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SURAJ C. 
Advanced Drug Delivery Systems Page 1 of 7 
TRANSDERMAL 
DRUG DELIVERY SYSTEMS 
(PHYSICAL PERMEATION ENHANCERS) 
“A review write up on several Physical Permeation Enhancers/Techniques in TDDS” 
Worked by: 
NIKHIL SUTAR 
Re-edited by: 
Suraj Choudhary 
I – M.PHARM 
DEPT. OF PHARMACEUTICS. 
2013-14
SURAJ C. 
Advanced Drug Delivery Systems Page 2 of 7 
PHYSICAL PERMEATION ENHANCERS 
1. Iontophoresis 
2. Sonophoresis 
3. Magnetophoresis 
IONTOPHORESIS 
 A technique of introducing ionic medicinal compounds into the body through the skin by applying a local electric current. 
ADVANTAGES: 
 Virtually painless when properly applied. 
 Provides option for patients unable to receive injections. Reduced risk of infection due to non-invasive nature. 
 Medications delivered directly to the treatment site. Minimizes potential for tissue trauma from an injection. Treatments are completed in minutes. 
LIMITATIONS: 
 An excessive current density = pain. 
 Burns = by electrolyte changes within the tissues. 
 High current density & time of application→generate extreme pH →chemical burn. 
 Electric shocks may cause by high current density at the skin surface. 
 Ionic form of drug in sufficient concentration is necessary for iontophoretic delivery. 
MECHANISM OF ACTION: 
 Electrode placement depends on the electric charge of ion(drug) to be delivered into the tissue. 
 Electrical energy assists the movement of ions across stratum corneum according to the basic electrical principle- -“like charges repel each other & opposite charges attract each other.” 
 Here the choice of drug is very important whether it is ionized or unionized.
SURAJ C. 
Advanced Drug Delivery Systems Page 3 of 7 
 +ve ion will be delivered from +ve electrode & -ve ion will be delivered by -ve electrode. 
 When -vely charged drug is to be delivered it is placed under -vely charged active electrode= it is repelled, attracted towards +ve electrode placed. 
 Iontophoresis enhances transdermal drug delivery by 3 mechanisms: 
 Ion-electric field interaction provides an additional force that drives ions through the skin. 
 The flow of electric current increases the permeability of the skin. 
 Electro-osmosis produces bulk motion of solvent that carries ions or neutral species with the solvent stream. Electro-osmotic flow occurs in a variety of membranes & is in the same direction as the flow of counter-ions. 
1. Passive Ionic Transdermal Drug Delivery System 
 Simple, relatively inexpensive & optimized enhancer patch system can accelerate the delivery of larger electrically charged drugs. 
 Faster drug transport. 
 Enhanced safety. 
 More rapid onset of drug delivery. 
2. Active Iontophoresis Transdermal Drug Delivery System 
 The application of external electric power source charges the drug substance; & facilitates
SURAJ C. 
Advanced Drug Delivery Systems Page 4 of 7 
movement of charged drugs to move into the skin. 
 Use of unique polymers to improve contact with skin & the rate and reliability of drug delivery. 
 Use of stable & safe electrode materials for iontophoretic delivery. 
 Streamlined product design for ease of use & improved patient compliance. 
 More rapid onset of drug delivery. 
 Potential for better control over the rate of delivery. 
 Minimal skin irritation and enhanced safety. 
COMPONENTS NEEDED FOR EFFECTIVE IONTOPHORESIS DELIVERY: 
 Power source for generating controlled direct current. 
 Electrodes that contain and disperse the drug. 
 Negatively or positively charged aqueous medication of relatively small molecule size (<8000 Daltons). 
 Localized treatment site. 
SELECTING THE APPROPRIATE ION: 
1. Negative ions accumulating at the positive pole or anode: 
 Produce an acidic reaction through the formation of hydrochloric acid. 
 Produce softening of the tissues by decreasing protein density-useful in treating scars or adhesions. 
