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A 21mg dose nicotine patch applied to the left arm
Contraceptive patch
Clonidine tablets and transdermal patch
A transdermal patch which delivers medication is applied to the skin in a medical setting. The patch is labelled with the time and date of administration as well as the administrator's initials.
Microneedle patch size comparison[1]

A transdermal patch is a medicated adhesive patch that is placed on the skin to deliver a specific dose of medication through the skin and into the bloodstream. An advantage of a transdermal drug delivery route over other types of medication delivery (such as oral, topical, intravenous, or intramuscular) is that the patch provides a controlled release of the medication into the patient, usually through either a porous membrane covering a reservoir of medication or through body heat melting thin layers of medication embedded in the adhesive. The main disadvantage to transdermal delivery systems stems from the fact that the skin is a very effective barrier; as a result, only medications whose molecules are small enough to penetrate the skin can be delivered by this method. The first commercially available prescription patch was approved by the U.S. Food and Drug Administration in December 1979. These patches administered scopolamine for motion sickness.[2][3][4][5]

In order to overcome restriction from the skin, researchers have developed microneedle transdermal patches (MNPs), which consist of an array of microneedles, which allows a more versatile range of compounds or molecules to be passed through the skin without having to micronize the medication beforehand. MNPs offer the advantage of controlled release of medication and simple application without medical professional assistance required.[6] With advanced MNPs technology, drug delivery can be specified for local usage, for example skin whitener[7] MNPs that are applied to the face. Many types of MNPs have been developed to penetrate tissues other than skin, such as internal tissues of the mouth and digestive tract. These promote faster and more direct delivery of the molecule to the targeted area.

Applications

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Adverse events

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  • In 2005, the FDA announced that they were investigating reports of death and other serious adverse events related to narcotic overdose in patients using Duragesic, the fentanyl transdermal patch for pain control. The Duragesic product label was subsequently updated to add safety information in June 2005.[18]
  • In 2007, Shire and Noven Pharmaceuticals, manufacturers of the Daytrana ADHD patch, announced a voluntary recall of several lots of the patch due to problems with separating the patch from its protective release liner.[19] Since then, no further problems with either the patch or its protective packaging have been reported.
  • In 2008, two manufacturers of the fentanyl patch, ALZA Pharmaceuticals (a division of major medical manufacturer Johnson & Johnson) and Sandoz, subsequently issued a recall of their versions of the patch due to a manufacturing defect that allowed the gel containing the medication to leak out of its pouch too quickly, which could result in overdose and death.[20] As of March 2009, Sandoz—now manufactured by ALZA—no longer uses gel in its transdermal fentanyl patch; instead, Sandoz-branded fentanyl patches use a matrix/adhesive suspension (where the medication is blended with the adhesive instead of held in a separate pouch with a porous membrane), similar to other fentanyl patch manufacturers such as Mylan and Janssen.[21]
  • In 2009, the FDA announced a public health advisory warning of the risk of burns during MRI scans from transdermal drug patches with metallic backings. Patients should be advised to remove any medicated patch prior to an MRI scan and replace it with a new patch after the scan is complete.[22]
  • In 2009, an article in Europace journal detailed stories of skin burns that occurred with transdermal patches that contain metal (usually as a backing material) caused by shock therapy from external as well as internal cardioverter defibrillators (ICD).[23]

Components

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The main components to a transdermal patch are:

  • Release liner – Protects the patch during storage. The liner is removed prior to use.
  • Drug – Drug solution in direct contact with release liner
  • Adhesive – Serves to adhere the components of the patch together along with adhering the patch to the skin
  • Membrane – Controls the release of the drug from the reservoir and multi-layer patches
  • Backing – Protects the patch from the outer environment
  • Penetration enhancer – These are permeation promoters for drugs, which increase delivery of drug.
  • Matrix filler – Provides bulk to the matrix, and some act as matrix stiffening agents.

Other components include stabilizers (antioxidants), preservatives, etc.

Types

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Sample transdermal patches. On left is a 'reservoir' type, on the right a 'Single-layer Drug-in-Adhesive' version. Both contain exactly the same active ingredient with identical release rates.

There are five main types of transdermal patches.

Single-layer drug-in-adhesive

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The adhesive layer of this system also contains the drug. In this type of patch the adhesive layer not only serves to adhere the various layers together, along with the entire system to the skin, but is also responsible for the releasing of the drug. The adhesive layer is surrounded by a temporary liner and a backing. It is characterized by the inclusion of the drug directly within the skin-contacting adhesive placed onto the epidermis.

Multi-layer drug-in-adhesive

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The multi-layer drug-in-adhesive patch is similar to the single-layer system; the multi-layer system is different, however, in that it adds another layer of drug-in-adhesive, usually separated by a membrane (but not in all cases). One of the layers is for immediate release of the drug, and the other layer is for controlled release of the drug from the reservoir. This patch also has a temporary liner-layer and a permanent backing. The drug release from this depends on membrane permeability and diffusion of drug molecules.

Reservoir

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Unlike the single-layer and multi-layer drug-in-adhesive systems, the reservoir transdermal system has a separate drug layer. The drug layer is a liquid compartment containing a drug solution or suspension separated by the adhesive layer. The drug reservoir is totally encapsulated in a shallow compartment molded from a drug-impermeable metallic plastic laminate, with a rate-controlling membrane made of a polymer like vinyl acetate on one surface.[24] This patch is also backed by the backing layer. In this type of system the rate of release is zero order. Reservoir patches should not be cut (with the exception of hyoscine hyrdobromide 1.5mg patch according to the British National Formulary for Children).[24][25]

Matrix

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The matrix system has a drug layer of a semisolid matrix containing a drug solution or suspension. The adhesive layer in this patch surrounds the drug layer, partially overlaying it. The release rate is determined by the physical properties of the matrix.[24] Also known as a monolithic device. Limited research indicates that it may be possible to cut some matrix patches to provide lower doses, provided the cut part not immediately used is stored at cool temperatures.[26]

Vapour patch

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In a vapour patch, the adhesive layer not only serves to adhere the various layers together but also to release vapour. Vapour patches release essential oils for up to 6 hours and are mainly used for decongestion. Other vapour patches on the market improve quality of sleep or aid in smoking cessation.

Microneedle patch

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Further information: Microneedle drug delivery

The microneedle patch (MNPs) is a type of transdermal patch which retains the advantages, but reduces the disadvantages of basic transdermal patches. Embedding as many as 102–104 needles per square centimetre of patch, encapsulated or coated with intended drug, MNPs can easily pass skin tissue known as the stratum corneum which is roughly 20 μm in thickness, allowing up to the size of macromolecule to pass.[6] MNPs were developed mainly because transdermal patch can deliver smaller size or micronized molecules such as nicotine and birth control which easily diffuse and penetrate the skin, but lack in delivering macro or large size molecules. The 100–1000 μm needles spread across the patch, making sure people will not feel any discomfort from the patch. There are two types of needles used in MNPs, the first one is non-water-soluble needles made out of metal, ceramic, or polymer, and the second one is water-soluble needles made out of saccharides or soluble polymers.[6]

MNPs can also be engineered to deliver molecules into other tissues. Some that as of 2018 have been under development include internal surfaces such as the mouth, vagina, gastrointestinal tract, and vascular wall; and external surfaces such as the skin, eyes, fingernails, anus, and scalp.[6]

MNPs drug delivery

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As mentioned earlier, MNPs deliver more efficient delivery compared to topical or oral intake. In drug delivery study, researchers want to gain faster peak concentrations (Cmax) in MNPs compared to other methods. Study shows that MNPs reach peak concentration as fast as 20 minutes (tmax), while oral intake reaches peak concentration in one hour. Furthermore, the Cmax from MNPs is higher up to six times, compared to oral intake.[6] Making the delivery fast and the body gets the most concentration of intended drugs. This value is only matched with direct injection, but with skin trauma and people with needle phobia, MNPs might be an alternative to reach roughly the same time and concentration.

