Formulasi Sediaan Parenteral
Formulasi Sediaan Parenteral
Formulasi Sediaan Parenteral
Sediaan
Parenteral
Linda Margata
1
• involves the injection of therapeutic agents, in the form of solutions,
suspensions or emulsions, into the body
• the major barriers to drug entry (the skin) is breeched.
• There are three routes by which parenterals are most frequently
administered:
1. intravenous (IV)
2. intramuscular (IM)
3. subcutaneous (SC)
2
Intravenous route
• administration of the parenteral formulation into a vein, usually a
large proximal vein. The veins are located beneath the subcutaneous
tissue, embedded within the muscle
• achieves a rapid and predictable response
• 100% drug bioavailability.
• Both large- (up to 500 ml) and small- (up to 10 ml) volume
formulations may be administered intravenously. Large volumes are
infused into the vein at a controlled rate, e.g. total parenteral
nutrition, infusion of solutions of electrolytes/nutrients either
containing or devoid of drugs.
3
• Formulations are usually solutions or emulsions (in which the size of the disperse
phase is small, <1 µm). Suspensions (or solutions that precipitate within the blood
stream) must not be administered IV due to disruption of blood flow.
• Due to the subsequent dilution of the injected dose and the relative insensitivity
of venous walls of veins, IV administration may be employed for the
administration of drugs that would normally be too irritating if administered by
other routes.
• Care must be taken regarding the rate of administration of the parenteral
formulation. If the administration is performed too quickly, an excessive
concentration of drug at the target organ may result, leading to drug-induced
shock.
• Training is required to ensure that the dosage form is actually administered to the
vein and that puncture of the vein is avoided
4
Intramuscular route
• administration into a muscle, usually the gluteal (buttocks), vastus lateralis (lateral
thigh) or deltoid (upper arm) muscles. The musculature resides below the
subcutaneous tissue (which itself lies beneath the epidermis and the dermis).
• The volume of injection is small, usually 1–3 ml or up to 10 ml in divided doses.
• Faulty injection technique may lead to local muscle damage.
• relatively rapid absorption, second only to IV with respect to the time taken for
the onset of action.
• nature of the formulation directly affects the rate of absorption of drugs
administered by the IM route. Drug absorption from aqueous solutions is greater
than from aqueous suspension or non-aqueous (oil-based) solutions of drugs.
• usually used for controlled-release formulations.
5
Subcutaneous route
• administration into the subcutaneous tissue, a layer of fat located
below the dermis.
• slower onset of action and sometimes less total absorption of
therapeutic agents when compared to the IV or IM
• the nature of the formulation directly affects the rate of drug
absorption from this site: oily solutions or aqueous suspension of
therapeutic agents exhibit slower drug absorption
6
• volume of injection is typically circa 1 ml; however, large-volume
parenteral solutions (electrolyte or dextrose, up to 1000 ml) may be
infused subcutaneously. This technique is termed hypodermoclysis
and is only employed when there is difficulty in accessing a vein. On
some occasions hyaluronidase may be administered to increase the
available volume at the site by catalysing the temporary breakdown
of the connective tissue at the site (hyaluronic acid).
• Viscous formulations are not generally administered subcutaneously.
• Typical sites of SC injection include the arms, legs and abdomen.
• Route of choice for the administration of insulin.
7
Miscellaneous routes
1. intradermal (ID)
2. intra-arterial (IA)
3. intrathecal (IT)
4. intradural and extradural;
5. intracardiac (IC)
8
Intradermal route
• injection into the dermal layer of the skin.
• generally used for diagnostic purposes, e.g. for the diagnosis of
allergy and for the tuberculin test.
• absorption is slow and limited from this region.
• Only small volumes may be injected, circa 0.1 ml.
9
10
Intra-arterial route
• injected into an accessible artery.
• requires specialist training as if the artery is missed, possible damage
to adjacent nerves may result.
• is used to administer radiopaque media to visualise organs, e.g. heart,
kidney.
