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Current Limitations and Recent Progress in Nanomedicine for Clinically Available Photodynamic Therapy

机译:临床可用光动力疗法纳米医生的当前限制和最近进展

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摘要

Photodynamic therapy (PDT) using oxygen, light, and photosensitizers has been receiving great attention, because it has potential for making up for the weakness of the existing therapies such as surgery, radiation therapy, and chemotherapy. It has been mainly used to treat cancer, and clinical tests for second-generation photosensitizers with improved physicochemical properties, pharmacokinetic profiles, or singlet oxygen quantum yield have been conducted. Progress is also being made in cancer theranostics by using fluorescent signals generated by photosensitizers. In order to obtain the effective cytotoxic effects on the target cells and prevent off-target side effects, photosensitizers need to be localized to the target tissue. The use of nanocarriers combined with photosensitizers can enhance accumulation of photosensitizers in the tumor site, owing to preferential extravasation of nanoparticles into the tumor vasculature by the enhanced permeability and retention effect. Self-assembly of amphiphilic polymers provide good loading efficiency and sustained release of hydrophobic photosensitizers. In addition, prodrug nanomedicines for PDT can be activated by stimuli in the tumor site. In this review, we introduce current limitations and recent progress in nanomedicine for PDT and discuss the expected future direction of research.
机译:光动力治疗(PDT)使用氧气,光线和光敏剂得到了极大的关注,因为它具有弥补现有疗法的弱点,如手术,放射治疗和化疗等疗法。已经主要用于治疗癌症,并且已经进行了具有改善的物理化学性质,药代动力学谱或单线氧量子产率的第二代光敏剂的临床试验。通过使用由光敏剂产生的荧光信号,还在癌症治疗中进行进展。为了获得对靶细胞的有效细胞毒性作用并防止脱靶副作用,光敏剂需要定位于靶组织。使用纳米载体与光敏剂联合的使用可以增强肿瘤部位的光敏剂积聚,由于纳米颗粒通过增强的渗透率和保留效应来渗入肿瘤脉管系统。两亲性聚合物的自组装提供良好的装载效率和疏水性光敏剂的持续释放。此外,PDT的前药纳米胺可以通过肿瘤部位的刺激激活。在这篇综述中,我们在PDT介绍了纳米医生的当前限制和最近进展,并讨论了预期的未来研究方向。

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