
bevel.
considered to be lipopolysaccharides).
- The hub is at one end of the needle and is the part
2. The USP pyrogen test is a qualitative fever response
that attaches to the syringe.
test in rabbits.
- The shaft is the long slender stem of the needle that
3. A more recent test is the Limulus amebocyte lysate
is beveled at one end to form a point.
(LAL) test for the presence of bacterial endotoxins,
- The hollow bore of the needle shaft is known as the
i.e., the USP Bacterial Endotoxins test
lumen.
- Needle size is designated by length and gauge.
Test for particulate matter
- The gauge of a needle, used to designate the size of
1. Light Obscuration Particle Count test
the lumen, ranges from 27 (the finest) to 13 (the
2. Microscopic Particle Count test
largest).
- There are two considerations when choosing a
DEVICES FOR ADMINISTRATION
needle size; the viscosity of the solution, and the
nature of the rubber closure on the parenteral
- The basic parts of a syringe are the barrel, plunger,
container
and tip.
- The barrel is a tube that is open at one end and
IV Infusion Pumps
tapers into a hollow tip at the other end.
- The set contains a spiked plastic device to pierce a
- The plunger is a piston-type rod with a slightly cone-
port on the IV container
shaped top that passes inside the barrel of the
- This connects to a sight or drip chamber that may be
syringe.
used to set the flow rate
- The tip of the syringe provides the point of
- Heparin lock is a short piece of tubing attached to a
attachment for a needle
needle or intravenous catheter
- Syringes come is different sizes
Dialysis solution
There are three common types of syringe tips:
- Dialysis – separation of substance from one another
1. Slip-Tips® allow the needle to be held on the syringe
in solution by taking advantage of their differing
by friction. The needle is reasonably secure, but it
diffusibility through membrane
may come off if not properly attached or if
- Peritoneal dialysis
considerable pressure is used.
- Hemodialysis
2. Luer-Lok® tips incorporate a collar with grooves that
lock the needle in place.
Radiopharmaceuticals
3. Eccentric tips, which are off-center, are used when
- These agents also represent an environmental
the needle must be parallel to the plane of injection
hazard and must be handled carefully. In addition to
such as in an intradermal injection.
adhering to the guidelines set forth for cytotoxic
agents, one may further reduce his exposure to these
agents by working with them in protective lead vial
shields
Cytotoxic Agents
- These agents present an environmental hazard. It is
now known that prolonged exposure to these agents
may lead to the development of cancers. For this
reason special precautions must be taken to
minimize the exposure of pharmacy personnel to
these agents. These agents should be prepared in a
shielded vertical flow hood, so that materials are not
blown into the operators face
Antibiotics
- Due to the allerginicity of the penicillins, it is
desirable to work with them in a shielded vertical
flow hood to avoid environmental contamination.
When working with any of the antibiotics, it is
important to remember that prolonged exposure
may lead to infections of exposed areas by
nonsusceptible bacteria and fungi
Irrigation solutions
- To bathe or wash wounds, surgical incisions or body
tissues
BIOLOGICS
- are substance derived from a living organism and
used for the prevention or treatment of disease.
- include antitoxins, bacterial and viral vaccines, blood
products and hormone extracts.
Immunity
- State of relative resistance to a disease that develops
after exposure to the specific disease-causing agent
- Natural immunity
- Acquired Immunity
- Active immunity
- Passive immunity
Immunization
- is the process by which an individual is exposed to an
agent that is designed to fortify his or her immune
system against that agent.
- The material is known as an immunogen
- human immune system 🡪 expose to an immunogen
in a controlled way 🡪 body will then be able to
protect itself from infection
- Substance used to produced immunization are
known as vaccines
- Edward Jenner originated vaccination procedure
- Dr. Raymond Parker defined a chemical nutrient
medium in which cells can grow and replicate
- Jonas Salk developed polio vaccine
- Albert Sabin polio developed the oral polio vaccine
few years later
Vaccines
- Active immunization is where the actual microbe is
taken in by a person. Antibodies are created by the
recipient and are stored permanently
- Natural active immunization - when an untreated
microbe is received by a person who has not yet
come into contact with the microbe and has no pre-
made antibodies for defense.
- Artificial active immunization - where the treated
microbe is injected into the person before they are
able to take it in naturally.