In order to get more direct local delivery, MNPs can be used in different tissues other than the skin.[27] In Table 1, there are at least five internal surfaces that MNPs have been studied for its delivery and four other external surfaces other than the skin.

MNPs may puncture stratum corneum to deliver directly to the dermis layer.[28]
Table 1: Tissues Studied for MNPs Delivery
Internal Surface External Surface
Mouth Skin
Vagina Eye
Gastrointestinal Tract Fingernail
Vascular Wall Anus
Scalp

Types of microneedle

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There are many types of microneedle that are distinguished by the shape and other characteristics. The types include: Dissolvable MNPs, solid non-soluble MNPs, and hollow MNPs. Different MNPs may be chosen depending on the situation and the drug properties.

Soluble or dissolvable MNPs

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One of the types of MNPs are water-soluble needles made out of soluble polymers or saccharide. However, dissolvable needles cannot efficiently deliver drugs to the dermal layer. Drug maximum concentration cannot be carried out to the skin, as the needles will dissolve beforehand. Fortunately, researchers have developed a water-insoluble backing layer, making the needle last longer in the human body environment. This design enables efficient delivery of more than 90% of the drug within 5 minutes of application of MNPs to the skin.[29]

Non-soluble or undissolvable MNPs

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Other than dissolvable MNPs, needles can also be made out of metal or ceramic that will not dissolve in the body environment. These coated drug needles can deliver consistent concentration of drugs without the needles dissolving in the body. This kind of MNPs has better performance, but compared to the soluble MNPs, metal or ceramic MNPs are the older version of MNPs. Even if the patches are small, the metal or ceramic MNPs may cause several waste issues. Recycling the metal and ceramic are very hard, as the quantity is very small to overcome the cost to recycle. That is why researchers try to develop the dissolvable MNPs with similar characteristic and performance of drug delivery in non-soluble MNPs.[29]

Hollow MNPs

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Among all of the MNPs, hollow needles allow a bigger amount of delivery up to 200μL. The mechanism mimics the operation of a hypodermic, but the fabrication is hard and complex. The hollow needles introduce a potential failure if the insertion is improper. That is why, among the others, hollow MNPs are the least popular because of the complex manufacturing and applying process.[1]

Advantages

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Disposing needlestick might cause injuries and transmission of pathogen.[30]
  1. The MNPs may puncture the skin surface, enabling rapid onset of drug bypassing directly into the dermal capillaries.[6]
  2. Pain-free.
  3. Can be localized to provide direct access to the intended tissues.[6]
  4. Less dependent on skilled medical workers, as MNPs can be administered safely by the patient themself.[6]
  5. Some drugs have poor solubility in water, with MNPs insoluble drugs and compounds can be directly "injected" to the dermal layer. Further enhancing the transdermal delivery of insoluble drugs.[31]
  6. Better safety compared to needle and syringe method (needlestick). Less waste, eliminate pathogen transmission, and injuries. At least 300,000 needlestick related injuries occurred in the US annually, with disposal contribute to almost half of the injuries.[31]

Application

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MNPs as vaccine delivery platform

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A set of conventional vaccine apparatus needed to be transported.[32]

MNPs vaccination might be an alternative from direct injection. Able to deliver bigger molecules than transdermal patch, MNPs can also deliver bioactive molecules with different physical sizes. Meaning that inactive virus or pathogen can be introduced in the body without discomfort or skin irritation from conventional injection. Possibly it can also reduce the cost of storage that usually needs to be transported in a particular temperature and condition. Stated in cdc.gov website, Mark Prausnitz, co-developer of the microneedle, says "A major advantage of the microneedle patch would be the ease of delivery." The MNPs are small and thin compared to bottles of vial, making it possible to transport in massive quantities in a single trip.[33] Medical waste such as syringes and dirty needles are also eliminated, reducing the possibility of pathogen transmission of blood-borne disease in rural areas.[7]

In a study, measles coated MNPs might be resistant to higher temperature compared to vial transport. Higher temperature resistance is a safe bet in low income countries, where there is no such luxury for refrigeration. Furthermore, the delivery of the vaccine is controlled by the MNPs. Less requiring highly trained medical workers in developing countries to apply the vaccine. However, the study in MNPs measles vaccine is still under development, but opening possibilities in the future for other types of vaccines[33]

MNPs for cosmetic and skin care

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Skin treatment including face whitening agent and dark eye circles serum can also incorporated in MNPs.[34] Its localized property enhance skin whitening delivery to the face area. Even a very specific spot like dark eye circles. By measuring the melanin (dark or black pigment found on the skin) index, subjects that are treated with whitening agents coated in MNPs show lower melanin index, compared to the whitening essence (topical) group. The treatment lasts for eight weeks, and the result shows MNPs might be a promising cosmetic vector because MNPs does not introduce skin irritation and can be engineered to localize or specific parts of the body.[35]

Safety

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MNPs may cause skin irritation on people with sensitive skin. Majority of studies show that MNPs do not irritate the skin. Especially for hollow MNPs, the not so stiff needles may cause unnecessary puncture of the skin outer layer, and may cause trauma to the skin and restricting the performance and flow of the drugs to the body.[1]

Future development

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Because most of MNPs applications are still under development, it is important to note the long effect of the efficiency of the drug deliveries. Furthermore, more research is needed to get information of what molecule can be delivered using MNPs. Disposal is also an important topic, as the small plastic backing may contribute to water pollution remembering the compact size can be easily carried away by wind and water without proper disposal.

Regulatory aspects

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A transdermal patch is classified by the U.S. Food and Drug Administration as a combination product, consisting of a medical device combined with a drug or biological product that the device is designed to deliver. Prior to sale in the United States, any transdermal patch product must apply for and receive approval from the Food and Drug Administration, demonstrating safety and efficacy for its intended use.[36]

See also

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References

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Further reading

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Revisions and contributorsEdit on WikipediaRead on Wikipedia

Transdermal patch

View on Grokipedia
from Grokipedia
A transdermal patch is a medicated adhesive device worn on the skin that delivers a controlled dose of medication directly into the bloodstream through diffusion across the cutaneous barrier, bypassing gastrointestinal absorption and hepatic first-pass metabolism.[1][2] These systems typically consist of a backing layer, drug reservoir or matrix, adhesive, and sometimes a rate-controlling membrane to achieve steady-state plasma concentrations over hours to days.[2] Introduced commercially in the late 1970s, transdermal patches represent an advancement in noninvasive drug delivery, with the first U.S. Food and Drug Administration-approved product being scopolamine for motion sickness prevention in 1979, followed by nitroglycerin for angina in 1980.[3][4] Transdermal patches offer advantages such as improved bioavailability for certain drugs, reduced dosing frequency enhancing patient adherence, and minimized peak-trough fluctuations that can mitigate side effects associated with oral routes.[5][1] Common applications include nicotine for smoking cessation, fentanyl for chronic pain management, estradiol for hormone replacement, and clonidine for hypertension, demonstrating their utility across diverse therapeutic areas.[1][3] However, limitations arise from the skin's stratum corneum acting as a formidable diffusion barrier, confining suitability to small, lipophilic molecules with molecular weights under 500 Da, and potential issues like local irritation or incomplete adhesion.[5][6] Ongoing innovations, including microneedle arrays to enhance permeability, aim to expand the range of deliverable therapeutics while preserving the method's safety profile.[2]

