Transcript Slide 1

Methods For Monitoring
Transdermal Drug Delivery
Analytical/Radio/Nuclear (ARN) Seminar
Jivan Yewle
Department of Chemistry
University of Kentucky
Overview
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Introduction
Skin Physiology
Transdermal Drug Delivery (TDD)
Methods For Monitoring TDD
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Confocal Laser scanning microscopy (CLSM)
Two photon fluorescence microscopy (TPFM)
Infrared Microscopic Imaging
Raman Microscopic Imaging
 Instrumentation
 Applications
 Advantages and Limitations
Introduction
Types of Drug Delivery system
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Oral Drug Delivery
Intravascular Drug Delivery
Transmucosal Drug Delivery
Transdermal Drug Delivery (TDD)
Skin Physiology
Stratum corneum
Epidermis
Dermis
Subcutaneous
tissue
www.uspharmacist.com
Skin Physiology
Characteristics:
 Tough
 Flexible
 Poor conductor of electricity
Functions of skin:
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To
To
To
To
protect the body from external insults
contain all body fluids
regulate body temperature
protect from electrical current
Transdermal Drug Delivery
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Delivery of drug through skin
Drugs (birth control patches, nicotine patches)
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Transdermal patches
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Transdermal Drug Delivery
Mechanism
 Penetration
 Intercellular route
 Follicular route
 Diffusion
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Transdermal Drug Delivery
Advantages of TDD:
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Steady permeation of drug across skin
Controlled drug delivery
Good for acid and enzyme reactive drugs.
Minimum risk of side effects
Limited toxic effects (if)
Convenience : may require only once weekly
Easy drug administration
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Good for lipophilic drug molecules
Transdermal Drug Delivery
Disadvantages and limitations of TDD
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Possibility of a local irritation
Allergic reactions are possible
Risky for children
Skin's low permeability
Molecular size and polarity of drug
Insufficient bioavailability
Damage to a transdermal patch
Transdermal Drug Delivery
Strategies for improving transport rate
Penetration enhancers
(eg: Water, Terpenes, Oleic acids, Menthol, Azones )
 Reduces barrier function of skin
 Some penetration enhancers remove lipids
from the skin
 Water: a natural penetration enhancer
 Alcohol: a solvent as well as a penetration
enhancer
Transdermal Drug Delivery
Strategies for improving transport rate
Liposomes
(Lipid vesicles)
 Spherical vesicles with a membrane composed
of a phosholipid bilayer
 Created by sonicating phospholipids in water
 Encapsulates drug molecule
 Lipid bilayer can fuse with other bilayers
 It neither penetrates nor fuses to SC
 It can be sensitive to temp, pH, light etc.
Instrumental tools for monitoring
TDD
1. Confocal Laser scanning microscopy
(CLSM)
2. Two photon fluorescence microscopy
(TPFM)
3. Infrared Microscopic Imaging
4. Raman Microscopic Imaging
1. Confocal Laser scanning microscopy
Instrumentation
http://en.wikipedia.org
1. Confocal Laser scanning microscopy
Applications in TDD
 Images parallel to skin surface
 Position of drug molecule under skin surface
 Information about penetration of drug
Other applications
 Evaluation of biological phenomenon
 Transport studies through biological membrane
 Surface study of different material
1. Confocal Laser scanning microscopy
Advantages
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Images of thick specimens at various depth
3D confocal images
High degree of precision
Blur-free images
Limitations and disadvantages
 Information about permeation of fluorescent
label only
 Images up to 25 mm depth only
 Smaller signal to noise ratio
2.Two Photon fluorescence microscopy
Instrumentation
2.Two Photon fluorescence microscopy
Applications in TDD
 Deeper images of skin up to 1mm
 Position of drug molecule under skin surface
 Information about penetration of drug
2.Two Photon fluorescence microscopy
Advantages
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Imaging up to depth of 1mm
Deeper tissue penetration
Reduced phototoxicity
Use of infrared light to excite fluorophores
High-resolution imaging.
Limitations
 Substance to be studied should have
fluorophores
Methods For Monitoring TDD
3. Infrared Microscopic Imaging
Instrumentation
3. Infrared Microscopic Imaging
Application in TDD
1,2-dipalmitoylphosphatidylcholine (DPPC-d62)
CD2-Symm/asymm-2100/2200
CH2-stre-2850-2920
Amide-1650/1550
C. Xiao, C.R. Flach, R. Mendelsohn. J Invest Dermatol. (2005), 124, 622-632
3. Infrared Microscopic Imaging
Advantages
 Sampling of much greater area (few mm)
 Higher signal to noise ratio
Limitations
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Unsuited to cofocal application
Limited applications for in vivo potential
Low spatial resolution (10-12 mm)
Requires careful sectioning of the skin (5 mm)
Methods For Monitoring TDD
4. Raman Microscopic Imaging
Application in TDD
CD2 Stretching
2000-2080 cm-1
www.shef.ac.uk
C. Xiao, C.R. Flach, R. Mendelsohn. J Invest Dermatol. (2005), 124, 622-632
4. Raman Microscopic Imaging
Advantages
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Non-intrusive and non-destructive
Analysis at various temperatures
Analysis within sealed systems
Direct spatially resolved concentration
Molecular structure information
Higher spatial resolution (1-2 mm)
4. Raman Microscopic Imaging
Applications
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Surface and materials science
Forensic research / investigation
Polymer science
Geology
Pharmaceutical science
Limitations
 Possibility of errors
Summary
 Transdermal drug delivery is an effective
technique for steady and consistent drug
delivery.
 Penetration enhancers and liposomes are good
solutions for the slow permeation of the skin.
 IR and Raman Microscopic imaging techniques
are more useful than others to monitor TDD.
References
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I.V. Zhigaltesv, N. Maurer. Biochemicaet Biophysica Acta. (2002),
1565, 129-135.
C. Xiao, C.R. Flach, R. Mendelsohn. J Invest Dermatol. (2005), 124,
622-632.
K.M.Hanson, R.M.Clegg. Biophys J. (2002), 83, 1682–1690.
E.N.Lewis,P.J.Treado. Anal Chem. (1995), 67, 3377–3381.
C.Xiao, R.Mendelsohn. Appl Spectrosc. (2004), 58, 382–389.
P.J.Caspers, G.J.Puppels. Biospectroscopy (1998), 4, S31–S39.
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www.uspharmacist.com
http://en.wikipedia.org
www.shef.ac.uk
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Acknowledgements
Dr. Vasilios Gavalas
University of Kentucky
Chemistry Department