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首页> 外文期刊>Cytometry, Part A: the journal of the International Society for Analytical Cytology >Characteristics of live parameters of the HS-5 human bone marrow stromal cell line cocultured with the leukemia cells in hypoxia, for the studies of leukemia-stroma cross-talk
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Characteristics of live parameters of the HS-5 human bone marrow stromal cell line cocultured with the leukemia cells in hypoxia, for the studies of leukemia-stroma cross-talk

机译:HS-5人骨髓基质细胞系与缺氧中白血病细胞的活性参数的特征,对白血病 - 基质串扰的研究

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摘要

The unique bone marrow microenvironment is created by stromal cells and such physical conditions as hypoxia. Both hypoxia and interactions with stromal cells have a significant impact on the biology of leukemia cells, changing their sensitivity to antileukemic therapies. Thus, it is crucial to introduce biological systems, which enable the investigation of leukemia-stroma cross-talk and verification of novel therapies effectiveness under such bone marrow niche-mimicking conditions. Here, we have established an experimental setup based on the hypoxic co-culture of stromal cells with different cell lines derived from various leukemia patients. Flow cytometry enables simultaneous fluorescent tracking of viable cells and analysis of fundamental cellular processes, also to monitor the basal vital state of cells in the hypoxic co-culture. This is critically important, as the stromal cells deliver a big variability of signals to protect leukemia cells and provide drug resistance. Therefore, keeping stromal cells at the healthy state is crucial during experimental procedures. In the proposed studies, viability, apoptosis, proliferation, ROS production, and mitochondrial membrane potential were monitored in both cell types, which were separated on the basis of the fluorescence of a cell tracker. We have shown that the proposed hypoxic co-culture conditions do not affect basal live parameters of stromal cells, indicating the relevance of proposed model. Finally, we utilized this experimental setup to monitor the stroma-mediated protection of leukemia cells from the imatinib-induced cell death, which contributes to the leukemia progression and development of therapy resistance. Altogether, we recommend such flow cytometric strategy as an elementary screen of the vital state of stromal cells, which should be performed when using the co-culture hypoxic models. The proposed approach can also be broadly used for other studies of the leukemia-stroma cross-talk and of the part playe
机译:独特的骨髓微环境是由基质细胞和缺氧的这种物理条件产生的。缺氧和与基质细胞的相互作用都对白血病细胞的生物学产生了重大影响,改变了它们对抗血症疗法的敏感性。因此,引入生物体系至关重要,这使得在这种骨髓利基模拟条件下进行白血病 - 基质串扰和验证新型疗法的效果。在这里,我们已经根据具有源自各种白血病患者的不同细胞系的基质细胞的缺氧共培养,建立了一种实验性设置。流式细胞术能够同时荧光跟踪可活细胞和基本细胞过程的分析,也可以监测缺氧共培养中的基底生命状态。这令人统计学意义重要,因为基质细胞为保护白血病细胞提供了大的信号并提供耐药性。因此,在实验程序期间保持健康状态的基质细胞至关重要。在两个细胞类型中监测在拟议的研究,活力,凋亡,增殖,ROS产生和线粒体膜电位,其在细胞跟踪器的荧光的基础上分离。我们已经表明,拟议的缺氧共培养条件不会影响基质细胞的基础活参数,表明所提出的模型的相关性。最后,我们利用这种实验设置来监测来自伊马替尼诱导的细胞死亡的基质介导的白血病细胞保护,这有助于白血病进展和治疗抵抗的发展。总共建议将这种流式细胞术策略作为基质细胞的重要状态的基本筛网,这应该在使用共培养缺氧模型时进行。所提出的方法也可以广泛地用于白血病 - 基质的其他研究串扰和部分播放

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