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Intercellular singlet oxygen-mediated bystander signaling triggered by long-lived species of cold atmospheric plasma and plasma-activated medium

机译:长寿命物种的冷大气血浆和血浆激活培养基触发细胞间单线态氧介导的旁观者信号

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Treatment of tumor cells with Hsub2/subOsub2/sub and nitrite, two long-lived species derived from cold atmospheric plasma, induces a complex autoamplificatory, singlet oxygen-mediated process, which leads to catalase inactivation and reactivation of intercellular apoptosis-inducing signaling. Experimental dissection and quantification of this process is described in this study. When tumor cells were pretreated with Hsub2/subOsub2/sub and nitrite, and then were added to untreated tumor cells, they propaged singlet oxygen mediated catalase inactivation and generation of singlet oxygen to the untreated cell population. This bystander effect allowed to analyze the biochemical requirements of a) induction of the bystander effect-inducing potential, b) transmission of the bystander effect to untreated neighbouring cells, and c) the biochemical consequences of these signaling events. The induction of bystander effect-inducing potential requires the generation of “primary singlet oxygen” through the reactions following the interaction between nitrite and Hsub2/subOsub2/sub, followed by local inactivation of a few catalase molecules. This primary effect seems to be very rare, but is efficiently enhanced by the generation of "secondary singlet oxygen" through the interaction between Hsub2/subOsub2/sub and peroxynitrite at the site of inactivated catalase. Transmission of bystander signaling between pretreated and untreated tumor cells depends on the generation of secondary singlet oxygen by the pretreated cells and singlet oxygen-mediated catalase inactivation of the untreated recipient cells. This induces autoamplificatory propagation of secondary singlet oxygen generation in the population. This experimental approach allowed to quantify the efficiencies of primary and secondary singlet oxgen generation after CAP and PAM action, to dissect the system and to study the underlying chemical biology in detail. Our data confirm that CAP and PAM-derived components are merely the trigger for the activation of autoamplificatory mechanisms of tumor cells, whereas the tumor cells efficiently propagate their cell death through their own ROS/RNS signaling potential.
机译:H 2 O 2 和亚硝酸盐(两种来自冷大气血浆的长寿命物种)对肿瘤细胞的治疗诱导了复杂的自扩增,单线态氧介导的过程,这导致过氧化氢酶的失活和细胞间凋亡诱导信号的重新激活。在这项研究中描述了对该过程的实验解剖和量化。当用H 2 O 2 和亚硝酸盐预处理肿瘤细胞,然后将其添加到未处理的肿瘤细胞中时,它们将单线态氧介导的过氧化氢酶失活和单线态氧的生成支持于未经处理的细胞群。该旁观者效应允许分析以下生化要求:a)诱导旁观者效应诱导潜力,b)旁观者效应传递至未处理的邻近细胞,以及c)这些信号事件的生化后果。诱导旁观者效应的潜能需要通过亚硝酸盐与H 2 O 2 之间相互作用后的反应生成“主要单线态氧”,然后局部失活一些过氧化氢酶分子。这种主要作用似乎很少见,但通过H 2 O 2 与过氧亚硝酸盐在位点处的相互作用产生“次级单线态氧”而得到有效增强。灭活的过氧化氢酶。旁观者信号在预处理的和未处理的肿瘤细胞之间的传递取决于预处理的细胞产生次生单线态氧和未经处理的受体细胞的单线态氧介导的过氧化氢酶失活。这会引起种群中次级单线态氧生成的自动扩增传播。这种实验方法可以量化CAP和PAM作用后一级和二级单线态氧的产生效率,剖析系统并详细研究基础化学生物学。我们的数据证实,CAP和PAM衍生的成分仅仅是激活肿瘤细胞自动扩增机制的触发因素,而肿瘤细胞则通过其自身的ROS / RNS信号传导潜能有效传播其细胞死亡。

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