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1
A Concise Presentation
By
Mr. Deepak Sarangi M.Pharm
 DEFINITION
 MECHANISM OF DRUG ABSORPTION THROUGH SKIN
 FUNDAMENTALS OF SKIN PERMEATION
 FACTORS AFFECTING TRANSDERMAL PERMEABILITY
 PERMEATION ENHANCERS
 TYPES
 ADVANTAGES
 DISADVANTAGES
 CONCLUSION
 REFERENCES
2
Transdermal therapeutic are defined as self contained
discrete dosage form which when applied to the intact skin
deliver the drugs, through the skin, at a controlled rate to the
systemic circulation.
(or)
Transdermal drug delivery system (TDDS) are systems
that utilize skin as a site for continuous drug administration
into the systemic circulation.
3
 Epidermis
a) Stratum corneum
b) Stratum lucidum
c) Stratum granulosum
d) Stratum spinosum
 Dermis
 Subcutaneous
4
a) Transfollicular route
Transfollicular route is the shortest pathway that drug has to follow
to reach the systemic circulation that provides a large area for
diffusion of drugs.
b) Transcellular route
Drug delivering through this route passes from corneocytes which
has highly hydrated keratin creating hydrophilic pathway.
The drug passes through the corneocytes of stratum corneum.
c) Intercellular route
In intercellular pathway the drug diffuses through the
continuous lipid matrix present between the cells.
5
Rate of permeation, dQ/dt, across a skin can be expressed as
dQ/dt = Ps[ cd - cr ]
Where,
dQ/dt – Rate of permeation
Ps – Permeability coefficient
Cd – Concentration in donor compartment
Cr – Concentration in receptor compartment
6
The principle transport mechanism across mammalian skin
is by passive diffusion. The factors influencing and having
differences in transdermal permeability of the stratum
corneum.
Lipid solubility:
At higher concentrations, the rate of penetration of the
alcohols is greatly increased, and does not follow the pattern
of absorption from weak solution.
But, high concentrations may damage the stratum corneum
impairing its 'barrier' properties.
7
Partition coefficient: Drugs possessing both water and lipid
solubility are favorably absorbed through the skin. Transdermal
permeability coefficient shows a linear dependency on partition
coefficient. A lipid/water partition of 1 or greater is generally
required for optimal transdermal permeability.
pH condition: The extent of dissociation in case of ionic drugs and
their transdermal permeability depends on pH condition of the skin
surface as well as the drug delivery system. Incase of ephedrine and
scopolamine, the transdermal flux of the drug increases with
increasing pH upto 1.2 approximately 1.2 higher than their
respective pKa values.
8
 These are compounds which promote skin permeability
by altering the skin as a barrier to the flux of a desired
penetrant.
 These may conveniently be classified below
i. Solvents
ii. Surfactants
iii. Miscellaneous chemicals
9
There are four main types of TDDS
1) Single-layer Drug-in-Adhesive
2) Multi-layer Drug-in-Adhesive
3) Drug Reservoir-in-Adhesive
4) Drug Matrix-in-Adhesive
10
 The Single-layer Drug-in-Adhesive system is characterized by
the inclusion of the drug directly within the skin-contacting
adhesive.
 In this transdermal system design, the adhesive not only serves
to affix the system to the skin, but also serves as the
formulation foundation, containing the drug and all the
excipients under a single backing film.
 The rate of release of drug from this type of system
is dependent on the diffusion across the skin.
11
12
 The Multi-layer Drug-in-Adhesive is similar to the Single-
layer Drug-in-Adhesive in that the drug is incorporated
directly into the adhesive.
 However, the multi-layer encompasses either the addition of a
membrane between two distinct drug-in-adhesive layers or the
addition of multiple drug-in-adhesive layers under a single
backing film.
13
14
 The Reservoir transdermal system design is
characterized by the inclusion of a liquid compartment
containing a drug solution or suspension separated from
the release liner by a semi-permeable membrane and
adhesive.
