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Far-Red Fluorescence Probe for Monitoring Singlet Oxygen during Photodynamic Therapy

机译:远红色荧光探针,用于在光动力治疗期间监测单线态氧

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摘要

Singlet oxygen (~1O_2), molecular oxygen in the lowest excited state, has a critical role in the cell-killing mechanism of photodynamic therapy (PDT). Although ~1O_2 phosphorescence measurement has been mainly used to monitor ~1O_2 formation during PDT, its intensity is far insufficient to obtain two-dimensional images of intracellular ~1O_2 with the subcellular spatial resolution using the currently available near-IR detector. Here, we propose a new far-red fluorescence probe of ~1O_2, namely, Si-DMA, composed of silicon-containing rhodamine and anthracene moieties as a chromophore and a ~1O_2 reactive site, respectively. In the presence of ~1O_2, fluorescence of Si-DMA increases 17 times due to endoperoxide formation at the anthracene moiety. With the advantage of negligible self-oxidation by photoirradiation Φ_Δ < 0.02) and selective mitochondrial localization, Si-DMA is particularly suitable for imaging ~1O_2 during PDT. Among three different intracellular photosensitizers (Sens), Si-DMA could selectively detect the ~1O_2 that is generated by 5-aminolevulinic acid-derived protoporphyrin Ⅸ, colocalized with Si-DMA in mitochondria. On the other hand, mitochondria-targeted KillerRed and lysosomal porphyrins could not induce fluorescence change of Si-DMA. This surprising selectivity of Si-DMA response depending on the Sens localization and photosensitization mechanism is caused by a limited intracellular ~1O_2 diffusion distance (~300 nm) and negligible generation of ~1O_2 by type-Ⅰ Sens, respectively. For the first time, we successfully visualized ~1O_2 generated during PDT with a spatial resolution of a single mitochondrial tubule.
机译:单重态氧(〜1O_2)是处于最低激发态的分子氧,在光动力疗法(PDT)的细胞杀伤机制中具有关键作用。尽管〜1O_2磷光测量主要用于监视PDT中〜1O_2的形成,但其强度远远不足以使用当前可用的近红外探测器获得亚细胞空间分辨率的细胞内〜1O_2的二维图像。在这里,我们提出了一种新的〜1O_2的远红外荧光探针,即Si-DMA,它由含硅的若丹明和蒽部分分别作为生色团和〜1O_2反应位点组成。在〜1O_2存在下,由于在蒽部分形成过氧化物,Si-DMA的荧光增加了17倍。 Si-DMA的优点是可以忽略不计的光辐射自氧化(Φ_Δ<0.02)和线粒体选择性定位,特别适合在PDT期间对〜1O_2成像。在三种不同的细胞内光敏剂(Sens)中,Si-DMA可以选择性检测由5-氨基乙酰丙酸衍生的原卟啉Ⅸ与Si-DMA共定位于线粒体中产生的〜1O_2。另一方面,针对线粒体的KillerRed和溶酶体卟啉不能诱导Si-DMA的荧光变化。取决于Sens定位和光敏化机理的Si-DMA响应的这种令人惊讶的选择性分别是由有限的细胞内〜1O_2扩散距离(〜300 nm)和可忽略的Ⅰ型Sens产生的〜1O_2引起的。首次,我们以单个线粒体小管的空间分辨率成功地观察了PDT过程中产生的〜1O_2。

著录项

  • 来源
    《Journal of the American Chemical Society》 |2014年第33期|11707-11715|共9页
  • 作者单位

    The Institute of Scientific and Industrial Research (SANKEN), Osaka University, Mihogaoka 8-1, Osaka, Ibaraki 567-0047, Japan;

    The Institute of Scientific and Industrial Research (SANKEN), Osaka University, Mihogaoka 8-1, Osaka, Ibaraki 567-0047, Japan;

    The Institute of Scientific and Industrial Research (SANKEN), Osaka University, Mihogaoka 8-1, Osaka, Ibaraki 567-0047, Japan;

    The Institute of Scientific and Industrial Research (SANKEN), Osaka University, Mihogaoka 8-1, Osaka, Ibaraki 567-0047, Japan;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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  • 入库时间 2022-08-18 03:11:11

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