 Some -ve ions can also produce an analgesic effect (salicylates). 
2. Positive ions that accumulate at the negative pole: 
 Produce an alkaline reaction with the formation of sodium hydroxide. 
 Produce hardening of the tissues by increasing protein density. 
TREATMENT PRECAUTIONS: 
 Patient has a good understanding of the existing condition which is to be treated. 
 Uses the most appropriate ions to accomplish the treatment goal. Uses appropriate treatment parameters and equipment set-up. 
FACTORS AFFECTING IONTOPHORETIC DELIVERY OF THE DRUG: 
 Operational Factors 
I. Composition of formulation: 
 Concentration of drug solution 
 pH of donor solution
SURAJ C. 
Advanced Drug Delivery Systems Page 5 of 7 
 Ionic strength 
 Presence of co-ions 
II. Physicochemical properties of the permeant: 
 Molecular size 
 Charge 
 Polarity 
 Molecular weight 
III. Experimental conditions: 
 Current density 
 Duration of treatment 
 Electrode material 
 Polarity of electrodes 
 Biological Factors 
 Regional blood flow 
 Skin pH 
 Condition of skin 
APPLICATIONS: 
1. Inflammation With Constant Pain (Red, Hot, and Swollen) 
 Dexamethasone Sodium Phosphate 0.4% (negative polarity) delivered from the cathode for 3 treatments per week for 2-4 weeks. 
 Diclofenac 5% (negative polarity) delivered from the cathode for 3 treatments per week for 2-4 weeks. 
 Ketoprofen 10% (negative polarity) delivered from the cathode for 3-5 treatments per week for 2-6 weeks. 
 Lidocaine Hydrochloride 4% (positive polarity) delivered from the anode for 3-5 treatments per week for 2 weeks.
SURAJ C. 
Advanced Drug Delivery Systems Page 6 of 7 
SONOPHORESIS 
 Sonophoresis is a technique which involves the use of ultrasonic energy to enhance skin penetration of active substances. 
 Cavitation principle. 20kHz to168 kHz. 
 Transdermal enhancement is particularly significant at low frequency regimes (20 KHz < f <100 KHz) than when induced by high frequency ultrasound. 
 Ultrasound parameters = treatment duration, intensity, pulse length & frequency are all known to affect percutaneous absorption. Frequency being the most important. 
MECHANISM OF ACTION: 
 Ultrasound produces thermal & non-thermal effects. 
 Due to this → formation of defects in stratum corneum of size 20 micron. 
 The mechanism of transdermal skin permeation involves the disruption of the stratum corneum lipids by the formation of gaseous cavities, thus allowing the drug to pass through the skin. 
Example: 
a) Sonophoresis of hypotensive agents & papain = treatment of eye diseases. 
b) Several antibiotics = tetracycline, biomycin, penicillin have been sonophoretically administered for the therapy of skin diseases. 
c) Sonoprep (Sontra medical corporation). Local anasthetic.
SURAJ C. 
Advanced Drug Delivery Systems Page 7 of 7 
MAGNETOPHORESIS 
 Application of a magnetic field = acts as an external driving force to enhance drug delivery across the skin. 
 Induces alteration in skin's structure that contribute to ↑ permeability. 
Magneto-liposomes 
Case Study: 
 Study investigated the mechanistic aspects of magnetophoretic transdermal drug delivery and also assessed the feasibility of designing a magnetophoretic transdermal patch system for the delivery of lidocaine. 
 In vitro drug permeation studies were carried out across the porcine epidermis at different magnetic field strengths. 
 The magnetophoretic drug permeation "flux enhancement factor" was found to increase with the applied magnetic field strength. 
 The mechanistic studies revealed that the magnetic field applied in this study did not modulate permeability of the stratum corneum barrier. 
 The predominant mechanism responsible for magnetically mediated drug permeation enhancement was found to be "magnetokinesis". 
 The octanol/water partition coefficient of drugs was also found to increase when exposed to the magnetic field. 