• is used to administer anticancer drugs to ensure that the highest
possible concentration of drug reaches the target organ.
11
Intrathecal (IT) route
• is used to administer
therapeutic agents to
the cerebrospinal fluid
• to ensure that the
appropriate
concentration of drug
is obtained at this site
(e.g. for the treatment
of infection).
12
Intradural and extradural routes
• is employed to achieve spinal anaesthesia.
• Intradural administration involves injection of the therapeutic agent
within the dural membrane surrounding the spinal cord.
• Extradural administration involves injection of the therapeutic agent
outside the dural membrane and within the spinal caudal canals.
13
Intracardiac (IC) route
• involves injection of the formulation directly into the muscles of the
heart.
• normally used whenever there is a cardiac emergency.
14
Advantages and Disadvantages
15
Advantages
• immediate physiological response (usually by the IV route) for acute
medical situations, e.g. cardiac arrest, anaphylactic shock, asthma.
• for drugs that offer poor bioavailability or those that are rapidly degraded
within the gastrointestinal tract (e.g. insulin and other peptides).
• method to administer drugs to patients who are unconscious or
uncooperative or for patients with nausea and vomiting (and additionally
dysphagia).
• As trained medical staff primarily administer parenteral formulations, there
is control of both the dosage and frequency of administration. The main
exception to this is the administration of insulin, which, in the absence of
complications (e.g. ketoacidosis), is performed exclusively by patients
16
• Local effects e.g. local anaesthesia.
• serious imbalances in electrolytes may be corrected (using infusion
solutions).
• offer a wide range of drug release profiles, including:
• rapidly acting formulations (IV)
• long-acting formulations (IM or SC). Examples: intermediate/long-acting
insulin formulations and steroid injections.
• nutrition may be provided using specially formulated solutions that
are infused into the patient.
17
Disadvantages
• manufacturing process is more complicated due to the requirement
for aseptic technique.
• Skill of administration is required
• associated with pain on administration
• If the patient is allergic to the formulation (the therapeutic agents
and/or the excipients), parenteral administration will result in both
rapid and intense allergic reactions.
• difficult to reverse the effects of drugs that have been administered
parenterally
18
Formulation Considerations
19
Type of preparation
• initial choice that must be made concerns the type of parenteral
formulation required, which is informed by:
1. physicochemical properties of the therapeutic agent
2. intended route of administration
3. volume to be administered
4. general preference for a particular formulation based on the perceived
pharmacological effect or onset of pharmacological effect.
5. etc.
20
Solubility of the therapeutic agent
1. Good solubility
• freely soluble in the chosen solvent (either aqueous or oil-based)
2. Moderate solubility
• use of co-solvents
• may be formulated as a suspension, although one cautionary note regarding
this approach is the potential recrystallisation of soluble drug during storage
3. Low solubility
• suspension formulation.
21
Preferred route of administration
• IV products must be aqueous solutions and must not precipitate in
the blood stream. Emulsions may also be administered by this route
provided the particle size of the internal phase is sufficiently small.
• Parenteral suspensions (aqueous or oil-based) and oil-based
parenteral solutions must be administered either SC or IM. Aqueous
solutions may also be administered IM or SC.
• other restrictions for those less commonly used routes
22
Volume of dose to be administered
• Large-volume (up to 500 ml) are administered IV (although the SC
route is infrequently used for this purpose).
• Small-volume may be administered by all routes (bearing in mind the
restrictions of oil-based and suspension formulations).
23
Onset/duration of action
• IV will have an immediate pharmacological effect. The rates of drug
absorption SC and IM are slower
• Absorption of therapeutic agents from aqueous solutions (IM or SC) is
faster than from oil-based solutions, oil-based suspensions and
aqueous suspensions:
the onset of action of soluble insulin (aqueous solution) is rapid (circa 30
minutes), peaks between 2 and 4 hours and has a duration of action of up to
8 hours.
intermediate/long-acting insulins (aqueous suspensions), have an onset of
action of 1–2 hours, a peak action between 4 and 12 hours and a duration
between 16 and 35 hours.