History

Early Conceptual Foundations

Topical poultices, such as mustard plasters, were widely used in the early 20th century for localized relief from ailments like respiratory congestion and muscular pain. These preparations, typically made from ground mustard seeds (Brassica nigra or similar species) combined with flour and activated by water to release allyl isothiocyanate, were applied directly to the skin as counterirritants, inducing hyperemia and mild blistering to alleviate underlying inflammation. Empirical observations revealed their efficacy stemmed primarily from superficial vascular effects rather than significant transdermal absorption, as systemic delivery was negligible due to the skin's stratum corneum acting as a lipid-rich diffusion barrier that restricted hydrophilic and large-molecule penetration.[7][8] In the 1960s and 1970s, foundational studies shifted toward quantitative models of skin permeation physics, applying Fick's first and second laws of diffusion to describe passive drug transport as proportional to concentration gradients and inversely related to barrier thickness. Researchers Robert J. Scheuplein and Irving H. Blank conducted pivotal experiments using radiolabeled compounds on excised skin and in vivo models, demonstrating that steady-state flux (J) follows J = -D * (dc/dx), where D is the diffusion coefficient influenced by molecular weight, lipophilicity (octanol-water partition coefficient), and skin hydration. Their work, culminating in a 1971 review, quantified permeability constants (K_p) for diverse solutes, confirming the epidermis—particularly the stratum corneum—as the rate-limiting layer with permeation rates orders of magnitude lower than vascularized tissues, thus necessitating enhancers or formulations for viable systemic delivery.[9] Preceding formalized products, early experiments in the 1960s tested simple adhesive systems for sustained release. In 1961, Donald E. Wurster and William E. Kramer affixed reservoir-type diffusion cells with pressure-sensitive adhesives to human forearms, monitoring urinary salicylate excretion over 24 hours to assess absorption kinetics. Results showed release rates modulated by patch surface area (up to 10 cm² tested) and occlusive conditions enhancing hydration, yielding detectable plasma levels but highlighting variability due to inter-individual skin differences and the barrier's resistance to non-optimized payloads. These adhesive tape prototypes demonstrated feasibility for prolonged cutaneous contact without needles, laying groundwork for controlled diffusion independent of gastrointestinal metabolism.[4]

Key Milestones in Development

In the 1970s, foundational research advanced steady-state diffusion models for transdermal drug delivery, applying Fick's first law of diffusion to quantify skin permeation rates and predict steady flux (J = K_m * D * (C_d - C_r)/h, where K_m is the membrane partition coefficient, D is the diffusion coefficient, C_d and C_r are donor and receptor concentrations, and h is stratum corneum thickness). These models, developed through in vitro permeation studies on excised skin, enabled engineers to optimize patch designs for zero-order release kinetics, addressing the skin's barrier properties to achieve therapeutic plasma levels without peaks and troughs associated with oral dosing.[4][10] The first systemic transdermal therapeutic system (TTS) gained U.S. FDA approval on December 3, 1979, with Transderm Scōp, a scopolamine patch manufactured by CIBA Pharmaceutical Company for preventing motion sickness. This 2.5 cm² reservoir-type patch, containing 1.5 mg of scopolamine in a gel reservoir with a rate-controlling membrane, demonstrated sustained release over 72 hours in pharmacokinetic studies, achieving steady-state plasma concentrations of 0.1-0.3 ng/mL effective for anticholinergic blockade while minimizing gastrointestinal side effects.[4][11][12] In 1981, the FDA approved the nitroglycerin transdermal system (e.g., Nitro-Dur by Key Pharmaceuticals), marking the first application of TTS for cardiovascular indications such as angina prophylaxis. This matrix or reservoir patch delivered 5-15 mg/day of nitroglycerin via passive diffusion, producing vasodilation with plasma levels of 0.2-0.8 ng/mL over 24 hours, as validated in clinical trials showing reduced ischemic episodes without significant tolerance buildup in short-term use.[4][3]

Commercialization and Expansion

The launch of the Nicoderm nicotine transdermal patch in late 1991 represented a breakthrough in commercialization, following FDA approval on December 6, 1991, as the first skin patch system for smoking cessation.[13] Supported by randomized controlled trials, such as a double-blind study published in the New England Journal of Medicine, the patch demonstrated significantly higher abstinence rates compared to placebo, with end-of-treatment quit rates reaching 44-61% for active doses versus 17% for placebo, though one-year sustained abstinence was lower at around 17-22%.[14] This empirical evidence of efficacy in alleviating nicotine withdrawal symptoms drove initial market adoption, establishing transdermal delivery as a viable alternative to oral or injectable therapies.[15] Expansion accelerated in the 1990s and 2000s as the technology proliferated beyond nicotine to hormone replacement and pain management. The Estraderm estradiol patch, approved by the FDA in 1986 for menopausal symptoms, gained broader use in estrogen therapy, exemplifying early adoption in endocrinology.[16] Similarly, the Duragesic fentanyl patch, approved in 1990 for severe chronic pain, emerged as a commercial success, achieving peak annual sales of over $2 billion by 2004 due to its sustained-release profile enabling consistent analgesia.[17] These developments underscored the market's recognition of transdermal patches' advantages in bioavailability and patient adherence, with the sector generating billions in cumulative revenue by the early 2000s.[4] A key milestone in accessibility occurred in 1996 when nicotine patches, including Nicoderm CQ, switched to over-the-counter status following FDA approval, reflecting real-world data on their safety and effectiveness in self-managed cessation without medical supervision.[18] This shift facilitated widespread adoption, contributing to industry growth as empirical metrics from post-marketing surveillance confirmed reduced withdrawal severity and higher quit attempts compared to unaided efforts.[19] By the 2000s, the transdermal market had matured, with diversification into additional indications driven by proven pharmacokinetic reliability rather than unverified claims.

Mechanism of Action

Fundamentals of Skin Permeation

The stratum corneum, the outermost layer of the epidermis consisting of 10–20 layers of flattened, anucleate corneocytes embedded in a brick-and-mortar-like structure of lipophilic intercellular lipids (primarily ceramides, cholesterol, and free fatty acids), functions as the primary barrier to transdermal drug permeation.[20] This lipophilic matrix, with its tortuous intercellular pathways, selectively impedes polar and large hydrophilic molecules while permitting diffusion of small, moderately lipophilic compounds, as confirmed by in vitro permeation studies using excised human skin.[21] The barrier's efficacy stems from its low water content (~10–15%), high lipid-protein packing density, and thickness of approximately 10–20 μm, which collectively minimize passive transport without active metabolic processes.[20] Successful transdermal permeation demands specific physicochemical properties in the permeant: molecular weight ideally below 500 Da to facilitate diffusion through the narrow lipid channels (effective pore sizes ~4.5–10 Å), octanol-water partition coefficient (log P) of 1–3 for balanced solubility in both the lipophilic stratum corneum and aqueous donor/acceptor phases, and sufficient melting point below 200°C to ensure molecular mobility.[22] These criteria arise from empirical correlations derived from quantitative structure-permeability relationships (QSPRs) in Franz diffusion cell experiments, where deviations—such as molecular weights exceeding 500 Da—result in exponentially reduced permeability coefficients (K_p often <10^{-6} cm/h).[23] Solubility in the vehicle is also critical to sustain the concentration gradient driving diffusion, as per Fickian principles. Under passive conditions, drug transport across the stratum corneum follows Fick's first law of diffusion, expressed as steady-state flux J = (D · K · ΔC) / h, where D is the diffusion coefficient within the skin lipids (typically 10^{-6} to 10^{-12} cm²/s, inversely related to molecular size), K is the skin-vehicle partition coefficient (reflecting lipophilicity matching), ΔC is the concentration gradient across the barrier, and h is the stratum corneum thickness.[24] This equation, validated through infinite-dose permeation assays on human cadaver skin, predicts fluxes on the order of μg/cm²/h for optimal candidates, yielding absolute bioavailabilities generally limited to 1–10% without permeation enhancers due to the barrier's resistance (e.g., nicotine permeation yields ~50% bioavailability in patches, but many peptides achieve <5%).[5] Empirical data from such models underscore that viable transdermal drugs must prioritize high potency to compensate for low flux rates. Appendageal routes, including hair follicles and sebaceous glands, represent minor shunts covering only ~0.1% of skin surface area and contribute negligibly (<1–5% of total flux) to steady-state permeation, as follicular infundibula are themselves lined by stratum corneum-like barriers and quickly saturate.[25] Claims of dominant follicular delivery overestimate this pathway's role, which is prominent only in transient early-phase uptake (e.g., within minutes of solvent-deposited solids) or for particulates targeting pilosebaceous units, but long-term transdermal absorption relies overwhelmingly on intercellular lipid diffusion (~90–99% of flux).[26] This is evidenced by comparable permeation rates in follicle-ablated versus intact skin models after initial transients.[27]

