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Li-Wen Zhang

Bio: Li-Wen Zhang is an academic researcher from Chang Gung University. The author has contributed to research in topics: Transdermal & Photodynamic therapy. The author has an hindex of 1, co-authored 1 publications receiving 43 citations.

Papers
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Journal ArticleDOI
TL;DR: Enhanced delivery systems for ALA in the skin will play an important role in ALA-PDT, and several enhancement techniques for increasing ALA permeation through the skin are introduced.

46 citations


Cited by
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Journal ArticleDOI
TL;DR: Current understanding of the antimicrobial mechanisms used by ALA‐based PDT and its role in the treatment of microbial infections along with its potential medical and nonmedical applications are reviewed.
Abstract: Exogenous 5-aminolevulinic acid (ALA) is taken up directly by bacteria, yeasts, fungi, and some parasites, which then induces the accumulation of protoporphyrin IX (PPIX). Subsequent light irradiation of PPIX leads to the inactivation of these organisms via photodamage to their cellular structures. ALA uptake and light irradiation of PPIX produced by host cells leads to the inactivation of other parasites, along with some viruses, via the induction of an immune response. ALA-mediated PPIX production by host cells and light irradiation result in the inactivation of other viruses via either the induction of a host cell response or direct photodynamic attack on viral particles. This ALA-mediated production of light-activated PPIX has been extensively used as a form of photodynamic therapy (PDT) and has shown varying levels of efficacy in treating conditions that are associated with microbial infection, ranging from acne and verrucae to leishmaniasis and onychomycosis. However, for the treatment of some of these conditions by ALA-based PDT, the role of an antimicrobial effect has been disputed and in general, the mechanisms by which the technique inactivates microbes are not well understood. In this study, we review current understanding of the antimicrobial mechanisms used by ALA-based PDT and its role in the treatment of microbial infections along with its potential medical and nonmedical applications.

121 citations

Journal ArticleDOI
Xiao Zhao1, Xinfang Li1, Peng Zhang1, Jianwei Du1, Youxiang Wang1 
TL;DR: In a subcutaneous mouse tumor model established in BALB/c nude mice, the PDT efficacy of ALA‐loaded HA microneedle group was much better than ALA injection group in spite of a relatively lower ALA dose with HA micronedles.

99 citations

Book ChapterDOI
14 Nov 2014
TL;DR: PACT therapy involves the use of a chemical dye which targets the organism cell wall, in this case the fungus, and the release of oxygen helps to destroy the cell wall of the fungus.
Abstract: PACT therapy involves the use of a chemical dye which targets the organism cell wall, in this case the fungus. The dye is activated by a high powered lamp which starts a chemical reaction, and the release of oxygen into the affected nail plate. This sudden and prolonged release of oxygen helps to destroy the cell wall of the fungus and over the course of your treatment helps to eradicate it from your nail plate.

96 citations

Journal ArticleDOI
TL;DR: This potential use of the laser affords a new treatment for topical/transdermal application with significant efficacy and should be used in optimizing the feasible conditions of the lasers in balancing the effectiveness of permeation enhancement and skin damage.
Abstract: Introduction: Using lasers can be an effective drug permeation-enhancement approach for facilitating drug delivery into or across the skin. The controlled disruption and ablation of the stratum corneum (SC), the predominant barrier for drug delivery, is achieved by the use of lasers. The possible mechanisms of laser-assisted drug permeation are the direct ablation of the skin barrier, optical breakdown by a photomechanical wave and a photothermal effect. It has been demonstrated that ablative approaches for enhancing drug transport provide some advantages, including increased bioavailability, fast treatment time, quick recovery of SC integrity and the fact that skin surface contact is not needed. In recent years, the concept of using laser techniques to treat the skin has attracted increasing attention. Areas covered: This review describes recent developments in using nonablative and ablative lasers for drug absorption enhancement. This review systematically introduces the concepts and enhancement mechani...

71 citations

Journal ArticleDOI
10 Sep 2015-PLOS ONE
TL;DR: The in vivo percutaneous absorption of ALA and rhodamine B examined by confocal microscopy confirmed the deficient resistance of epidermal barrier for facilitating cutaneous delivery of drugs via psoriasis-like skin and established the topical delivery profiles of anti-psoriatic drugs via imiquimod-treated psoriiasis- like skin.
Abstract: Objective Psoriasis is a chronic inflammatory skin disease and topical therapy remains a key role for treatment. The aim of this study is to evaluate the influence of psoriasis-like lesions on the cutaneous permeation of anti-psoriatic drugs. Methods We first set up imiquimod-induced dermatitis in mice that closely resembles human psoriasis lesions. The development of the lesions is based on the IL-23/IL17A axis for phenotypical and histological characteristics. Four drugs, 5-aminolevulinic acid (ALA), tacrolimus, calcipotriol, and retinoic acid, were used to evaluate percutaneous absorption. Results The most hydrophilic molecule, ALA, revealed the greatest enhancement on skin absorption after imiquimod treatment. Imiquimod increased the skin deposition and flux of ALA by 5.6 to 14.4-fold, respectively, compared to normal skin. The follicular accumulation of ALA was also increased 3.8-fold. The extremely lipophilic drug retinoic acid showed a 1.7- and 3.8-fold increase in skin deposition and flux, respectively. Tacrolimus flux was enhanced from 2 to 21 μg/cm2/h by imiquimod intervention. However, imiquimod did not promote skin deposition of this macrolide. The lipophilicity, but not the molecular size, dominated drug permeation enhancement by psoriatic lesions. The in vivo percutaneous absorption of ALA and rhodamine B examined by confocal microscopy confirmed the deficient resistance of epidermal barrier for facilitating cutaneous delivery of drugs via psoriasis-like skin. Conclusion We established the topical delivery profiles of anti-psoriatic drugs via imiquimod-treated psoriasis-like skin.

49 citations