24
Physicochemical properties of the
therapeutic agent
• important determinants of the stability and absorption of the
therapeutic agents
• directly affect the rate of dissolution (and hence the rate of
absorption)
25
Solid-state properties
• therapeutic agents may exist in either crystalline or amorphous states
• Polymorphism refers to the ability of molecules to exist in more than one
crystalline form
• Usually one crystalline form is the stable form and the other(s) are less
stable, being referred to as metastable. Over time the metastable form(s)
will revert to the stable form.
• different polymorphic forms of a particular therapeutic agent will exhibit
different melting points and, as a result, will exhibit different dissolution
rates
• different solubilities of the different polymorphs will lead to different rates
of dissolution after IM or SC administration and hence different rates of
drug absorption
26
Solubilities of insoluble salt forms
• different salt forms exhibit different aqueous solubilities
• For example, the solubility of protamine insulin is dramatically lower
than soluble insulin. Protamine insulin greater duration of action
• The duration of action of insulin may be further enhanced by forming
a salt with zinc or with protamine and zinc, which has lower solubility
and hence a lower rate of dissolution
27
Particle size
• controls both the rate of dissolution and physical stability of
parenteral suspensions.
• rate of dissolution of a poorly soluble drug increases as the surface
area of the particle increases
• decreasing the particle size may increase the rate of dissolution of an
insoluble therapeutic agent
• A suspension of testosterone propionate (particle size range 40–100 µm)
exhibits a duration of action of 8 days following IM administration.
• A suspension of testosterone propionate (particle size range 50–200 µm)
exhibits a duration of action of 12 days following IM administration
28
• It is accepted that reducing the rate of sedimentation of the
dispersed drug particles will enhance the physical stability of
suspensions
• Increasing the particle size of the dispersed drug will both increase
the rate of sedimentation (and possibly decrease the physical stability
of the formulation)
29
Vehicle
Aqueous vehicles
• Water for injection is the major vehicle of choice for:
• freely soluble therapeutic agents (parenteral solutions)
• therapeutic agents of low aqueous solubility (parenteral suspensions)
• the external phase of parenteral emulsions.
30
Specifications of water for injection:
• appearance (clear, odourless, pH range 5–7)
• purity (limits on the mass of ions, heavy metals, oxidisable
compounds, total amount of dissolved solids < 10 ppm)
• sterility:
• Water for Injections USP non-sterile, will be terminally sterilised (i.e. during
or after the manufacture process).
• Sterile Water for Injections USP intended to be used as a vehicle for
products that have been packaged and sterilised, e.g. for the reconstitution of
antibiotic powders as solutions or suspensions
31
• must be free of pyrogens (fever-producing compounds) that are
primarily associated with Gram-negative bacteria.
effectively removed from water using either distillation or reverse osmosis.
removal of pyrogens from the storage containers is typically performed by
heating the container at either 250C for 30–45 minutes or at 180C for 3–4
hours.
32
Non-aqueous vehicles
• employed for the production of:
non-aqueous parenteral solutions of therapeutic agents that are
water-insoluble
non-aqueous parenteral suspensions of therapeutic agents that are
water-soluble and/or exhibit aqueous instability
the internal phase of parenteral emulsions.
• Fixed oils are predominantly used as non-aqueous vehicles (e.g. corn
oil, cottonseed oil, peanut oil, sesame oil); however, non-aqueous
esters may be used, e.g. ethyl ethanoate:
33
• Two major problems associated with the use of non-aqueous
pharmaceutical solutions are:
1. Pain/irritation on injection. Viscosity of fixed oils increases at lower storage
temperatures.
2. Patients may exhibit sensitivity to the oils oil used in the formulation must
be explicitly stated on the label/patient information.