Drug Release and Absorption Dynamics

Transdermal patches employ membrane-controlled or matrix diffusion systems to facilitate zero-order drug release kinetics, wherein the rate of drug diffusion remains constant over time, independent of the remaining drug concentration within the system.[28][29] This controlled release mechanism contrasts with oral dosing, which often exhibits first-order kinetics leading to fluctuating plasma concentrations due to gastrointestinal absorption variability and extensive hepatic first-pass metabolism.[30] By bypassing the portal circulation, transdermal delivery maintains more stable therapeutic plasma levels, minimizing peaks that risk toxicity and troughs that compromise efficacy.[31] Following patch application, an initial lag phase occurs, typically lasting 1-3 hours, before steady-state permeation is achieved, as drug molecules diffuse through the skin's stratum corneum to establish equilibrium flux.[20][32] The absorption half-life and overall flux are modulated by patch dimensions, with larger surface areas enabling proportionally higher delivery rates due to increased diffusive area.[33] Application site further influences absorption dynamics; for instance, sites with higher cutaneous blood flow, such as the abdomen or trunk, promote faster permeation compared to extremities like limbs, where vascularity is lower.[34] Empirical bioavailability exemplifies these dynamics: fentanyl transdermal patches achieve approximately 90% systemic availability, as measured by area under the curve (AUC) comparisons, owing to evasion of first-pass effects that reduce oral fentanyl bioavailability to around 30%.[30][35] This enhanced efficiency allows for lower nominal doses to attain equivalent exposure, with steady-state concentrations reached after an observed time to maximum plasma level (T_max) of about 3-4 hours.[36]

Components

Structural Layers and Materials

The backing layer forms the outermost protective barrier in a transdermal patch, typically constructed from occlusive, impermeable polymers such as polyethylene, polypropylene, or polyester to prevent moisture loss, drug evaporation, and ingress of external contaminants while providing mechanical support and flexibility for skin conformity.[2] These materials are selected for their low permeability to water vapor and gases, ensuring the integrity of internal components over the patch's duration of use, which can extend up to 7 days in some formulations.[37] The adhesive layer, integral to skin attachment, employs pressure-sensitive polymers including acrylics, silicones, or polyisobutylenes, which maintain intimate contact without causing irritation and may incorporate the drug for direct release in certain designs.[37] [38] The drug itself is contained within a dedicated reservoir—often a liquid or gel formulation—or dispersed homogeneously in a solid polymer matrix, utilizing biocompatible materials like ethylene-vinyl acetate copolymers or hydrophilic polymers to enable controlled diffusion through the stratum corneum while minimizing burst release.[2] [39] A removable release liner, usually silicone-coated paper or polymer film, covers the adhesive surface prior to application, protecting the patch during storage and handling; it is peeled away to expose the adhesive without residue.[40] [41] All structural materials undergo rigorous stability testing per International Council for Harmonisation (ICH) guidelines, including accelerated conditions at 40°C/75% relative humidity, to verify 24-month shelf-lives with retained drug content above 90-95% and unchanged physical properties.[42] [43]

Role of Excipients and Enhancers

Excipients in transdermal patches include permeation enhancers that facilitate drug diffusion across the stratum corneum by temporarily disrupting its lipid matrix or improving drug partitioning into the skin. Alcohols such as ethanol and propylene glycol enhance flux by extracting lipids and proteins from the stratum corneum while increasing drug solubility, often achieving 2- to 5-fold increases in permeation rates for lipophilic drugs like indomethacin.[44] [45] Fatty acids, exemplified by oleic acid, interact with intercellular lipids to create transient aqueous channels, boosting flux by up to 10-fold in some formulations, though this efficacy is tempered by potential skin irritation from prolonged exposure.[46] [47] These enhancers are selected based on empirical flux measurements via Franz diffusion cells, prioritizing those with reversible effects to minimize barrier impairment post-application.[48] Pressure-sensitive adhesives (PSAs), such as acrylics and silicones, serve dual roles as excipients by providing adhesion to the skin and acting as drug reservoirs in drug-in-adhesive systems, where the active pharmaceutical ingredient is homogeneously dispersed within the adhesive matrix to control release kinetics.[49] [50] This integration modulates drug diffusion without separate layers, with adhesive tack and peel strength optimized to exceed 1 N/cm for reliable skin contact over 24-72 hours.[51] Antioxidants like butylated hydroxytoluene and preservatives such as parabens are incorporated to maintain formulation stability by inhibiting oxidative degradation and microbial growth, with stability studies demonstrating impurity leaching below 0.5% over shelf-life periods under ICH guidelines.[52] These additives ensure drug potency retention, as evidenced by accelerated aging tests showing less than 1% active loss in matrix systems.[53]

Types

Passive Diffusion Patches

Passive diffusion patches deliver therapeutic agents across the skin without external energy sources, relying solely on the concentration gradient between the drug reservoir in the patch and the lower concentration in the skin to drive molecular diffusion through the stratum corneum.[2] This mechanism adheres to Fick's laws of diffusion, where flux is proportional to the concentration difference and inversely related to skin barrier thickness, enabling controlled release without mechanical, electrical, or thermal enhancements.[32] Such patches are distinguished from active systems by their simplicity, as no pumps, microneedles, or iontophoresis are required, limiting applicability to lipophilic, low-molecular-weight drugs (<500 Da) with adequate skin permeability.[54] Drug-in-adhesive designs predominate in passive systems, incorporating the active pharmaceutical ingredient directly into the pressure-sensitive adhesive layer that contacts the skin, facilitating immediate diffusion upon application.[55] Single-layer variants embed the drug uniformly in the adhesive backed by an impermeable membrane, while multi-layer configurations separate drug loading from skin-facing adhesive to optimize release kinetics and prevent dose dumping.[2] The adhesive not only secures the patch but solubilizes the drug for partitioning into the skin's lipid matrix, with release rates tuned by polymer composition, drug loading (typically 5-20% w/w), and enhancers like alcohols or terpenes that transiently disrupt stratum corneum lipids without compromising patch integrity.[56] These systems achieve steady-state delivery over extended periods, with empirical data showing skin permeation rates of 5-20 μg/cm²/h for suitable candidates like nicotine or estradiol.[37] Vapour-permeable passive patches, often matrix-based, target volatile compounds such as essential oils (e.g., menthol or eucalyptol), allowing evaporation and localized permeation through a semi-occlusive backing that permits vapor diffusion to the skin surface.[57] Primarily designed for topical effects like aroma therapy or mild analgesia, these patches release volatiles over 4-8 hours, but systemic absorption remains minimal due to rapid evaporation and poor bioavailability of hydrophilic or high-volatility payloads, with limited clinical trials demonstrating quantifiable plasma levels.[58] Efficacy for transdermal systemic delivery is constrained by low partition coefficients and short residence times, restricting use to adjunctive rather than primary therapeutics.[59] The inherent simplicity of passive diffusion patches yields manufacturing advantages, including lower costs from fewer components and scalability via solvent casting or hot-melt extrusion, alongside clinical benefits like consistent zero-order kinetics reducing peak-trough fluctuations.[6] Wear times typically range from 24 to 72 hours, determined by drug solubility, patch size (10-30 cm²), and adhesion strength to minimize irritation or detachment, though patient factors like perspiration can reduce effective duration.[60] This design supports high patient adherence through non-invasive application but demands precise formulation to avoid saturation or incomplete release.[61]