- Passive immunization is where pre-made antibodies
are given to a person.
o Immunization begins to work very quickly, but it
is short lasting, because the antibodies are
naturally broken down, and not stored for later
use.
- Natural passive immunization - when antibodies are
being transferred from mother to fetus during
pregnancy, to help protect the fetus before and
shortly after birth.
- Artificial passive immunization - given by injection
and is used if there has been a recent outbreak of a
particular disease or as an emergency treatment to
poisons.
Types of Vaccines
- Live attenuated vaccines contain bacteria or viruses
that have been altered so they can't cause disease.
- Killed vaccines contain killed bacteria or inactivated
viruses.
- Toxoid vaccines contain toxins (or poisons)
produced by the germ that have been made
harmless.
- Component vaccines contain parts of the whole
bacteria or viruses.
Live attenuated vaccines
- usually are created from the naturally occurring
germ itself.
- Viruses are weakened by growing them over and
over again in a laboratory under nourishing
conditions called cell culture.
- The process of growing a virus repeatedly-also
known as passing serves to lessen the disease-
causing ability of the virus.
Examples of live attenuated vaccines include:
- Measles vaccine (as found in the MMR vaccine)
- Mumps vaccine (MMR vaccine)
- Rubella (German measles) vaccine ( MMR vaccine)
- Oral polio vaccine (OPV)
- Varicella (chickenpox) vaccine
Inactivated (killed) vaccines
- cannot cause an infection, but they still can stimulate
a protective immune response.
- Viruses are inactivated with chemicals such as
formaldehyde.
Examples of inactivated (killed) vaccines
- Inactivated polio vaccine (IPV), which is the shot
form of the polio vaccine
- Inactivated influenza vaccine
Toxoid vaccines
- made by treating toxins produced by germs with
heat or chemicals, such as formalin, to destroy their
ability tocause illness.
- o not cause disease but they stimulate the body
toproduce protective immunity just like the germs'
natural toxins.
Examples of toxoid vaccines
- Diphtheria toxoid vaccine (may be given alone or as
one of the components in the DTP, DTaP, or dT
vaccines)
- Tetanus toxoid vaccine (may be given alone or as part
of DTP, DTaP, or dT)
Component vaccines
- made by using only parts of the viruses or bacteria.
Examples of component vaccines:
- Haemophilus influenzae type b (Hib) vaccine
- Hepatitis B (Hep B) vaccine
- Hepatitis A (Hep A) vaccine
- Pneumoccocal conjugate vaccine
PRODUCTION
- Extraction – culture, isolation
- Chemical synthesis
- GENETIC ENGINEERING
- Uses a bioreactor
Bioreactor is defined as a vessel that carries out
a biological reaction and is used to culture aerobic cells
for conducting cellular or enzymatic immobilization
Genetic engineering is the artificial alteration of
the genetic composition of cells or organisms. Gene
cloning is fundamental to genetic engineering.
- A segment of DNA from any donor organism is joined
in the test tube to a second DNA molecule, known as
a vector, to form a "recombinant " DNA molecule.
- Adjuvants – enhances the immune response of the
antigen (alum, aluminum hydroxide, aluminum
sulfate)
- Stabilizers – increase the storage life (2-
phenoxyethanol)
- Preservatives – allow the use of multiple dose vials
(Thimerosal (49.6%) is the common preservative)
- Dispensed in units of
o Total # of organism/ml or dose
o mcg of immunogen/ml or dose
o For toxoids – in flocculating units
- Biologicals are sensitive to extreme temperature
- These are kept in a biological refrigerator or an
insulated container
- Diagnostic skin biologics
o Contains antigen
o Multiple Skin Antigens
RADIOPHARMACEUTICAL
- chemical containing a radioactive isotope for use in
humans, for the diagnosis, mitigation, or treatment
of a disease
- Products should meet requirements of state agency,
FDA and NRC
Isotopes
- Any of two or more forms of chemical element,
having the same number of protons in the nucleus,
but having different number of neutrons in the
nucleus
Occurrence in Nature
- All isotopes are not equally abundant in nature
- For example, naturally occurring isotopes of
hydrogen (hydrogen-2 is the only common isotope
which has its own name, and is generally called
deuterium)
Radioactive isotopes
- Radioactive isotope or radioisotope, natural or
artificially created isotopes of a chemical element
having an unstable nucleus that decays, emitting
alpha, beta, or gamma rays until stability is reached.
