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Apoptotic and autophagic responses to photodynamic therapy in 1c1c7 murine hepatoma cells

机译:1c1c7小鼠肝癌细胞对光动力疗法的凋亡和自噬反应

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摘要

Photodynamic therapy (PDT) is a process that can induce apoptosis, autophagy or both depending on the cell phenotype. Apoptosis is a pathway to cell death while autophagy can protect from photokilling or act as a death pathway. In a previous study, we reported a cytoprotective effect of autophagy in murine leukemia cell lines where both autophagy and apoptosis occur within minutes after irradiation of photosensitized cells. In this study, we examined the effects of mitochondrial photodamage catalyzed by low (≤1 µM) concentrations of the photosensitizing agent termed benzoporphyrin derivative (BPD, Verteporfin) on murine hepatoma 1c1c7 cells. Apoptosis was not observed until several hours after irradiation of photosensitized cells. Autophagy was clearly cytoprotective since PDT efficacy was significantly enhanced in a knockdown sub-line (KD) in which the level of a critical autophagy protein (Atg7) was markedly reduced. This result indicates that autophagy can protect from phototoxicity even when apoptosis is substantially delayed. Much higher concentrations (≥10 µM) of BPD had previously been shown to inhibit autophagosome formation. Phototoxicity studies performed with 10 µM BPD and a proportionally reduced light dose were consistent with the absence of an autophagic process in wild-type (WT) cells under these conditions.
机译:光动力疗法(PDT)是一个可以诱导凋亡,自噬或同时取决于细胞表型的过程。凋亡是细胞死亡的途径,而自噬可以保护细胞免受光杀作用或充当死亡途径。在以前的研究中,我们报道了自噬在小鼠白血病细胞系中的细胞保护作用,其中自噬和凋亡均在光敏细胞照射后数分钟内发生。在这项研究中,我们检查了低浓度(≤1µM)的光敏剂苯并卟啉衍生物(BPD,Verteporfin)对小鼠肝癌1c1c7细胞催化的线粒体光损伤的影响。直到光敏细胞照射几小时后才观察到细胞凋亡。自噬明显具有细胞保护作用,因为在击倒亚系(KD)中PDT的功效显着增强,其中关键自噬蛋白(Atg7)的水平明显降低。该结果表明,即使细胞凋亡被显着延迟,自噬也可以防止光毒性。先前已证明更高浓度的BPD(≥10µM)会抑制自噬体的形成。在这些条件下,使用10 µM BPD和成比例减少的光剂量进行的光毒性研究与野生型(WT)细胞中不存在自噬过程一致。

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