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光笼式DNA结合光敏剂实现双靶点光动力疗法中核进入的光控

Photocaged DNA-Binding Photosensitizer Enables Photocontrol of Nuclear Entry for Dual-Targeted Photodynamic Therapy.

作者信息

Digby Elyse M, Ayan Seylan, Shrestha Pradeep, Gehrmann Elizabeth J, Winter Arthur H, Beharry Andrew A

机构信息

Department of Chemical and Physical Sciences, University of Toronto Mississauga, Mississauga, OntarioL5L 1C6, Canada.

Department of Chemistry, Iowa State University, Ames, Iowa50011, United States.

出版信息

J Med Chem. 2022 Dec 22;65(24):16679-16694. doi: 10.1021/acs.jmedchem.2c01504. Epub 2022 Dec 8.

Abstract

Photodynamic therapy (PDT) is a clinically approved cancer treatment that requires a photosensitizer (PS), light, and molecular oxygen─a combination which produces reactive oxygen species (ROS) that can induce cancer cell death. To enhance the efficacy of PDT, dual-targeted strategies have been explored where two photosensitizers are administered and localize to different subcellular organelles. To date, a single small-molecule conjugate for dual-targeted PDT with light-controlled nuclear localization has not been achieved. We designed a probe composed of a DNA-binding PS (Br-DAPI) and a photosensitizing photocage (WinterGreen). Illumination with 480 nm light removes WinterGreen from the conjugate and produces singlet oxygen mainly in the cytosol, while Br-DAPI localizes to nuclei, binds DNA, and produces ROS using one- or two-photon illumination. We observe synergistic photocytotoxicity in MCF7 breast cancer cells, and a reduction in size of three-dimensional (3D) tumor spheroids, demonstrating that nuclear/cytosolic photosensitization using a single agent can enhance PDT efficacy.

摘要

光动力疗法(PDT)是一种临床批准的癌症治疗方法,它需要一种光敏剂(PS)、光和分子氧,这种组合会产生活性氧(ROS),从而诱导癌细胞死亡。为了提高光动力疗法的疗效,人们探索了双靶向策略,即使用两种光敏剂并使其定位于不同的亚细胞器。迄今为止,尚未实现具有光控核定位的用于双靶向光动力疗法的单一小分子共轭物。我们设计了一种由DNA结合光敏剂(Br-DAPI)和光敏光笼(冬绿油)组成的探针。用480nm光照射会使冬绿油从共轭物中脱离,并主要在细胞质中产生单线态氧,而Br-DAPI定位于细胞核,结合DNA,并通过单光子或双光子照射产生活性氧。我们在MCF7乳腺癌细胞中观察到协同光细胞毒性,并且三维(3D)肿瘤球体的尺寸减小,这表明使用单一试剂进行核/细胞质光敏化可以提高光动力疗法的疗效。

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