Principle, Advantages, Disadvantages, Application S of Different Sterilisation Methods and in Process Control
Principle, Advantages, Disadvantages, Application S of Different Sterilisation Methods and in Process Control
Principle, Advantages, Disadvantages, Application S of Different Sterilisation Methods and in Process Control
DISADVANTAGES, APPLICATION
S OF DIFFERENT STERILISATION
METHODS AND IN PROCESS
CONTROL
PREPARED BY
KOSARAJU SAI VIVEK
I M.PHARMACY,
DEPARTMENT OF PHARMACEUTICS
Jss college of pharmacy
contents
1. WHAT IS STERILIZATION
2. METHODS OF STERILIZATION
3. MERITS, DEMERITS
ANDAPPLICATIONS OF DIFFERENT
METHODS OF STERILIZATION
4. PHARMACEUTICAL IMPORTANCE OF
STERILIZATION
5. PHARMACEUTICAL IN PROCESS
CONTROL
WHAT IS STERILIZATION:
It is a useful Undesirable
Radiation sterilization is
method for the changes occur in
Radiation generally applied to articles
2 Ionization of industrial irradiated
sterilization in the dry state; including
nucleic acids sterilization of products,an
surgical instruments,
heat sensitive example is
sutures, prostheses, unit
products aqueous solution
dose ointments, plastics
where radiolysis
of water occurs.
S.n METHOD MERITS DEMERITS APPLICATIONS
o MECHANISM
1 Filtration Does not destroy It is used for both Does not This method is Sterilizing
sterilization but removes the the clarification and differentiate grade filters are used in
microorganisms sterilization of between viable the treatment of heat
liquids and gases as and non viable sensitive injections and
it is capable of particles ophthalmic solutions,
preventing the biological products and
passage of both air and other gases for
viable and non supply to aseptic areas
viable particles
Pharmaceutical Importance of
Sterilization
• Moist heat sterilization is the most efficient biocidal
agent. In the pharmaceutical industry it is used for:
Surgical dressings, Sheets, Surgical and diagnostic
equipment, Containers, Closures, Aqueous injections,
Ophthalmic preparations and Irrigation fluids etc.
• Dry heat sterilization can only be used for thermo
stable, moisture sensitive or moisture impermeable
pharmaceutical and medicinal. These include products
like; Dry powdered drugs, Suspensions of drug in non
aqueous solvents, Oils, fats waxes, soft hard paraffin
silicone, Oily injections, implants, ophthalmic
ointments and ointment bases etc.
• Gaseous sterilization is used for sterilizing
thermolabile substances like; hormones,
proteins, various heat sensitive drugs etc.
• U.V light is perhaps the most lethal
component in ordinary sunlight used in
sanitation of garments or utensils.
• Gamma-rays from Cobalt 60 are used to
sterilize antibiotic, hormones, sutures, plastics
and catheters etc.
Filtration sterilizations are used in the
treatment of Heat sensitive injections and
ophthalmic solutions, biological products, air
and other gases for supply to aseptic areas.
They are also used in industry as part of the
venting systems on fermentors, centrifuges,
autoclaves and freeze driers. Membrane filters
are used for sterility testing.
PHARMACEUTICAL IN
PROCESS
CONTROL
In-process controls (IPC) are checks that are
carried out before the manufacturing process
is completed.
The In-Process Quality Control system lays
emphasis on the responsibility of
manufacturers processors in ensuring
consistency in quality during all stages of
production by adopting quality control drills
and exercising control on raw materials and
bought-out components, manufacturing
process, packing and final testing.
In-Process Quality Control tests of
tablets
• SIZE & SHAPE
• TABLET THICKNESS
• COLOUR
• HARDNESS
• FRIABILITY
• POTENCY & CONTENT UNIFORMITY
• WEIGHT / WEIGHT VARIATION
• DISINTEGRATION TIME
BLENDING:
Blend Uniformity:
Not less than 90.0 % and not more than110.0
1 Particulate matter
2 Uniformity of content
3 Extractable volume
4 Sterility
5 Pyrogens
6 Uniformity of weight
7 Clarity of solution
8 Leakage
Particulate matter
Parenteral preparations including solutions
constituted from sterile. solids are expected to be
free from particles of approximately 50 μm or
more that can be observed byinspection with the
unaided eye
Particulate matter
Sterility
Culture Media
MEMBRANE FILTRATION.
After transferring the contents of the container or
containers to be tested to the membrane add an
inoculum of a small number of viable micro-organisms
(not more than 100 CFU) to the final portion of sterile
diluent used to rinse the filter.
After filtration, aseptically remove the membrane(s)
from the holder, transfer the whole membrane or cut it
aseptically into 2 equal parts. Transfer one half to each
of two suitable media.
Direct Inoculation. After transferring the contents of
the container or containers to be tested to the culture
medium add an inoculum of a small number of viable
micro-organisms (not more than 100 CFU) to the
medium
Quantity in each container Minimum quantity to be
used
Less than 1 ml Total contents of a
container
40 ml or more but less than 1 ml or more but less than
100 ml 20 ml 40 ml Half the
contents of a container