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调制光敏化过程以改善靶向光动力疗法。

Modulation of photosensitization processes for an improved targeted photodynamic therapy.

机构信息

Laboratoire Réactions et Génie des Procédés, Nancy-Université, CNRS, 1 rue Grandville BP 20451, 54001, Nancy, France.

出版信息

Curr Med Chem. 2010;17(32):3925-43. doi: 10.2174/092986710793205453.

Abstract

Photodynamic therapy (PDT) is a cancer treatment modality involving the combination of light, a photosensitizer (PS) and molecular oxygen, which results in the production of cytotoxic reactive oxygen species (ROS). Singlet oxygen ((1)O(2)) is one of the most important of these ROS. Because the lifetime and diffusion of (1)O(2) is very limited, a controllable singlet oxygen generation with high selectivity and localization would lead to more efficient and reliable PDT. The lack of selective accumulation of the PS within tumour tissue is a major problem in PDT. Targeted PDT would offer the advantage to enhance photodynamic efficiency by directly targeting diseased cells or tissues. Many attempts have been made to either selectively deliver light to diseased tissues or increase the uptake of the photoactive compounds by the target cells. The review will survey the literature regarding the multi-level control of (1)O(2) production for PDT applications. The mechanisms of ROS formation are described. The different strategies leading to targeted formation of (1)O(2) are developed. Some active PDT agents have been based on energy transfer between PS by control of the aggregation/ disaggregation. The concept of molecular beacon based on quenching-dequenching upon protease cleavage is capable of precise control of (1)O(2) by responding to specific cancer-associated biomarkers.

摘要

光动力疗法(PDT)是一种癌症治疗方式,涉及光、光敏剂(PS)和分子氧的结合,从而产生细胞毒性活性氧(ROS)。单线态氧((1)O(2))是这些 ROS 中最重要的一种。由于(1)O(2)的寿命和扩散非常有限,因此具有高选择性和定位的可控单线态氧生成将导致更有效和可靠的 PDT。PS 在肿瘤组织内缺乏选择性积累是 PDT 的一个主要问题。靶向 PDT 通过直接靶向患病细胞或组织提供了提高光动力效率的优势。已经做出了许多尝试来选择性地将光传递到患病组织,或通过靶细胞增加光活性化合物的摄取。该综述将调查有关 PDT 应用中(1)O(2)产生的多水平控制的文献。描述了 ROS 形成的机制。开发了导致(1)O(2)靶向形成的不同策略。一些活性 PDT 剂基于 PS 通过控制聚集/解聚集之间的能量转移。基于蛋白酶切割时淬灭-去淬灭的分子信标概念能够通过响应特定的癌症相关生物标志物来精确控制(1)O(2)。

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