Reservoir-Type Patches

Reservoir-type transdermal patches incorporate a dedicated drug reservoir, typically a pouch or compartment filled with a liquid or gel formulation of the active pharmaceutical ingredient, overlaid by a rate-controlling membrane that governs the permeation rate to the skin.[37] This membrane, often composed of materials like ethylene-vinyl acetate copolymer, functions as the primary barrier to achieve predictable, steady-state diffusion independent of reservoir concentration gradients.[62] The design supports zero-order kinetics, delivering a constant flux over extended periods, such as 72 hours in the case of scopolamine patches used for motion sickness prevention.[3] The reservoir's liquid-based formulation facilitates high drug loading for potent agents, with the membrane ensuring controlled release that mimics intravenous infusion profiles by maintaining plasma concentrations within therapeutic windows without peak-trough fluctuations.[31] Examples include fentanyl patches like Duragesic, which employ a gel reservoir for opioid delivery in chronic pain management, and certain estradiol reservoir systems for hormone replacement therapy in postmenopausal women, providing stable estrogen levels comparable to continuous infusion.[63] These systems are particularly suited to lipophilic, low-molecular-weight drugs requiring sustained systemic exposure, as the membrane's permeability is engineered to match skin permeation rates empirically determined in vitro and in vivo.[2] A key drawback is the risk of unintended dose dumping or leakage from the reservoir if the patch is punctured or improperly manufactured, potentially leading to rapid drug release and toxicity, as highlighted in quality guidelines emphasizing seal integrity testing.[64] However, intact reservoir patches demonstrate consistent delivery uniformity, with clinical pharmacokinetic data confirming near-zero-order profiles over 3 days without significant variability in flux, as validated in stability and release studies for approved products.[3] This reliability stems from the membrane's role as the rate-limiting step, overriding potential inconsistencies in the reservoir's viscous medium.[37]

Matrix-Type Patches

Matrix-type transdermal patches feature the active pharmaceutical ingredient dispersed homogeneously within a polymeric matrix that functions as both the drug reservoir and the primary rate-controlling element, enabling controlled release via molecular diffusion driven by concentration gradients.[65] This solid dispersion design eliminates the liquid reservoir found in other systems, minimizing risks of leakage or initial burst release while simplifying manufacturing through direct incorporation of the drug into biocompatible polymers such as hydroxypropyl methylcellulose (HPMC) or ethylcellulose (EC).[66] Multi-layer configurations, often including an adhesive backing and rate-modulating membranes, further refine release kinetics to achieve zero-order delivery profiles over extended periods.[37] These patches are cost-effective to produce due to fewer components and streamlined fabrication processes like solvent casting or hot-melt extrusion, which avoid complex reservoir assembly.[67] Common applications include nicotine replacement therapy, where patches like Nicoderm deliver steady nicotine levels for 16 to 24 hours to support smoking cessation by mitigating withdrawal symptoms.[3] Fentanyl matrix patches, such as Durogesic DTrans, provide analgesia for chronic pain over 72 hours by maintaining therapeutic plasma concentrations through sustained diffusion.[68] [69] While the matrix structure inherently reduces dose-dumping potential compared to reservoir types, physical damage or adhesive failure can compromise integrity, leading to rapid drug release and heightened overdose risk.[1] [65] Clinical guidelines emphasize intact application and prohibit cutting or altering patches to preserve predictable pharmacokinetics.[70] Efficacy data from wear studies confirm stable absorption, with fentanyl utilization rates reaching approximately 82% over 72 hours in matrix formulations versus lower in alternatives.[68]

Active Delivery Patches

Active delivery patches incorporate external energy sources or mechanical interventions to actively enhance transdermal drug permeation, surpassing the limitations of passive diffusion by disrupting the stratum corneum barrier or driving molecules electrophoretically.[71] These systems address challenges with high molecular weight or hydrophilic drugs that exhibit poor passive flux.[72] Iontophoresis employs a low-intensity direct current, typically in the range of 0.1-0.5 mA/cm², to propel charged drug ions across the skin via electrophoresis and electroosmosis.[73] This method can increase transdermal flux by several-fold to over 10 times compared to passive diffusion, depending on the drug's charge and formulation.[74] For instance, increasing current density from 0.1 to 0.3 mA/cm² has yielded approximately a 4.2-fold flux enhancement for methotrexate in ex vivo studies.[75] Higher densities up to 0.5 mA/cm² further amplify delivery but require monitoring for skin irritation.[76] Microneedles, micron-scale projections measuring 50-900 μm in length, create transient microchannels through the stratum corneum to facilitate convective drug transport.[77] Hollow microneedles enable pressurized infusion of liquid formulations, while dissolvable variants, often composed of polymers like polyvinyl alcohol, embed the drug for sustained release as the needles degrade in interstitial fluid.[78] This approach bypasses the lipophilic barrier, achieving near-instantaneous penetration depths sufficient for viable epidermis targeting without reaching pain receptors.[79] Techniques such as ultrasound (sonophoresis) and electroporation apply acoustic waves or high-voltage pulses to induce transient pores, respectively, enhancing permeability for macromolecules.[80] However, these methods exhibit limited commercial adoption in patch formats due to requirements for bulky transducers or pulse generators, complicating portability and increasing device complexity over simpler iontophoretic or microneedle designs.[81] Empirical data indicate variable flux gains, often 10- to 100-fold under optimized conditions, but reproducibility challenges and potential skin trauma hinder widespread integration.[82]

Applications

Pain Management and Analgesics

Transdermal fentanyl patches were approved by the U.S. Food and Drug Administration on August 7, 1990, for chronic severe pain in opioid-tolerant patients requiring continuous opioid administration.[83] These patches deliver the drug at a controlled rate, achieving steady plasma concentrations that minimize peak-trough fluctuations associated with oral dosing. Randomized controlled trials comparing fentanyl patches to oral morphine in chronic pain management, including non-cancer indications, have found equivalent analgesic efficacy, with the transdermal route often associated with fewer episodes of breakthrough pain due to consistent delivery.[84] [85] Lidocaine 5% transdermal patches are approved for postherpetic neuralgia and have demonstrated efficacy in randomized trials for localized neuropathic pain, reducing pain intensity scores significantly versus placebo.[86] Systematic reviews of clinical data indicate that approximately 50-70% of patients with peripheral neuropathic conditions experience clinically meaningful relief, defined as at least moderate pain reduction, with meta-analyses confirming superior outcomes over placebo in conditions like diabetic neuropathy and post-surgical neuralgia.[87] The localized action limits systemic exposure, supporting use in targeted analgesia. Buprenorphine transdermal patches, delivering low doses (5-20 mcg/hour), are indicated for moderate to severe chronic pain and function as partial mu-opioid agonists, providing dose-dependent analgesia up to a ceiling effect.[88] In randomized placebo-controlled trials, these patches significantly reduce pain intensity in non-cancer chronic pain, comparable to full agonists but with lower risks of respiratory depression escalation.[89] Their abuse potential is reduced relative to fentanyl or other extended-release opioids, as evidenced by lower diversion and misuse rates in surveillance data, attributed to partial agonism limiting euphoric effects and extraction challenges from the matrix.[90] [91]

