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局部光动力疗法治疗良性皮肤病:原理与新应用

Topical PDT in the Treatment of Benign Skin Diseases: Principles and New Applications.

作者信息

Kim Miri, Jung Haw Young, Park Hyun Jeong

机构信息

Department of Dermatology, Yeouido St. Mary's Hospital, The Catholic University of Korea, Seoul 150-713, Korea.

出版信息

Int J Mol Sci. 2015 Sep 25;16(10):23259-78. doi: 10.3390/ijms161023259.

Abstract

Photodynamic therapy (PDT) uses a photosensitizer, light energy, and molecular oxygen to cause cell damage. Cells exposed to the photosensitizer are susceptible to destruction upon light absorption because excitation of the photosensitizing agents leads to the production of reactive oxygen species and, subsequently, direct cytotoxicity. Using the intrinsic cellular heme biosynthetic pathway, topical PDT selectively targets abnormal cells, while preserving normal surrounding tissues. This selective cytotoxic effect is the basis for the use of PDT in antitumor treatment. Clinically, PDT is a widely used therapeutic regimen for oncologic skin conditions such as actinic keratosis, squamous cell carcinoma in situ, and basal cell carcinoma. PDT has been shown, under certain circumstances, to stimulate the immune system and produce antibacterial, and/or regenerative effects while protecting cell viability. Thus, it may be useful for treating benign skin conditions. An increasing number of studies support the idea that PDT may be effective for treating acne vulgaris and several other inflammatory/infective skin diseases, including psoriasis, rosacea, viral warts, and aging-related changes. This review provides an overview of the clinical investigations of PDT and discusses each of the essential aspects of the sequence: its mechanism of action, common photosensitizers, light sources, and clinical applications in dermatology. Of the numerous clinical trials of PDT in dermatology, this review focuses on those studies that have reported remarkable therapeutic benefits following topical PDT for benign skin conditions such as acne vulgaris, viral warts, and photorejuvenation without causing severe side effects.

摘要

光动力疗法(PDT)利用光敏剂、光能和分子氧来造成细胞损伤。暴露于光敏剂的细胞在吸收光后易受破坏,因为光敏剂的激发会导致活性氧的产生,进而产生直接的细胞毒性。利用细胞内源性血红素生物合成途径,局部光动力疗法可选择性地靶向异常细胞,同时保留周围正常组织。这种选择性细胞毒性作用是光动力疗法用于抗肿瘤治疗的基础。临床上,光动力疗法是一种广泛应用于治疗诸如光化性角化病、原位鳞状细胞癌和基底细胞癌等肿瘤性皮肤病的治疗方案。在某些情况下,光动力疗法已被证明可刺激免疫系统并产生抗菌和/或再生作用,同时保护细胞活力。因此,它可能对治疗良性皮肤病有用。越来越多的研究支持光动力疗法可能有效治疗寻常痤疮和其他几种炎症性/感染性皮肤病的观点,包括银屑病、玫瑰痤疮、病毒疣和与衰老相关的变化。本综述概述了光动力疗法的临床研究,并讨论了该疗法的各个基本方面:其作用机制、常用光敏剂、光源以及在皮肤科的临床应用。在众多光动力疗法在皮肤科的临床试验中,本综述重点关注那些报道局部光动力疗法对寻常痤疮、病毒疣和光嫩肤等良性皮肤病具有显著治疗益处且未引起严重副作用的研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ece9/4632697/951c093b75f7/ijms-16-23259-g001.jpg

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