- The stable end product is a nonradioactive isotope of
another element, i.e., radium- | 226 decays finally to
lead-206.
Stable isotopes
- Stable isotopes are chemical isotopes that may or
may not be radioactive, but if radioactive, have half
lives too long to be measured.
- Only 90 nuclides from the first 40 elements are
energetically stable .
- there are 255 known stable nuclides of the 80
elements which have one or more stable isotopes.
Related Terms
- Isotope — substances that have the same number of
protons but have varying numbers of neutrons
- Radioisotope — an isotope of an element that emits
alpha, beta or gamma radiation during its decay into
another element
- Radioactive — substance that emit energy in the
form of alpha, beta or gamma rays. Naturally
occurring radioactive elements include radium and
uranium
RADIOACTIVE DECAY
- Half-life - the time required for a radioisotope to
decay to 50% of its original activity
- dis transformation or decay constant ~ HALF-LIFE of
a particular radionuclide is PARTICULAR to that
radionuclide 0 IDENTITY
Units of Measure
- Curie — defined as radionuclide decaying ata rate of
3.700 x 10'9 nuclear transmission per second
- Becquerel — equal to one disintegration per second
- Radioactive dose — amount of radiation absorbed
by the body tissue in which a radioactive substance
resides (rad, Gray)
History
- Henri Becquerel (1852-1908) discovered the
existence of multiple masses for the same element
when he realized a product of uranium's radioactive
decay, ionium, was unable to be retrieved again by
chemical means from the element thorium.
- Because chemical uniqueness is a defining
characteristic of an element, it had to be concluded
that ionium was not a new element, just a different
variation of thorium.
Types of Decay
- An atom of a radioactive isotope will spontaneously
decay into another element through one of three
common processes:
- Alpha decay
- Beta decay
- Spontaneous fission
Types of Radioactivity
- An alpha particle is a helium nucleus.
- An beta particle is an electron.
- A gamma particle is a high energy photon.
ALPHA
- Spontaneously throw off an alpha particle.
- An alpha particle is made up of two protons and two
neutrons bound together
- Composition: identical to helium nucleus
- Velocity: low velocity, 1/10 the speed of light or
10,000 miles per second
- Penetrating power: low
- How to stop penetration: paper or layer of human
skin
- Hazards to the body: not hazardous unless
swallowed or inhaled
Alpha decay(a)
- In alpha decay, the nucleus emits an alpha particle;
an alpha particle is essentially a helium nucleus, so
it's a group of two protons and two neutrons. A
helium nucleus is very stable.
BETA
- Positron
- In beta decay, a neutron in the nucleus
spontaneously turns into a proton, an electron, and
a third particle called an antineutrino
- Composition: identical to electron
- Velocity: greater velocity than alpha
- Penetrating power: moderate
- How to stop penetration: wood block, aluminum
plate
- Hazards to the body: cause damage to skin and eyes
Beta Decay(f)
- A beta particle is often an electron, but can also be a
positron, a positively-charged particle that is the
anti-matter equivalent of the electron. If an electron
is involved, the number of neutrons in the nucleus
decreases by one and the number of protons
increases by one.
GAMMA
- Atom actually splits instead of throwing off an alpha
or beta particle: Neutron radiation
- Composition: high energy radiation
- Velocity: equal to velocity of light (3 x 101° cm/s)
- Penetrating power: high
- How to stop penetration: several layers of blocks of
Pb
- Hazards to the body: affect the genes causing
mutations
Gamma Decay (ry)
- The third class of radioactive decay is gamma decay,
in which the nucleus changes from a higher-level
energy state to a lower level. Similar to the energy
levels for electrons in the atom, the nucleus has
energy levels.
Types of Radiation
- Nuclear medicine depend on radiopharmaceuticals
that decay by gamma emission e
- Radiopharmaceuticals are produced by the process
of nuclear activation in a nuclear reactor
- Uses of radiopharmaceuticals include:
o diagnosis of disease or evaluation of progression
of disease, evaluation of drug induced toxicity
o used therapeutically
DIAGNOSTIC RADIOPHARMACEUTICALS
- are used to derive detailed description of the
morphology and dynamic functioning of the various
internal organs of the body.
- The radiopharmaceutical accumulated in an organ of
interest emit gamma radiation which are used for
imaging of the organs with the help of an external
imaging device called gamma camera.