Hormone and Nicotine Replacement

Transdermal nicotine patches, approved by the U.S. Food and Drug Administration in December 1991 for prescription use as an aid to smoking cessation, deliver controlled doses of nicotine across the skin to alleviate withdrawal symptoms while avoiding first-pass hepatic metabolism associated with oral ingestion.[92] Clinical trials lasting 8 to 12 weeks have demonstrated that these patches approximately double continuous abstinence rates at 6 months compared to placebo, with meta-analyses confirming a 50% to 70% increase in quitting success.[93] This delivery method provides steady plasma nicotine levels, reducing the peaks that reinforce smoking behavior. Estradiol transdermal patches, first approved in 1986 for treating menopausal symptoms, administer 17β-estradiol directly into the bloodstream, achieving steady-state serum levels more rapidly than oral formulations and avoiding hepatic first-pass effects that cause variability in estrogen exposure.[94] Unlike oral estradiol, which undergoes significant gut and liver metabolism leading to fluctuating hormone profiles, transdermal application maintains consistent therapeutic concentrations, potentially improving symptom relief for hot flashes and vasomotor instability while minimizing dose-related peaks.[95] Testosterone transdermal patches, used for hypogonadism in men, effectively normalize 24-hour average serum testosterone levels in approximately 86% of patients, mimicking diurnal rhythms and improving sexual function and mood comparably to other replacement forms.[96] Combined hormonal contraceptive transdermal patches, approved by the FDA in 2001, release ethinylestradiol and norelgestromin weekly, achieving pregnancy prevention efficacy similar to oral contraceptives with Pearl Indexes around 0.8 to 1.2 in clinical use.[97] However, epidemiological data indicate a potentially higher risk of nonfatal venous thromboembolism compared to equivalent low-dose norgestimate oral contraceptives, with incidence rates estimated at 9.7 events per 10,000 woman-years for patch users versus 5.7 for oral users in some observational studies.[98] This elevated risk may stem from higher steady-state estrogen exposure due to transdermal pharmacokinetics, though absolute VTE incidence remains low overall.[99]

Other Therapeutic Indications

Transdermal scopolamine patches, approved by the U.S. Food and Drug Administration on December 31, 1979, are indicated for preventing nausea and vomiting due to motion sickness in adults.[100] The patch is applied behind the ear at least four hours before anticipated exposure, providing anticholinergic effects for up to three days.[101] A systematic review and meta-analysis of 20 trials involving 753 participants found scopolamine reduced the risk of nausea with a relative risk of 0.35 (95% CI not specified in summary) compared to placebo, indicating substantial preventive efficacy against motion-induced symptoms.[102] Transdermal rivastigmine patches are approved for the symptomatic treatment of mild to moderate dementia of the Alzheimer's type, delivering the cholinesterase inhibitor to enhance cholinergic neurotransmission and improve cognitive function, with a better tolerability profile regarding gastrointestinal side effects compared to oral formulations.[103] In cardiovascular applications, transdermal nitroglycerin patches deliver the nitrate to prevent angina pectoris by promoting vasodilation and reducing cardiac preload.[104] Clinical studies demonstrate sustained hemodynamic effects, including decreased blood pressure and improved exercise tolerance, persisting up to 24 hours after application of patches like Deponit 10 mg/24 h.[105] However, continuous use often leads to tolerance, necessitating intermittent application to maintain efficacy.[106] Transdermal clonidine patches, such as Catapres-TTS, are approved for hypertension management, providing steady alpha-2 adrenergic agonism to lower blood pressure via central sympatholytic action.[107] Evaluations in hypertensive patients show antihypertensive effects sustained throughout the seven-day patch duration and up to three months of continuous therapy, with minimal rebound hypertension compared to oral forms due to gradual release.[108][109] Prototypes for transdermal insulin delivery, including microneedle-enhanced patches, have demonstrated feasibility in lowering blood glucose in animal models and small human trials.[110] Despite these advances, no such systems have received FDA approval as of 2024, primarily due to inter- and intra-subject variability in absorption rates and challenges in achieving consistent bioavailability comparable to subcutaneous injection.[110][111]

Advantages

Pharmacokinetic Benefits

Transdermal patches bypass hepatic first-pass metabolism by delivering drugs directly into systemic circulation via the skin, thereby enhancing bioavailability for compounds prone to extensive liver inactivation.[112] This route avoids the presystemic elimination that reduces oral drug efficacy, as evidenced by comparative pharmacokinetic studies showing superior absorption profiles for transdermal systems.[5] A key example is estradiol, where transdermal administration yields bioavailability approaching 90-100% due to circumvention of first-pass effects, compared to only 2-5% for oral dosing, which requires substantially higher doses to achieve equivalent plasma levels.[113][114] Many patch designs, particularly reservoir and matrix types, facilitate near-zero-order release kinetics, maintaining constant drug flux across the skin to produce stable plasma concentrations and avert the sharp peaks and troughs typical of oral or bolus dosing.[3] For fentanyl, this results in predictable delivery over 48-72 hours, with studies demonstrating reduced fluctuation in opioid levels versus intermittent oral intake, thereby lowering risks of concentration-dependent toxicity such as respiratory depression from peak exposures.[115][116] Empirical data from bioavailability trials indicate that steady-state plasma levels are generally reached within 12-24 hours for optimized systems, though up to 72 hours for lipophilic agents like fentanyl, supporting sustained efficacy for chronic therapies without frequent redosing.[84][117] This temporal profile aligns with the patches' capacity for consistent therapeutic drug monitoring in long-term applications.[2]

Patient Compliance and Practicality

Transdermal patches promote higher patient compliance compared to regimens requiring multiple daily doses, as their weekly or biweekly application aligns with preferences for infrequent administration. In a study of asthma and COPD patients, 83.2% expressed preference for once-daily dosing, correlating with improved adherence metrics observed in transdermal systems.[118] Adherence rates for transdermal rivastigmine in Alzheimer's patients reached 60.5% versus lower rates with oral formulations in comparative real-world evaluations.[119] For hormone replacement therapy, compliance with estradiol patches exceeded 90% in postmenopausal women, attributed to simplified dosing.[120] In nicotine replacement therapy trials, transdermal patches achieved adherence rates near 80%, surpassing oral nicotine products which demand repeated active dosing and exhibit lower compliance due to user burden.[121] Continuation rates in smoking cessation programs favor patches for their ease, with general nicotine replacement therapy adherence averaging 61% across formats but higher for passive transdermal delivery.[122][123] As a non-invasive option, patches serve as a discreet alternative to injections, reducing adherence barriers like needle phobia reported in up to 20-30% of patients averse to parenteral routes.[124] This usability supports long-term therapy persistence, with dementia treatment studies showing transdermal adherence rising to 85.9% at six months.[125] Overall, these factors contribute to practical advantages in outpatient settings, enhancing real-world treatment outcomes through sustained use.[1]

Limitations and Criticisms

Physicochemical Constraints

Passive transdermal delivery is governed by Fick's laws of diffusion, where drug flux across the stratum corneum depends on the concentration gradient, diffusivity, and partition coefficient between the vehicle and skin lipids. The stratum corneum's lipophilic nature imposes strict physicochemical requirements: effective candidates typically have molecular weights under 500 Da, log P values of 1-3 for balanced lipophilicity, and low daily doses (<20 mg) to compensate for inherently low permeation rates (often 1-10 μg/cm²/h). Hydrophilic compounds or those exceeding these thresholds partition poorly into the barrier, resulting in flux insufficient for therapeutic efficacy.[37][126][32] High-molecular-weight biologics exemplify these constraints; insulin, with a molecular weight of approximately 5800 Da and hydrophilic character, achieves negligible passive permeation, with in vitro studies reporting cumulative delivery below detectable therapeutic thresholds without active enhancement. Such limitations restrict passive patches to a narrow subset of small-molecule drugs like nicotine, fentanyl, or estradiol, excluding peptides, proteins, or vaccines that dominate modern pharmacotherapeutics.[127][128] Inherent skin variability further exacerbates predictability: factors including age-related thinning of the stratum corneum, hydration levels altering barrier fluidity, and ethnic differences in lipid composition can cause 20-50% interindividual variation in absorption, as evidenced by pharmacokinetic studies comparing permeation across diverse cohorts. These fluctuations stem from causal differences in corneocyte packing and intercellular lipid organization, undermining dose uniformity without individualized adjustments.[32][53]