 A reservoir type transdermal patch system with a magnetic backing was designed for in vivo studies. 
 The dermal bioavailability (AUC(0-6h)) from the magnetophoretic patch system in vivo, in rats was significantly higher than the similarly designed non-magnetic control patch.

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Transdermal Drug Delivery Systems - (Physical enhancers through the skin) - A writeup

  • 1. SURAJ C. Advanced Drug Delivery Systems Page 1 of 7 TRANSDERMAL DRUG DELIVERY SYSTEMS (PHYSICAL PERMEATION ENHANCERS) “A review write up on several Physical Permeation Enhancers/Techniques in TDDS” Worked by: NIKHIL SUTAR Re-edited by: Suraj Choudhary I – M.PHARM DEPT. OF PHARMACEUTICS. 2013-14
  • 2. SURAJ C. Advanced Drug Delivery Systems Page 2 of 7 PHYSICAL PERMEATION ENHANCERS 1. Iontophoresis 2. Sonophoresis 3. Magnetophoresis IONTOPHORESIS  A technique of introducing ionic medicinal compounds into the body through the skin by applying a local electric current. ADVANTAGES:  Virtually painless when properly applied.  Provides option for patients unable to receive injections. Reduced risk of infection due to non-invasive nature.  Medications delivered directly to the treatment site. Minimizes potential for tissue trauma from an injection. Treatments are completed in minutes. LIMITATIONS:  An excessive current density = pain.  Burns = by electrolyte changes within the tissues.  High current density & time of application→generate extreme pH →chemical burn.  Electric shocks may cause by high current density at the skin surface.  Ionic form of drug in sufficient concentration is necessary for iontophoretic delivery. MECHANISM OF ACTION:  Electrode placement depends on the electric charge of ion(drug) to be delivered into the tissue.  Electrical energy assists the movement of ions across stratum corneum according to the basic electrical principle- -“like charges repel each other & opposite charges attract each other.”  Here the choice of drug is very important whether it is ionized or unionized.
  • 3. SURAJ C. Advanced Drug Delivery Systems Page 3 of 7  +ve ion will be delivered from +ve electrode & -ve ion will be delivered by -ve electrode.  When -vely charged drug is to be delivered it is placed under -vely charged active electrode= it is repelled, attracted towards +ve electrode placed.  Iontophoresis enhances transdermal drug delivery by 3 mechanisms:  Ion-electric field interaction provides an additional force that drives ions through the skin.  The flow of electric current increases the permeability of the skin.  Electro-osmosis produces bulk motion of solvent that carries ions or neutral species with the solvent stream. Electro-osmotic flow occurs in a variety of membranes & is in the same direction as the flow of counter-ions. 1. Passive Ionic Transdermal Drug Delivery System  Simple, relatively inexpensive & optimized enhancer patch system can accelerate the delivery of larger electrically charged drugs.  Faster drug transport.  Enhanced safety.  More rapid onset of drug delivery. 2. Active Iontophoresis Transdermal Drug Delivery System  The application of external electric power source charges the drug substance; & facilitates
  • 4. SURAJ C. Advanced Drug Delivery Systems Page 4 of 7 movement of charged drugs to move into the skin.  Use of unique polymers to improve contact with skin & the rate and reliability of drug delivery.  Use of stable & safe electrode materials for iontophoretic delivery.  Streamlined product design for ease of use & improved patient compliance.  More rapid onset of drug delivery.  Potential for better control over the rate of delivery.  Minimal skin irritation and enhanced safety. COMPONENTS NEEDED FOR EFFECTIVE IONTOPHORESIS DELIVERY:  Power source for generating controlled direct current.  Electrodes that contain and disperse the drug.  Negatively or positively charged aqueous medication of relatively small molecule size (<8000 Daltons).  Localized treatment site. SELECTING THE APPROPRIATE ION: 1. Negative ions accumulating at the positive pole or anode:  Produce an acidic reaction through the formation of hydrochloric acid.  