PRINCIPLE OF NUCLEAR IMAGING TECHNIQUE
The Stepwise Procedure of Nuclear Imaging:
- Radionuclides are administered via vein or mouth
- They distribute in the body according to their affinity
for particular tissues so called target tissues
- Radionuclides emit gamma radiations
- Detected by y-scintillation camera
- Which forms images showing location of
radionuclides in the body
Examples
- Tc 99 —- ‘ideal” radionuclide for imaging
- Abscess and infection—Gallium Citrate Ga 67,
Indium In 111 Oxyquinoline
- Appendicitis—Technetium (99m Tc) Fanolesomab
- Biliary tract blockage—Technetium Tc 99m
Disofenin, Technetium Tc 99m Lidofenin,
Technetium Tc 99m Mebrofenin
- Blood volume studies—Radioiodinated Albumin,
Sodium Chromate Cr 51
- Blood vessel diseases—Sodium Pertechnetate Tc
99m
THERAPEUTIC RADIOPHARMACEUTICALS
- are radiolabeled molecules designed to deliver
therapeutic doses of ionizing radiation to specific
diseased sites (ex. Using MABs)
- The concept explains that certain radionuclides
possessing particulate emission such as alpha and
beta radiations or low-energy, low-range electrons
(Auger electrons) possess the ability to destroy
diseased tissues
Effect of Radioactive Decay
- Ionizing radiation- uranium atoms break into smaller
atoms and particles, which enter a human cell, strike
the nucleus, and damage the DNA, causing it to
divide in uncontrolled way- cancer
Radioisotopes may be used internally or externally.
- externally or as implants in sealed capsules in a
tissue, the dose could be terminated by removal of
the sources.
- internally as unsealed source: the dose cannot be
stopped by removal of the source.
The total dose in therapeutic applications may be
calculated on the ff. basis:
1. effective half- life of the isotope
2. concentration of the isotope
3. type and energy of radiation emitted.
- lodine 131 — is used both as diagnostic agent and
therapeutic agent
Methods of manufacturing radionuclide
- Nuclear Fission — Uranium iodine, molybdenum or
xenon
- Charged particle bombardment- charged particles
- Neutron bombardment — neutron (Cyclotron)
- Radionuclide generator system- parent nuclide:
short half life radionuclide.
CYCLOTRON - an apparatus in which charged atomic and
subatomic particles are accelerated by an alternating
electric field while following an outward spiral or circular
path in a magnetic field.
Positron emission tomography (PET)
- Anuclear medicine medical imaging technique which
produces a threedimensional image or map of
functional processes in the body.
- The technique was first developed by Michel
(Michael) Ter-Pogossian, Michael E. Phelps and
others at the Washington University school of
Medicine in 1975
PET principle
- Short-lived radioactive isotope are introduced to the
body emit positron After travelling up to ajfew mm.
the positron encounters and annihilates with an
electron, producing a pair of annihilation gamma
photons moving in almost opposite directions. These
are detected when they reach a scintillator material
in the scanning device, creating a burst of light which
is detected by photomultiplier tubes or silicon
avalanche photodiodes (Si APD).
Radioisotopes used in PET
- carbon-11 (~20 min)
- nitrogen-13 (~10 min)
- oxygen-15 (~2 min)
- fluorine-18 (~110 min)
- These radionuclides are incorporated into
compounds normally used by the body such as
glucose, water or ammonia and then injected into
the body to trace where they become distributed.
Such labelled compounds are known as radiotracers
Drug Antidote for Radiation Exposure
- Prussian Blue (ferric hexacyanoferrate)
- Initially used for Thallium and Cesium poisoning
- Acts by trapping the ions and preventing
reabsorption
Drugs used as interventional pharmaceutical drugs
- Acetazolamide (used in cerebral perfusion studies)
- Captopril (used in renovascular hypertension
studies)
- Dipyridamole and Adenosine (used for cardiac
imaging)
- Furosemide (used in renograms)
- Cimetidine (in diverticulum imaging)
NUCLEAR PHARMACY
- Nuclear Pharmacy is the patient-oriented service
that embodies the scientific knowledge and
professional judgment required to improve and
promote health through the assurance of the safe
and efficacious use of radioactive drugs for diagnosis
and treatment
- Nuclear pharmacy is the first specialty in pharmacy
recognized by the Board of Pharmaceutical
Specialties
The practice is composed of the following areas:
- Procurement
- Compounding
- Routine quality control procedures
- Dispensing and distribution
- Implementation of basic radiation protection
procedures
- Consultation and education
RADIOPHARMACEUTICALS USED IN MEDICINE
- Albumin Microspheres Tc 99m, In 111, In 113m, Pb
203 — used for lung imaging.
