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利用类胡萝卜素在光动力分子信标中的单线态氧清除特性,将对非靶向细胞的光损伤降至最低。

Using the singlet oxygen scavenging property of carotenoid in photodynamic molecular beacons to minimize photodamage to non-targeted cells.

作者信息

Chen Juan, Jarvi Mark, Lo Pui-Chi, Stefflova Klara, Wilson Brian C, Zheng Gang

机构信息

Division of Biophysics and Bioimaging, Ontario Cancer Institute, Toronto, ON M5G 1L7, Canada.

出版信息

Photochem Photobiol Sci. 2007 Dec;6(12):1311-7. doi: 10.1039/b706820d. Epub 2007 Aug 20.

DOI:10.1039/b706820d
PMID:18046487
Abstract

We recently introduced the concept of photodynamic molecular beacons (PMB) for selective control of photodynamic therapy (PDT). The PMB consists of a peptide linker that is sequence specific to a cancer-associated protease. A photosensitizer (PS) and a singlet oxygen (1O2) quencher are conjugated to the opposite ends of this linker. Proximity of the PS and quencher can efficiently inhibit 1O2 generation. In the presence of a targeted protease, the substrate sequence is cleaved and the PS and quencher will separate so that the PS can be photo-activated. There are two ways to optimize the PMB selectivity to cancer cells. The first is to increase the protease specificity to targeted cells and the second is to minimize the phototoxicity of intact (uncleaved) PMBs in non-targeted (normal) cells. Carotenoids (CARs) are well known in nature for their role in quenching excited states of PS and in directly scavenging 1O2. The purpose of this study is to evaluate whether the CAR with dual quenching modes (PS excited states deactivation and 1O2 scavenging) can be used to minimize the photodamage of intact PMBs to non-targeted cells. Thus, we synthesized a beacon (PPC) with a caspase-3 cleavable peptide linking a PS and a CAR quencher. It was confirmed that CAR deactivates the PS excited states and also directly scavenges 1O2. Moreover, the in vitro PDT response showed that CAR completely shuts off the photodynamic effect in non-targeted HepG(2) cells, while PS without CAR (control) remains highly potent even at a much lower (30-fold) dose.

摘要

我们最近引入了光动力分子信标(PMB)的概念,用于光动力疗法(PDT)的选择性控制。PMB由一个与癌症相关蛋白酶具有序列特异性的肽接头组成。一种光敏剂(PS)和一个单线态氧(1O2)猝灭剂与该接头的相对两端相连。PS和猝灭剂的接近可以有效抑制1O2的产生。在靶向蛋白酶存在的情况下,底物序列被切割,PS和猝灭剂将分离,从而使PS能够被光激活。有两种方法可以优化PMB对癌细胞的选择性。第一种是提高蛋白酶对靶向细胞的特异性,第二种是将完整(未切割)的PMB在非靶向(正常)细胞中的光毒性降至最低。类胡萝卜素(CARs)在自然界中因其在猝灭PS激发态和直接清除1O2方面的作用而广为人知。本研究的目的是评估具有双重猝灭模式(PS激发态失活和1O2清除)的CAR是否可用于将完整PMB对非靶向细胞的光损伤降至最低。因此,我们合成了一种信标(PPC),其具有一个可被半胱天冬酶-3切割的肽,连接一个PS和一个CAR猝灭剂。已证实CAR可使PS激发态失活,并直接清除1O2。此外,体外PDT反应表明,CAR完全关闭了非靶向HepG(2)细胞中的光动力效应,而没有CAR的PS(对照)即使在低得多(30倍)的剂量下仍保持高效。

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