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基于偶氮的光动力治疗敏化剂的在低氧条件下的开发。

Development of an Azo-Based Photosensitizer Activated under Mild Hypoxia for Photodynamic Therapy.

机构信息

Graduate School of Pharmaceutical Sciences, The University of Tokyo , 7-3-1 Hongo, Bunkyo-ku, Tokyo 113-0033, Japan.

Molecular Spectroscopy Laboratory, RIKEN , 2-1 Hirosawa, Wako 351-0198, Japan.

出版信息

J Am Chem Soc. 2017 Oct 4;139(39):13713-13719. doi: 10.1021/jacs.7b05019. Epub 2017 Sep 25.

Abstract

Photodynamic therapy (PDT) utilizes photoirradiation in the presence of photosensitizers to ablate cancer cells via generation of singlet oxygen (O), but it is important to minimize concomitant injury to normal tissues. One approach for achieving this is to use activatable photosensitizers that can generate O only under specific conditions. Here, we report a novel photosensitizer that is selectively activated under hypoxia, a common condition in solid tumors. We found that introducing an azo moiety into the conjugated system of a seleno-rosamine dye effectively hinders the intersystem crossing process that leads to O generation. We show that the azo group is reductively cleaved in cells under hypoxia, enabling production of O to occur. In PDT in vitro, cells under mild hypoxia, within the range typically found in solid tumors (up to about 5% O), were selectively ablated, leaving adjacent normoxic cells intact. This simple and practical azo-based strategy should be widely applicable to design a range of activatable photosensitizers.

摘要

光动力疗法(PDT)利用光敏剂在光照射下产生单线态氧(O)来消融癌细胞,但重要的是要尽量减少对正常组织的伴随损伤。实现这一目标的一种方法是使用可激活的光敏剂,只有在特定条件下才能产生 O。在这里,我们报告了一种新型的光敏剂,它可以在缺氧条件下选择性激活,缺氧是实体肿瘤中的常见情况。我们发现,在硒-罗沙明染料的共轭系统中引入偶氮基团可以有效地阻止导致 O 生成的系间穿越过程。我们表明,在缺氧条件下,细胞中的偶氮基团被还原裂解,从而能够发生 O 的生成。在体外 PDT 中,轻度缺氧下的细胞(通常在实体肿瘤中发现的范围内,约 5% O)被选择性消融,而相邻的正常氧细胞则完好无损。这种简单实用的基于偶氮的策略应该广泛适用于设计一系列可激活的光敏剂。

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