- Chromated Cr 51 Albumin Injection - detection and
quantitation of gastrointestinal protein loss and
placental localization.
- lodinated | 125 Albumin Injection — diagnostic aid
in the determination of total blood and plasma
volumes.
- Iodinated I 131 Albumin Injection – diagnostic aid in
the determination of total blood and plasma
volumes, circulation times or cardiac output and as
adjunct to other diagnostic procedures in the
detection and localization of brain tumors, in
placental localization and in cisternography.
- Iodinated I 131 Albumin Aggregated Injection –
diagnostic study of the lungs (pulmonary embolism)
by radioisotope scanning.
- Chlormerodrin Hg 197 Injection — diagnostic aid for
scanning the brain for suspected lesions and the
kidneys for anatomical and functional abnormalities.
- Chlormerodrin Hg 203 Injection — same uses as
above.
- Chromic Phosphate P 32 Injection – neoplastic
suppressant for palliative treatment of pleural and
peritoneal effusions.
- Cobalt Co 60 and Iridium Ir 192 Sources – 60 Co has
replaced radium, which is relatively expensive for
many radiation uses of the latter element.
- Cyanocobalamin Co 57 and Co 60 Capsules and
Solution – diagnostic aid to study the absorption and
deposition of Vit. B12 in normal individuals and in
patients with megaloblastic anemias.
- Ferric hydroxide In 113m – diagnostic agent for lung
imaging.
- Ferrous nitrate Fe 59 Injection – diagnostic aid for
the evaluation of the kinetics of iron metabolism.
- Ferrous Hydroxide Tc 99m – diagnostic aid in
pulmonary scintigraphy.
- Fibrinogen I 125 Injection – diagnosis and
localization of deep-vein thrombosis, the
accumulation of fibrinogen in clots is observable by
use of a radiation detector pressed to the surface of
the limb.
- Gallium Citrate Ga 67 Injection – diagnosis of lesions
of the lungs, breast, maxillary sinuses and liver by
using scanning and organ-imaging techniques. A
positive 67 Ga uptake is a potential indicator of
 certain malignancies such as lymphomas,
bronchogenic carcinoma, and Hodgkin’s disease.
- Indium Chloride In 113m Injection – blood-pool
studies, including visualization, aneurysms, and in
placental scintigraphy.
- Indium Hydroxide In 113m Injection – for liver,
spleen and bone marrow scintigraphy.
- Insulin I 125 and I 131 - in vitro assay of circulating
insulin either free or bound.
- Iodohippurate Sodium I 131 Injection – for kidney
function.
- Krypton Kr 81m – lung function, ventilation and
perfusion and radiocardiology.
- Liothyronine I 125 and I 131 – in vitro evaluation of
thyroid function.
- Levothyroxine I 125 and I 131 – study metabolism of
endogenous thyroxine, supplementing other tests of
thyroid function.
- Oleic acid I 125 and I 131, Trinolein I 125 and I 131 –
diagnostic agents for measuring fat absorption in
suspected pancreatic disease and other
gastrointestinal dysfunction.
- Pentetate Indium Trisodium In 113 Injection –
diagnostic aid for brain scanning, for studies of
glomerular filtration and for kidney imaging.
- Pentetate Indium Disodium In 111 Injection –
diagnostic aid for studies of cardiac output, for
cisternography, for evaluation of glomerular
filtration and in renal scintigraphy.
- Pentetate Ytterbium Trisodium Yb 169 Injection –
for brain and kidney imaging and for cisternographic
diagnosis of CSF rhinorrhea.
- Potassium Chloride K 42 Injection – tumor
localization and studies of renal blood flow.
- Potassium Chloride K 43 Injection – for heart
imaging.
- Rose Bengal Sodium I 131 Injection – diagnostic aid
(liver function), especially for differential diagnosis of
hepatobiliary diseases.
- Selenomehtionine Se 75 Injection – scintigraphy of
the pancreas and parathyroid glands.