• In some oily formulations, agents may be added to enhance the
solubility of the therapeutic agent in the oil vehicle (ex. benzyl
benzoate)
34
Inclusion of co-solvents
• potentially greater toxicity of co-solvents when administered parenterally
should be carefully considered
• toxicity is greater whenever administered by the IV in comparison to the IM
and SC routes.
• Examples:
• Glycerol
• ethanol (high concentrations of ethanol are known to produce pain on injection)
• propylene glycol
• polyethylene glycol 400.
• concentration of co-solvent used should be sufficient, but should not be
irritant or toxic
35
Surface-active agents
• may be incorporated into aqueous or non-aqueous (oil-based) vehicles to
enhance the solubility concentration of surface-active agent employed
will exceed the critical micelle concentration (CMC) of the surface-active
agent
• act to enhance the physical stability by adsorbing to the surface of the
dispersed therapeutic agent and preventing caking of the solid particles
concentrations of surface-active agents that are below the CMC may be
used. . It is extremely common for non-ionic surface-active agents to be
used in this manner. Examples:
polyoxyethylene sorbitan fatty acid esters (Tween series): 0.1–0.5% w/v
poly(oxyethylene)-poly(oxypropylene) block co-polymers (Poloxamers): 0.01–5%
w/v
Lecithin: 0.5–2.0% w/w
36
• choices of surface-active agent and the concentration are dependent
on the nature of the vehicle and the type of parenteral formulation
(i.e. solution or suspension).
Low hydrophile–lipophile balance (HLB) values to stabilise oil-based drug
suspensions
High HLB values to stabilise aqueous drug suspensions
• The use of surface-active agents to solubilise therapeutic agents is
commercially employed.
• Steroids have been solubilised using Tween and Span
• poorly water-soluble vitamins (A, D, E and K) may be solubilised using
surface-active agents
37
Buffers
• Control the pH of the formulation
• Maintain the solubility of the drug
• Enhance the chemical stability of the therapeutic agent
• Examples:
• acetic acid/sodium acetate,
• citric acid/sodium citrate
• sodium phosphate/disodium phosphate
38
Polymers to modify formulation viscosity
and/or drug solubility
• occurs more frequently in suspensions than in parenteral increased
formulation viscosity may result in difficulties in administration and
pain at the injection site
• restricted to aqueous solutions to enhance the solubility of the
therapeutic agent by complexation
• Example: Low molecular weight of Polyvinylpyrrolidone (PVP) (circa
12000)
• Lipophilic polymers are rarely used due to their limited availability.
• Hydrophilic polymers maintain the physical stability of suspensions.
39
Preservatives
• For multidose preparation
• For product that has not been terminally sterilised, e.g. by irradiation
or heat. Preservative is required to guard against any possible
breakdown in the aseptic manufacturing process
• Examples:
• esters of parahydroxybenzoic acid, e.g. methyl and propyl parebens are often
used in combination in a ratio of 9:1. The concentration is usually circa 0.2%
w/v
• phenolic compounds, e.g. phenol (0.25–0.5% w/v) or chlorocresol (0.1–0.3%
w/v)
40
Consideration for preservatives inclusion:
• Hydrophilic surfactants may interact with parabens preservative
efficacy are decreased. This problem is resolved by increasing the
concentration of preservative (generally up to 0.25% w/v).
• Preservatives may similarly interact with the container and closure of
the parenteral product increase in the concentration of
preservative required or, preferably, a change in the type of container
closure.
• phenol has been shown to interact with rubber closures the rubber closure
may be exchanged with a suitable replacement, e.g. nitrile closures.
41
• Preservative must not adversely affect the chemical and physical
stability of the parenteral product. Ex: physical stability of zinc insulin
is compromised in the presence of phenol (but not methyl paraben).
• Preservative is required in the aqueous phase of the emulsion to
exert the antimicrobial effect. Distribution between the oil and
aqueous phases will therefore decrease the concentration of
preservative in the aqueous phase reduce the preservative efficacy.