Adhesion and Efficacy Challenges

Adhesion failures in transdermal patches commonly arise from environmental factors such as sweat and skin oils, which compromise the adhesive interface and result in partial or complete detachment before the intended wear period.[129] These failures disrupt steady-state drug delivery, often leading to subtherapeutic plasma levels; for instance, in fentanyl patches, inadequate adhesion after 48 hours can mimic end-of-dosage attenuation, prompting premature replacement to maintain analgesia but risking inconsistent dosing if undetected.[130] Medication errors exacerbate efficacy challenges, particularly in hospital environments where overlapping applications of patches—such as multiple opioid systems—have been linked to unintended overdose due to cumulative drug release.[131] Clinical audits and error reports highlight administration mishaps, including failure to remove prior patches, as recurrent issues in transdermal opioid use, contributing to variable therapeutic outcomes and heightened toxicity risks.[132] Claims of sustained, reliable delivery in transdermal systems frequently underperform in heterogeneous populations, where inter-individual differences in skin permeability— influenced by factors like age, ethnicity, and hydration—alter drug flux rates and undermine pharmacokinetic predictability.[133] This variability challenges the generalization of controlled-release profiles from idealized trials to real-world application, revealing gaps between promotional assertions and empirical performance across diverse demographics.[32]

Safety and Withdrawal Cases

The Zecuity sumatriptan iontophoretic transdermal patch, approved by the FDA in January 2015 and commercially available from September 2015, was voluntarily suspended by Teva Pharmaceuticals in June 2016 amid reports of application-site burns and scarring. Post-marketing surveillance identified adverse events including severe redness, cracked skin, blistering, welts, and permanent scars in a subset of users, with the FDA documenting a "large number" of such cases despite an overall incidence below 1%. The iontophoretic mechanism, relying on low-level electrical current to drive drug delivery, was causally implicated in these thermal and electrochemical injuries, prompting full market withdrawal by January 2017 due to unacceptable risk-benefit imbalance in real-world use.[134][135] Fentanyl transdermal patches, such as Duragesic, have documented post-approval risks from interactions with external heat sources, which accelerate drug release and permeation through the skin barrier. FDA labeling cites clinical pharmacology studies and adverse event reports showing that heat exposure—via heating pads, hot baths, saunas, or fever—can elevate systemic fentanyl levels, with absorption rates increasing substantially (up to twofold or more in controlled heating scenarios), leading to overdose and death from respiratory depression. Between 2004 and 2014, U.S. poison control data linked over 1,200 fentanyl patch-related fatalities to such factors, including cases where warnings failed to prevent misuse near heat, highlighting design limitations in temperature-dependent matrix diffusion despite patch safeguards like rate-limiting membranes.[136][137] These withdrawal cases illustrate causal vulnerabilities in transdermal formulations, including iontophoretic irritation and thermolabile absorption, often unpredicted by pre-approval trials due to controlled conditions masking inter-patient skin variability and environmental confounders. While transdermal systems generally reduce injection-associated hazards like needlestick injuries (estimated at 384,000 annually in U.S. healthcare) and subcutaneous infections, post-market data critiques reveal underemphasized pharmacokinetic inconsistencies, such as 20-50% inter-subject absorption variability, contributing to rare but severe failures that necessitate enhanced real-world monitoring over idealized safety profiles.[138][32]

Adverse Events

Common Dermatological Reactions

The most prevalent dermatological reactions to transdermal patches are irritant contact dermatitis manifestations, such as erythema (redness) and pruritus (itching), reported in 20% to 50% of users across clinical trials of various systems including fentanyl, buprenorphine, and rivastigmine patches.[139] [140] These localized reactions are generally mild to moderate in severity, confined to the application site, and transient, resolving within hours to days after patch removal without sequelae in most cases.[141] They predominantly stem from mechanical irritation or adhesive components, such as pressure-sensitive polymers, rather than the transdermal drug itself, with similar incidences observed in placebo-controlled arms of studies.[142] Allergic contact dermatitis occurs less commonly, in approximately 1% to 5% of users, and involves type IV hypersensitivity to specific patch constituents like acrylate adhesives frequently employed in nicotine replacement therapy systems.[142] [143] Symptoms may include vesicular eruptions or persistent erythema beyond patch removal, necessitating discontinuation and potential patch testing for allergens such as 2-ethylhexyl acrylate; for example, in nicotine patch trials, acrylate-related cases have been confirmed via diagnostic testing.[144] Contributing risk factors encompass extended wear duration exceeding 24-72 hours, occlusive patch designs that elevate transepidermal water loss and microbial proliferation under the patch, and application to moist or compromised skin sites, which amplify irritant potential across delivery systems.[140] [32] In rivastigmine patch trials involving over 1,000 patients, application site erythema affected 43.1% and pruritus 40.2%, underscoring variability by formulation but consistent predominance of irritant over allergic mechanisms.[145] Preventive strategies, such as site rotation every 7 days and cleansing with water prior to application, mitigate incidence without altering patch efficacy.[141]

Systemic Risks and Errors

Improper disposal of transdermal patches poses significant risks of accidental overdose, particularly in pediatric populations, as residual active ingredients can remain potent post-use. Fentanyl patches have been linked to multiple child fatalities annually through such exposures, with children often mistaking discarded patches for stickers or toys, leading to transdermal absorption or ingestion causing respiratory depression and death.[146] The U.S. Food and Drug Administration (FDA) has documented ongoing cases of severe poisoning in children from both new and used patches, emphasizing that even low-level exposure can be lethal due to fentanyl's high potency.[146] Pharmacovigilance reports highlight that males under age five are disproportionately affected, with improper storage or disposal cited as primary causal factors in reported incidents.[147] Drug interactions exacerbate systemic risks by altering patch-delivered pharmacokinetics, potentially resulting in supratherapeutic plasma levels and toxicity. For opioids like fentanyl, co-administration with cytochrome P450 3A4 (CYP3A4) inhibitors—such as certain antibiotics (e.g., ciprofloxacin) or antifungals—can inhibit metabolism, elevating drug concentrations and precipitating overdose symptoms including sedation and respiratory arrest.[136] Fentanyl patch labeling explicitly warns of this interaction, noting increased plasma exposure that may necessitate dose adjustments or discontinuation to avert life-threatening events.[136] Case reports from pharmacovigilance databases confirm instances of acute toxicity, including fatalities, attributed to such pharmacokinetic synergies rather than patch malfunction alone.[148] Interindividual variability in transdermal absorption can mimic dosing errors or non-compliance, complicating clinical management and indirectly heightening overdose risks through compensatory over-adjustments. Skin factors like thickness, hydration, and perfusion lead to inconsistent drug flux, with studies showing up to several-fold differences in bioavailability across patients, potentially yielding subtherapeutic or unexpectedly high systemic exposure.[149] This variability has been flagged in pharmacovigilance analyses as a contributor to adverse events misattributed to patient behavior, prompting erroneous dose escalations that amplify toxicity in susceptible individuals. Rare systemic hypersensitivity or enhancer-related toxicities, such as from permeation facilitators like terpenes, have been noted but remain infrequent, with most concerns tied to cumulative absorption rather than acute overdose.[150]