- Sodium chloride Na 22 Injection – determining
circulating times, sodium space and total
exchangeable sodium.
- Sodium chromate Cr 51 Injection – biological tracer
to measure circulating red-cell volume, red-cell
survival time and whole blood volume.
- Sodium Fluoride F 18 Injection – bone imaging,
especially to define area of altered osteogenic
activity.
- Sodium Iodide I 123, I 125, I 131 – thyroid function.
- Sodium Pertechnetate Tc 99m Injection – detection
and location of cranial lesion, thyroid and salivary
glands, imaging placental localization and blood pool
imaging.
- Sodium Phosphate P 32 Solution – neoplastic and
polycythemic suppressant, diagnostic aid for
localization of ocular tumor.
- Strontium Sr 85 Injection – diagnostic aid for
scanning bones to detect and define lesions and to
study bone growth and abnormal formation.
- Technetium Tc 99m Etidrenate Injection – best
agent for bone imaging.
- Technetium Tc 99m Iminodiacetic acid (TIDA) or
Hepatobiliary Iminodiacetic acid (HIDA) –
hepatobiliary imaging agent.
- Technetium Tc 99m Ferpentate Injection – kidney
imaging.
- Technetium Tc 99m Pentetate Injection – brain and
kidney visualization, for vascular dynamic studies for
measurement of glomerular filtration and lung
ventilation studies.
- Technetium Tc 99m Pyrophosphate Injection –
skeletal imaging agent used to demonstrate regions
of altered osteogenesis.
- Technetium Tc 99m Sulfur Colloid Injection –
diagnostic aid for liver scanning.
- Technetium Tc 99m Gluceptate Injection – a renal
imaging agent and localization of brain, lung and gall
bladder lesions.
- Technetium Tc 99m sodium phosphates Injection –
bone and renal imaging.
- Technetium Tc 99m Sodium Phytate Injection – for
liver and spleen imaging.
- Thallium Tl 201 chloride Injection – myocardial
perfusion imaging for diagnosis and localization of
myocardial ischemia and infarction.
- Xenon Xe 133 Injection – as gas for lung imaging to
detect alveolar blockage.
Products of Biotechnology
Techniques used:
1. rDNA
2. Monoclonal antibodies
3. Polymerase chain reaction
4. Gene therapy
5. Antisense or Nucleotide blockade
MEDICAL DEVICES
- A medical device is an instrument, apparatus, in vitro
reagent , implant or other similar or related article,
which is intended for use in the diagnosis of disease
or other condition, or in the cure, mitigation ,
treatment , or prevention of disease or intended to
affect the structure or any function of the body and
 which does not achieve any of its primary intended
purposes through its chemical action within or on the
body
- Diagnosis, prevention, monitoring, treatment or
alleviation of disease
- Diagnosis, monitoring, treatment, alleviation of or
compensation for an injury or handicap
- Investigation, replacement or modification of the
anatomy or of a physiological process
- Control of conception
- And which does not achieve its principal intended
action in or on the human body by pharmacological,
immunological or metabolic means, but which may
be assisted in its function by such means

Classification
- Medical Devices are classified as per their risk level
and intended use

MDD-Risk Based Classification

- Class A (Class-I) – Devices involving low risk levels
- Class B (Class-II a) – Devices involving low to medium
risk
- Class C (Class-II b) – Devices involving moderate to
high risk
- Class D (Class-III) – Devices involving high risk

By USFDA
- Class-I : Elastic bandages, Examination Glove, Adult
Incontinence Pad
- Class –II: Catheter Cannula, Dialyzer , Piston syringe ,
Needle, Infusion Pumps, Bone fixation screw, Blood
pressure kit
- Class-III: Pacemakers, Dental Lasers, Heart Valves.

Registration of Medical Devices – United States

- FDA ‘APPROVAL PROCESS’ BY CLASS OF DEVICE
- Note: Approval of Class-3 Devices is complicated and
involves clinical trials. Less than 10% of devices are
considered Class-3 by the FDA
- CLASS 1: NO FDA APPROVAL NEEDED. Must register
device and company on FDA website
- CLASS 2: FDA CLEARANCE REQUIRED. Typically, via
510 K premarket notification submission
- CLASS 3: FDA APPROVAL REQUIRED. Typically via
premarket (PMA) approval process