To overcome this, the concentration of preservative in the dosage
form should be increased.
42
• Oil-based parenteral products (solutions and suspensions) do not
generally require the inclusion of a preservative due to the low water
activity of this medium
• potential toxicity of preservatives. It is therefore desirable to avoid
the inclusion of preservatives whenever possible
43
Agents to modify the osmolarity of
parenteral products
• Osmolarity: the mass of solute that, when dissolved in 1 litre of
solution, will produce an osmotic pressure equivalent to that
produced by a one-molar (1 mol) solution of ideal unionised
substance
• units for osmolarity: mosmol/kg
• isotonic solution: same effective osmotic pressure as blood serum
• hypotonic solution: solution in which the osmotic pressure exerted by
the solution is less than blood serum
• hypertonic solution: solution in which the osmotic pressure exerted
by the solution is greater than blood serum
44
• In the presence of a hypotonic solution, red blood cells will swell (due
to water entry into the cell) and eventually burst (termed haemolysis)
• in the presence of a hypertonic solution, water will leave the red
blood cells, leading to crenation.
• IV administration of parenteral should be isotonic (circa 291
mosmol/l) to avoid potential damage.
• However, many parenteral products designed for IV administration
are hypertonic. Products within the osmolarity range of 300–500
mosmol/l may be administered by the IV route rapidly
45
• Parenteral formulations designed for IV administration should not be
hypotonic.
• Compounds that will increase the osmotic pressure of the solution:
sodium chloride or dextrose
• There are two methods by which the mass of these compounds
required to render the solution isotonic may be calculated:
1. consideration of the gram-molecular concentration; and
2. consideration of the freezing-point depression of the solution.
46
47
48
49
50
51
52
53
Antioxidants
• Oxidation may occur due to:
1. the action of molecular oxygen; however, this is a slow process, especially in
aqueous solution in which the concentration of dissolved oxygen is low
2. facilitated by free radicals, with breakdown occurring via a chain reaction process.
• Radicals are formed due to the action of light, heat or transition metals
(e.g. iron, copper) that are present in the formulation.
• Antioxidants are included in parenteral formulations to slow down or
inhibit oxidative degradation of therapeutic agents.
butylated hydroxyanisole (BHA)
butylated hydroxytoluene (BHT)
sodium metabisulphite
sodium formaldehyde sulphoxylate
54
• Chelating agents, e.g. ethylenediamine diacetic acid (EDTA), may be
added to extract dissolved transition metals
• Flushing the injection container/vial with nitrogen prior to closure
to remove oxygen (but require the availability of specialised filling
equipment)
55
Parenteral emulsion
• Whilst two forms of emulsion exist, water in oil (w/o) and oil in water
(o/w), it is the latter type (o/w) that is usually administered
parenterally.
• Several problems associated with the use of parenteral emulsions:
1. limited list of surfactant (due to toxicity concerns).
2. droplet size must be <1 µm to prevent blockage of blood flow. The physical
instability of emulsions coalesce potential dangerous
3. difficult to sterilise. Normal sterilisation methods (heat and filtration) are
generally inappropriate
56
Manufacture of parenteral formulations
• Two essential requirements:
1. Sterility
2. Absence of pyrogens
• Sterilisation: the absence of viable microorganisms (either through the
destruction of all living microorganisms or by their removal) in
pharmaceutical preparations.
• Sterilisation methods:
1. moist-heat sterilisation
2. dry-heat sterilisation
3. filtration sterilisation
4. sterilisation by exposure to ionising radiation
5. gas sterilisation
57
Moist-heat sterilisation
• performed in an autoclave and employs steam under pressure
• lower temperatures than dry-heat sterilization
• denaturation/coagulation of microbial proteins
• pressure in the autoclave is increased to enable an increase in the
processing temperature
• at 103.4 kPa (i.e. 15 pounds per square inch) and 121°C sterilisation is
achieved in 20 minutes
• at 68.91 kPa (10 pounds per square inch) sterilisation is achieved in
30 minutes.