Regulatory Aspects

Approval Standards and Processes

Transdermal patches are regulated by the U.S. Food and Drug Administration (FDA) primarily as drug products under the Federal Food, Drug, and Cosmetic Act, though advanced variants incorporating microneedles or other active delivery mechanisms may qualify as combination drug-device products subject to additional oversight by the Center for Devices and Radiological Health.[151] Approval for new patches typically proceeds via New Drug Application (NDA) pathways under section 505(b)(1) for full innovator data or 505(b)(2) for those relying partly on existing studies, requiring demonstration of safety and efficacy through pharmacokinetic (PK) profiles, including steady-state plasma concentrations and dose proportionality.[42] Generic equivalents submit Abbreviated New Drug Applications (ANDAs), mandating bioequivalence to the reference listed drug via in vivo PK studies showing 80-125% confidence intervals for area under the curve (AUC) and maximum concentration (C_max), alongside in vitro release testing to confirm comparable drug permeation rates.[42][111] Adhesion performance constitutes a critical quality attribute, evaluated through clinical studies in healthy volunteers under labeled use conditions, with the test product required to achieve adhesion comparable to the reference (e.g., less than 10% detachment in at least 80% of subjects across body sites).[152] These assessments align with United States Pharmacopeia (USP) general chapter <698> on deliverable volume and related adhesive tests, including peel adhesion, tack, and shear strength to ensure consistent skin contact and drug delivery.[153] Skin irritation and sensitization potentials are assessed via in vivo models, such as primary dermal irritation in rabbits (historically using Draize scoring where mean scores below 1 indicate minimal irritation) or human repeated insult patch tests, with requirements for cumulative irritation scores not exceeding mild levels to mitigate dermatological risks.[154] The European Medicines Agency (EMA) applies analogous standards through its Guideline on the Quality of Transdermal Patches, emphasizing pharmaceutical development data including in vitro permeation across human or animal skin models to verify flux equivalence, alongside adhesion/cohesion balance to prevent issues like cold flow.[155] For generic applications, EMA requires demonstration of similarity in quality attributes, such as release profiles and impurity controls, without significant divergence from the originator. Post-1979 regulatory evolutions, including enhanced scrutiny under the 1976 Medical Device Amendments, have imposed stricter criteria for patches with structural innovations like microneedles, often classifying them as Class II or III devices necessitating premarket notification (510(k)) or approval (PMA) alongside drug review to address delivery mechanism reliability.[42][32]

Post-Market Monitoring and Recalls

Post-market surveillance for transdermal patches primarily relies on voluntary reporting systems such as the FDA's FAERS and MedWatch programs, which capture adverse events including device failures like adhesion issues that can compromise drug delivery and lead to therapeutic inefficacy. For instance, the FDA has documented numerous reports of adhesion failures in prescription lidocaine 5% patches, manifesting as edge curling, partial lifting, or complete detachment, potentially resulting in suboptimal pain relief and prompting investigations into manufacturing consistency.[156][157] These reports highlight gaps in real-world performance not fully anticipated during pre-market testing, with under-adhesion linked to factors like skin perspiration or application errors, though causal attribution remains challenging due to self-reported data limitations. Recalls of transdermal patches have occurred due to manufacturing defects affecting potency or delivery integrity. In January 2025, Alvogen, Inc. voluntarily recalled one lot of Fentanyl Transdermal System 25 mcg/h patches to the consumer level owing to a defective delivery system that could cause inconsistent dosing and elevate risks of respiratory depression or inadequate analgesia.[158] Similarly, Teva Pharmaceuticals USA recalled two lots of buprenorphine transdermal patches after testing revealed release rates below specifications, risking subtherapeutic opioid levels in chronic pain management.[159] Such actions underscore manufacturing variability as a causal factor in post-approval safety concerns, often identified through routine quality checks or sporadic adverse event clusters rather than widespread surveillance signals. Regulatory approaches vary internationally, with the European Medicines Agency (EMA) enforcing stricter controls on extractables and leachables—substances that may migrate from patch components into the skin or environment—potentially precipitating recalls for contamination risks not as stringently prioritized in U.S. guidelines.[155] The EMA's pharmacovigilance framework coordinates assessments of quality defects across member states, emphasizing systemic leachables testing to mitigate toxicity, which has led to targeted withdrawals in cases of non-compliance with these thresholds.[160] This contrast reflects differing emphases on environmental and long-term exposure hazards, though both regions depend on manufacturer-initiated recalls supplemented by passive reporting, exposing limitations in proactive detection of rare defects.

Recent Developments

Advances in Microneedle and Nanoparticle Integration

Dissolvable microneedles have advanced transdermal delivery by creating transient microchannels in the stratum corneum, enabling painless administration of biologics such as vaccines and insulin from 2020 onward. In preclinical models, dissolving microneedles loaded with Ag85B DNA vaccine for tuberculosis elicited robust immune responses at high doses, surpassing subcutaneous injection in antigen-specific T-cell activation.[161] For insulin, microneedle arrays in diabetic mouse models achieved sustained release over weeks, resulting in a 21.92% ± 2.51% body weight reduction and improved insulin sensitivity without hypoglycemia.[162] Emerging applications also include microneedle patches for skin tumor treatments, facilitating delivery of chemotherapy agents and enhancing photodynamic therapy by improving penetration to deeper lesions.[163] These developments address poor drug loading and dosing consistency challenges inherent in earlier designs.[164] Integration of nanoparticles, particularly liposomes and ethosomes, has enhanced the delivery of hydrophilic compounds by improving stratum corneum partitioning and reservoir effects. Ethosomes, with their smaller size and negative zeta potential, outperformed conventional liposomes in transdermal flux for hydrophilic drugs like 5-fluorouracil, achieving up to 2-3 fold permeation increases in ex vivo skin studies.[165] A 2023 review highlighted nanostructured lipid carriers in patches yielding 20-40% higher bioavailability for water-soluble actives compared to passive diffusion, attributed to lipid fusion with skin lipids.[166] These gains stem from nanoencapsulation stabilizing payloads against degradation and facilitating follicular and intercellular pathways. Hybrid systems merging microneedles with iontophoresis have shown promise for chronic conditions by combining mechanical disruption with electrophoretic forces. In ex vivo evaluations, olanzapine flux increased sharply—up to several-fold—when microneedles pretreated skin before iontophoretic application, enabling therapeutic levels for antipsychotic delivery.[167] For neurodegenerative diseases, electrically triggered microneedle patches in 2024 rodent trials delivered levodopa analogs on-demand, reducing motor symptoms in Parkinson's models with minimal skin irritation.[168] Such synergies mitigate variability in chronic disease management, though clinical translation requires addressing electrical safety and patch adhesion.[169]

Long-Acting and Smart Patch Innovations

Innovations in long-acting transdermal patches post-2020 have emphasized extended-release mechanisms, such as molecularly imprinted polymers (MIPs), which create tailored cavities for drugs to enable sustained diffusion over weeks, thereby minimizing reapplication frequency compared to daily systems. MIP-integrated formulations achieve high drug loading and near-zero-order release kinetics in prototypes, supporting durations up to monthly applications in preclinical models by controlling permeation rates through skin barriers.[37] These approaches address limitations of conventional matrix or reservoir patches, which typically last 1-7 days, by enhancing polymer-drug affinity for prolonged efficacy without burst release.[170] In opioid analgesia, buprenorphine patches exemplify this progression, with 7-day systems validated in 2024 clinical studies for chronic non-cancer pain, showing sustained analgesia and fewer adverse events over 12 months versus shorter-acting alternatives. Such patches maintain therapeutic plasma concentrations (e.g., 20-100 pg/mL) through optimized acrylic matrices, reducing dosing intervals while mitigating withdrawal risks associated with abrupt cessation.[171] Ongoing trials explore further extensions via hybrid MIP designs, though human data remain limited to weekly prototypes as of 2024.[172] Smart patches incorporate embedded sensors for real-time monitoring of adherence, drug flux, and biomarkers, enabling closed-loop adjustments via wireless feedback to apps or clinicians. For example, infrared sensor-integrated prototypes detect patch detachment or skin conditions, triggering automated release modulation or alerts, which preliminary bench tests indicate could reduce non-compliance by providing objective usage data.[173] These systems, often powered by flexible batteries or energy harvesting, have demonstrated in vitro responsiveness to physiological cues like pH or temperature, though regulatory hurdles persist for integrating electronics in FDA-approved devices.[174] Sustainability efforts in these innovations include biodegradable backings from natural polymers like hyaluronic acid or agro-waste derivatives, which degrade post-use to curb plastic waste from discarded patches—estimated at millions annually in healthcare. Such materials maintain adhesion and release profiles akin to synthetics in lab settings but face scalability issues, including inconsistent manufacturing yields and higher costs, limiting commercialization beyond prototypes.[175][176]

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