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光动力疗法治疗皮肤癌:如何增强药物渗透?

Photodynamic therapy for skin cancer: How to enhance drug penetration?

机构信息

LETI-DTBS, CEA, 17 rue des Martyrs, Grenoble Cedex, France; U1189 - ONCO-THAI - Image Assisted Laser Therapy for Oncology, CHU Lille, Univ. Lille, Inserm, F-59000 Lille, France.

LETI-DTBS, CEA, 17 rue des Martyrs, Grenoble Cedex, France.

出版信息

J Photochem Photobiol B. 2019 Aug;197:111544. doi: 10.1016/j.jphotobiol.2019.111544. Epub 2019 Jul 2.

Abstract

Photodynamic therapy (PDT) induced by protoporphyrin IX (PpIX) has been widely used in dermatological practices such as treatment of skin cancers. Clearance rate depends on different factors such as light irradiation, skin oxygenation and drug penetration. The poor penetration of 5-aminolevulinic acid (5-ALA) with topical application is limited and restrains the production of PpIX which could restrict PDT outcomes. This review will focus on techniques already used to enhance drug penetration in human skin, and will present their results, advantages, and drawbacks. Chemical and physical pretreatments will be discussed. Chemical pre-treatments comprise of drug formulation modification, use of agents that modify the heme cycle, enhance PpIX formation, and the combination of differentiation-promoting agent prior to PDT. On the other hand, physical pretreatments affect the skin barrier by creating holes in the skin or by removing stratum corneum. To promote drug penetration, iontophoresis and temperature modulation are interesting alternative methods. Cellular mechanisms enrolled during chemical or physical pretreatments have been investigated in order to understand how 5-ALA penetrates the skin, why it is preferentially metabolized in PpIX in tumour cells, and how it could be accumulated in deeper skin layers. The objective of this review is to compare clinical trials that use innovative technology to conventional PDT treatment. Most of these pretreatments present good or even better clinical outcomes than usual PDT.

摘要

光动力疗法(PDT)由原卟啉 IX(PpIX)诱导,已广泛应用于皮肤科治疗皮肤癌等领域。清除率取决于不同因素,如光辐射、皮肤氧合和药物渗透。局部应用 5-氨基酮戊酸(5-ALA)的渗透能力差,限制了 PpIX 的产生,从而可能限制 PDT 的效果。本综述将重点介绍已用于增强人皮肤中药物渗透的技术,并介绍其结果、优点和缺点。将讨论化学和物理预处理。化学预处理包括药物制剂的修饰、使用改变血红素循环、增强 PpIX 形成的试剂,以及在 PDT 之前使用分化促进剂。另一方面,物理预处理通过在皮肤中形成孔或去除角质层来影响皮肤屏障。为了促进药物渗透,离子电渗疗法和温度调节是很有前途的替代方法。为了了解 5-ALA 如何渗透皮肤、为何它在肿瘤细胞中优先代谢为 PpIX 以及如何在更深的皮肤层中积累,研究了化学或物理预处理过程中涉及的细胞机制。本综述的目的是比较使用创新技术与传统 PDT 治疗的临床试验。这些预处理中的大多数比常规 PDT 具有更好或甚至更好的临床效果。

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