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首页> 外文期刊>Nanoscale >An acceptor-shielding strategy of photosensitizers for enhancing the generation efficiency of type I reactive oxygen species and the related photodynamic immunotherapy
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An acceptor-shielding strategy of photosensitizers for enhancing the generation efficiency of type I reactive oxygen species and the related photodynamic immunotherapy

机译:一种提高I型活性氧生成效率的光敏剂受体屏蔽策略及相关光动力免疫疗法

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摘要

Developing efficient photosensitizers (PSs) that can generate type I reactive oxygen species (ROS) under illumination is considered an effective way to improve photodynamic therapy (PDT) outcomes due to the hypoxic nature of the tumor environment, but also is very challenging. Herein, a new PS of the multiarylpyrrole (MAP) derivative with a typical donor–acceptor structure was synthesized to efficiently generate type I ROS by using an acceptor-shielding strategy in their aggregated state. The enhanced generation mechanism of type I ROS originated from its ultralong triplet lifetime and the narrow singlet–triplet energy gap of the MAP. More importantly, type I ROS can transform protumoral M2 macrophages (M2) into antitumoral M1 macrophages (M1), which showed synergistic immunotherapy in in vivo experiments. Therefore, introducing shielding groups into acceptors provides general guidance for developing efficient PSs in the aggregation state for clinical PDT.
机译:发展有效的敏化(PSs)可以生成I型活性氧(ROS)在照明被认为是有效的方法提高光动力疗法(PDT)的结果由于缺氧肿瘤的性质环境,但也非常具有挑战性。这里,一个新的PS multiarylpyrrole(地图)导数与一个典型的亲结构是合成高效地生成通过使用一个acceptor-shielding I型ROS在他们的聚合状态的战略。I型ROS的产生机制从它的超长三联体一生和缩小singlet-triplet能量差距的地图。更重要的是,我ROS可以变换类型antitumoral protumoral M2巨噬细胞(M2)M1巨噬细胞(M1),显示协同在体内实验中免疫疗法。将屏蔽组引入受体为发展提供一般指导高效的PSs的聚合状态临床PDT。

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