58
• used to sterilise materials that are both thermostable and through
which moisture can perfuse. These include:
glassware
dressings
closures
aqueous solutions (assuming that the therapeutic agent is thermostable)
59
Dry-heat sterilisation
• microorganisms are destroyed following cellular dehydration and
then pyrolysis/oxidation.
• performed in ovens
• performed at higher temperatures and requires longer times of
exposure of the microorganism to this temperature:
170°C for 1 hour
160°C for 2 hours
140°C for 4 hours.
60
• to sterilise materials/products that cannot be readily sterilised by
moist heat and which are thermostable following exposure to the
sterilisation cycle) e.g.:
oils and other aqueous vehicles (e.g. glycerin, propylene glycol)
heat-stable therapeutic agents/excipients
glassware (e.g. bottles).
61
Filtration sterilisation
• microorganisms are removed (not destroyed) using sterilising filters
of pore diameter 0.22 µm
• solution is passed through a series of clarifying filters of defined
diameter, e.g. 1 µm, 0.45 µm, prior to passage through the sterilising
filter To maximise the lifetime of the filter
• Used for therapeutic agents that are thermolabile
• Efficient and inexpensive
• Possible concern: the product being nonsterile due to a flaw in the
manufacture
62
Sterlisation by exposure to ionising radiation
• gamma radiation (25–40 kGy)
• requires specialist equipment expensive
• Used for parenteral formulations that are manufactured and
packaged under aseptic conditions but are neither terminally
sterilised nor sterilised by filtration
• effects of ionising radiation on the stability of formulation ingredients
must be individually examined
63
Gas sterilisation
• mixtures of ethylene oxide or propylene oxide and an inert gas, e.g.
carbon dioxide
• efficiency increases in the presence of moisture (up to 60%) and
elevated temperature (circa 55°C)
• highly penetrative nature frequently used for medical devices (e.g.
packaged catheters) and porous surgical accessories (e.g. blankets)
• toxicity of the gas mixture sufficient time must be allowed after
sterilisation to enable the sterilising gas to be desorbed
64
Specific manufacturing
requirements
65
Aqueous parenteral solutions
• formulation components (including the therapeutic agent) are
dissolved in the main mixing vessel
• Thermostable drug formulation is filled into the final containers and
sealed. Sterilisation performed using moist-heat sterilization.
Inclusion of preservatives in multidose product.
• Thermolabile drug product is sterilised using filtration and collected
into a second mixing vessel, from which filling into the final container
is performed.
66
Oil-based parenteral solutions
• Moist-heat sterilisation cannot be used to sterilise oil-based solutions
• main steps involved in the manufacture:
Sterilisation of the oil-based vehicle (containing the various soluble
excipients) within the mixing vessel in the aseptic manufacturing suite
(performed using dry-heat sterilisation)
If the therapeutic agent is thermolabile, sterile drug should be dissolved in
the sterile oil-based vehicle using normal mixing facilities
67
Aqueous parenteral suspensions
• filtration cannot be performed to render the product sterile
• sterile drug must be added to the chosen vehicle and suitably
dispersed under aseptic conditions
68
• Main steps in the manufacture of aqueous parenteral suspensions:
1. dissolution of the formulation excipients
2. sterilisation of the vehicle by filtration
3. dispersal of the (sterile) therapeutic agent into the sterile vehicle. Particle
size may be reduced by passage through a ball mill
4. Filling into the final container, followed by sealing
5. formulation may be followed by terminal sterilization (moist-heat
sterilization), if stable.
69
Oil-based parenteral suspensions
• Main steps in manufacturing:
1. sterilisation of the oil-based vehicle (+ soluble excipients) performed using
dry-heat sterilization
2. mixing of the sterile therapeutic agent
3. filling into and sealing the final container
4. may be sterilised using dry heat, if formulation is stable
70
71