Produce softening of the tissues by decreasing protein density-useful in treating scars or adhesions.  Some -ve ions can also produce an analgesic effect (salicylates). 2. Positive ions that accumulate at the negative pole:  Produce an alkaline reaction with the formation of sodium hydroxide.  Produce hardening of the tissues by increasing protein density. TREATMENT PRECAUTIONS:  Patient has a good understanding of the existing condition which is to be treated.  Uses the most appropriate ions to accomplish the treatment goal. Uses appropriate treatment parameters and equipment set-up. FACTORS AFFECTING IONTOPHORETIC DELIVERY OF THE DRUG:  Operational Factors I. Composition of formulation:  Concentration of drug solution  pH of donor solution
  • 5. SURAJ C. Advanced Drug Delivery Systems Page 5 of 7  Ionic strength  Presence of co-ions II. Physicochemical properties of the permeant:  Molecular size  Charge  Polarity  Molecular weight III. Experimental conditions:  Current density  Duration of treatment  Electrode material  Polarity of electrodes  Biological Factors  Regional blood flow  Skin pH  Condition of skin APPLICATIONS: 1. Inflammation With Constant Pain (Red, Hot, and Swollen)  Dexamethasone Sodium Phosphate 0.4% (negative polarity) delivered from the cathode for 3 treatments per week for 2-4 weeks.  Diclofenac 5% (negative polarity) delivered from the cathode for 3 treatments per week for 2-4 weeks.  Ketoprofen 10% (negative polarity) delivered from the cathode for 3-5 treatments per week for 2-6 weeks.  Lidocaine Hydrochloride 4% (positive polarity) delivered from the anode for 3-5 treatments per week for 2 weeks.
  • 6. SURAJ C. Advanced Drug Delivery Systems Page 6 of 7 SONOPHORESIS  Sonophoresis is a technique which involves the use of ultrasonic energy to enhance skin penetration of active substances.  Cavitation principle. 20kHz to168 kHz.  Transdermal enhancement is particularly significant at low frequency regimes (20 KHz < f <100 KHz) than when induced by high frequency ultrasound.  Ultrasound parameters = treatment duration, intensity, pulse length & frequency are all known to affect percutaneous absorption. Frequency being the most important. MECHANISM OF ACTION:  Ultrasound produces thermal & non-thermal effects.  Due to this → formation of defects in stratum corneum of size 20 micron.  The mechanism of transdermal skin permeation involves the disruption of the stratum corneum lipids by the formation of gaseous cavities, thus allowing the drug to pass through the skin. Example: a) Sonophoresis of hypotensive agents & papain = treatment of eye diseases. b) Several antibiotics = tetracycline, biomycin, penicillin have been sonophoretically administered for the therapy of skin diseases. c) Sonoprep (Sontra medical corporation). Local anasthetic.
  • 7. SURAJ C. Advanced Drug Delivery Systems Page 7 of 7 MAGNETOPHORESIS  Application of a magnetic field = acts as an external driving force to enhance drug delivery across the skin.  Induces alteration in skin's structure that contribute to ↑ permeability. Magneto-liposomes Case Study:  Study investigated the mechanistic aspects of magnetophoretic transdermal drug delivery and also assessed the feasibility of designing a magnetophoretic transdermal patch system for the delivery of lidocaine.  In vitro drug permeation studies were carried out across the porcine epidermis at different magnetic field strengths.  The magnetophoretic drug permeation "flux enhancement factor" was found to increase with the applied magnetic field strength.  The mechanistic studies revealed that the magnetic field applied in this study did not modulate permeability of the stratum corneum barrier.  The predominant mechanism responsible for magnetically mediated drug permeation enhancement was found to be "magnetokinesis".  The octanol/water partition coefficient of drugs was also found to increase when exposed to the magnetic field.  A reservoir type transdermal patch system with a magnetic backing was designed for in vivo studies.  The dermal bioavailability (AUC(0-6h)) from the magnetophoretic patch system in vivo, in rats was significantly higher than the similarly designed non-magnetic control patch.