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Integration of Multiple Platforms for the Analysis of Multifluorescent Marking Technology Applied to Pediatric GBM and DIPG

机译:多荧光标记技术分析应用于儿科GBM和DIPG的多函数平台集成

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摘要

The intratumor heterogeneity represents one of the most difficult challenges for the development of effective therapies to treat pediatric glioblastoma (pGBM) and diffuse intrinsic pontine glioma (DIPG). These brain tumors are composed of heterogeneous cell subpopulations that coexist and cooperate to build a functional network responsible for their aggressive phenotype. Understanding the cellular and molecular mechanisms sustaining such network will be crucial for the identification of new therapeutic strategies. To study more in-depth these mechanisms, we sought to apply the Multifluorescent Marking Technology. We generated multifluorescent pGBM and DIPG bulk cell lines randomly expressing six different fluorescent proteins and from which we derived stable optical barcoded single cell-derived clones. In this study, we focused on the application of the Multifluorescent Marking Technology in 2D and 3D in vitro/ex vivo culture systems. We discuss how we integrated different multimodal fluorescence analysis platforms, identifying their strengths and limitations, to establish the tools that will enable further studies on the intratumor heterogeneity and interclonal interactions in pGBM and DIPG.
机译:肠内异质性代表了治疗儿科胶质母细胞瘤(PGBM)和弥漫性本征性胶质瘤(DIPG)的有效疗法的最困难的挑战之一。这些脑肿瘤由非均相细胞群组成,共存和配合构建负责其侵略性表型的功能性网络。理解维持这种网络的细胞和分子机制对于鉴定新的治疗策略至关重要。为了研究更多的深入这些机制,我们试图应用多荧光标记技术。我们在随机表达六种不同荧光蛋白的多荧光PGBM和DIPG散装细胞系以及我们衍生的光学条形码单细胞衍生的克隆。在这项研究中,我们专注于多荧光标记技术在体外/离体培养系统中的应用中的应用。我们讨论了我们如何综合不同的多模式荧光分析平台,确定其优点和限制,以建立能够进一步研究PGBM和DIPG中的腹腔内异质性和间环中相互作用的工具。

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