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      Current regulatory scenario and alternative surrogate methods to establish bioequivalence of topical generic products

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      Journal of Drug Delivery Science and Technology
      Elsevier BV

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          Is Open Access

          Skin models for the testing of transdermal drugs

          The assessment of percutaneous permeation of molecules is a key step in the evaluation of dermal or transdermal delivery systems. If the drugs are intended for delivery to humans, the most appropriate setting in which to do the assessment is the in vivo human. However, this may not be possible for ethical, practical, or economic reasons, particularly in the early phases of development. It is thus necessary to find alternative methods using accessible and reproducible surrogates for in vivo human skin. A range of models has been developed, including ex vivo human skin, usually obtained from cadavers or plastic surgery patients, ex vivo animal skin, and artificial or reconstructed skin models. Increasingly, largely driven by regulatory authorities and industry, there is a focus on developing standardized techniques and protocols. With this comes the need to demonstrate that the surrogate models produce results that correlate with those from in vivo human studies and that they can be used to show bioequivalence of different topical products. This review discusses the alternative skin models that have been developed as surrogates for normal and diseased skin and examines the concepts of using model systems for in vitro–in vivo correlation and the demonstration of bioequivalence.
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            Overcoming the Stratum Corneum: The Modulation of Skin Penetration

            It is preferred that topically administered drugs act either dermally or transdermally. For that reason they have to penetrate into the deeper skin layers or permeate the skin. The outermost layer of the human skin, the stratum corneum, is responsible for its barrier function. Most topically administered drugs do not have the ability to penetrate the stratum corneum. In these cases modulations of the skin penetration profiles of these drugs and skin barrier manipulations are necessary. A skin penetration enhancement can be achieved either chemically, physically or by use of appropriate formulations. Numerous chemical compounds have been evaluated for penetration-enhancing activity, and different modes of action have been identified for skin penetration enhancement. In addition to chemical methods, skin penetration of drugs can be improved by physical options such as iontophoresis and phonophoresis, as well as by combinations of both chemical and physical methods or by combinations of several physical methods. There are cases where skin penetration of the drug used in the formulation is not the aim of the topical administration. Penetration reducers can be used to prevent chemicals entering the systemic circulation. This article concentrates on the progress made mainly over the last decade by use of chemical penetration enhancers. The different action modes of these substances are explained, including the basic principles of the physical skin penetration enhancement techniques and examples for their application.
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              New insights into skin structure: scratching the surface.

              The formation, structural organization, and barrier functions of stratum corneum (SC) are reviewed. Stratum corneum is considered as a composite material and a biopolymer with properties so unique as to consider it a 'smart material'. SC, together with stratum granulosum (SG) responds (as an actively smart material) to environmental signals with appropriate modulations in its barrier properties. Current theories on the mode of barrier formation, validity of use of animal models and ex vivo human skin in studies of percutaneous absorption, as well as its implications in development of transdermal systems (TDS) are discussed. Potential pitfalls in extrapolating from animal data and the use of cadaver skin/epidermal membranes in evaluations of TDS are also stressed.
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                Author and article information

                Contributors
                (View ORCID Profile)
                Journal
                Journal of Drug Delivery Science and Technology
                Journal of Drug Delivery Science and Technology
                Elsevier BV
                17732247
                February 2021
                February 2021
                : 61
                : 102090
                Article
                10.1016/j.jddst.2020.102090
                8a477b48-9675-48f8-a9c9-0cf9d191fbe3
                © 2021

                https://www.elsevier.com/tdm/userlicense/1.0/

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