 The adhesive component of the product responsible for
skin adhesion can either be incorporated as a continuous
layer between the membrane and the release liner or in a
concentric configuration around the membrane.
15
16
 The Matrix system design is characterized by the inclusion of
a semisolid matrix containing a drug solution or suspension
which is in direct contact with the release liner.
 The component responsible for skin adhesion is incorporated
in an overlay and forms a concentric configuration around the
semisolid matrix.
17
 Avoidance of significant presystemic metabolism and the
need therefore a lower daily dose.
 Recent inter & intra patient variability.
 Drug input can be terminated simply by removal of patch.
 Drug levels can be maintained in the systemic circulation,
with in the therapeutic window for a prolonged period of time.
 Self administration is possible.
18
 It is limited only to potent drug molecule.
 Drugs must not be locally irritating or sensitizing.
 Drug or drug formulation may cause skin irritation or
sensitization.
 Drugs with short biological half lifes that are subject to large
first pass metabolism.
19
 Transdermal drug delivery technologies are becoming one of
the fastest growing sectors within the pharmaceutical industry.
 Advance in drug delivery systems having increasingly
brought about rate controlled delivery with fewer side effects
as well as increased efficacy and constant drug delivery.
20
 Miller MA, Pisani E. The cost of unsafe injections. Bull World
Health Organisation. 1999;77: pg no:808-811.
 Ramteke K.H., Dhole S.N., Patil S.V. Journal of Advanced
Scientific Research, 2012, vol:3(1), Pg no:22-35.
 Richard.H.Guy, Jonathan Hardgraft.Transdermal Drug
Delivery, second edition, Revised and expanded. India Special
edition,2012,vol123,page no: 1-143,361-367.
 Dipen Patel, Sunita A. Chaudhary, Bhavesh Parmar, Nikunj
Bhura, Vol. 1 No. 4, 2012 ,Pg no:78-87.
21
22

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Transdermal drug delivery system ppt

  • 1. 1 A Concise Presentation By Mr. Deepak Sarangi M.Pharm
  • 2.  DEFINITION  MECHANISM OF DRUG ABSORPTION THROUGH SKIN  FUNDAMENTALS OF SKIN PERMEATION  FACTORS AFFECTING TRANSDERMAL PERMEABILITY  PERMEATION ENHANCERS  TYPES  ADVANTAGES  DISADVANTAGES  CONCLUSION  REFERENCES 2
  • 3. Transdermal therapeutic are defined as self contained discrete dosage form which when applied to the intact skin deliver the drugs, through the skin, at a controlled rate to the systemic circulation. (or) Transdermal drug delivery system (TDDS) are systems that utilize skin as a site for continuous drug administration into the systemic circulation. 3
  • 4.  Epidermis a) Stratum corneum b) Stratum lucidum c) Stratum granulosum d) Stratum spinosum  Dermis  Subcutaneous 4
  • 5. a) Transfollicular route Transfollicular route is the shortest pathway that drug has to follow to reach the systemic circulation that provides a large area for diffusion of drugs. b) Transcellular route Drug delivering through this route passes from corneocytes which has highly hydrated keratin creating hydrophilic pathway. The drug passes through the corneocytes of stratum corneum. c) Intercellular route In intercellular pathway the drug diffuses through the continuous lipid matrix present between the cells. 5
  • 6. Rate of permeation, dQ/dt, across a skin can be expressed as dQ/dt = Ps[ cd - cr ] Where, dQ/dt – Rate of permeation Ps – Permeability coefficient Cd – Concentration in donor compartment Cr – Concentration in receptor compartment 6
  • 7. The principle transport mechanism across mammalian skin is by passive diffusion. The factors influencing and having differences in transdermal permeability of the stratum corneum. Lipid solubility: At higher concentrations, the rate of penetration of the alcohols is greatly increased, and does not follow the pattern of absorption from weak solution. But, high concentrations may damage the stratum corneum impairing its 'barrier' properties. 7
  • 8. Partition coefficient: Drugs possessing both water and lipid solubility are favorably absorbed through the skin. Transdermal permeability coefficient shows a linear dependency on partition coefficient. A lipid/water partition of 1 or greater is generally required for optimal transdermal permeability. pH condition: The extent of dissociation in case of ionic drugs and their transdermal permeability depends on pH condition of the skin surface as well as the drug delivery system. Incase of ephedrine and scopolamine, the transdermal flux of the drug increases with increasing pH upto 1.2 approximately 1.2 higher than their respective pKa values. 8
  • 9.  These are compounds which promote skin permeability by altering the skin as a barrier to the flux of a desired penetrant.  These may conveniently be classified below i. Solvents ii. Surfactants iii. Miscellaneous chemicals 9
  • 10. There are four main types of TDDS 1) Single-layer Drug-in-Adhesive 2) Multi-layer Drug-in-Adhesive 3) Drug Reservoir-in-Adhesive 4) Drug Matrix-in-Adhesive 10
  • 11.  The Single-layer Drug-in-Adhesive system is characterized by the inclusion of the drug directly within the skin-contacting adhesive.  In this transdermal system design, the adhesive not only serves to affix the system to the skin, but also serves as the formulation foundation, containing the drug and all the excipients under a single backing film.  The rate of release of drug from this type of system is dependent on the diffusion across the skin. 11
  • 12. 12
  • 13.  The Multi-layer Drug-in-Adhesive is similar to the Single- layer Drug-in-Adhesive in that the drug is incorporated directly into the adhesive.  However, the multi-layer encompasses either the addition of a membrane between two distinct drug-in-adhesive layers or the addition of multiple drug-in-adhesive layers under a single backing film. 13
  • 14. 14
  • 15.  The Reservoir transdermal system design is characterized by the inclusion of a liquid compartment containing a drug solution or suspension separated from the release liner by a semi-permeable membrane and adhesive.  The adhesive component of the product responsible for skin adhesion can either be incorporated as a continuous layer between the membrane and the release liner or in a concentric configuration around the membrane. 15
  • 16. 16
  • 17.  The Matrix system design is characterized by the inclusion of a semisolid matrix containing a drug solution or suspension which is in direct contact with the release liner.  The component responsible for skin adhesion is incorporated in an overlay and forms a concentric configuration around the semisolid matrix. 17
  • 18.  Avoidance of significant presystemic metabolism and the need therefore a lower daily dose.  Recent inter & intra patient variability.  Drug input can be terminated simply by removal of patch.  Drug levels can be maintained in the systemic circulation, with in the therapeutic window for a prolonged period of time.  Self administration is possible. 18
  • 19.  It is limited only to potent drug molecule.  Drugs must not be locally irritating or sensitizing.  Drug or drug formulation may cause skin irritation or sensitization.  Drugs with short biological half lifes that are subject to large first pass metabolism. 19
  • 20.  Transdermal drug delivery technologies are becoming one of the fastest growing sectors within the pharmaceutical industry.  Advance in drug delivery systems having increasingly brought about rate controlled delivery with fewer side effects as well as increased efficacy and constant drug delivery. 20
  • 21.  Miller MA, Pisani E. The cost of unsafe injections. Bull World Health Organisation. 1999;77: pg no:808-811.  Ramteke K.H., Dhole S.N., Patil S.V. Journal of Advanced Scientific Research, 2012, vol:3(1), Pg no:22-35.  Richard.H.Guy, Jonathan Hardgraft.Transdermal Drug Delivery, second edition, Revised and expanded. India Special edition,2012,vol123,page no: 1-143,361-367.  Dipen Patel, Sunita A. Chaudhary, Bhavesh Parmar, Nikunj Bhura, Vol. 1 No. 4, 2012 ,Pg no:78-87. 21
  • 22. 22