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High-content image informatics of the structural nuclear protein NuMA parses trajectories for stem/progenitor cell lineages and oncogenic transformation

机译:结构核蛋白NuMA的高内涵图像信息学解析了干/祖细胞谱系和致癌转化的轨迹

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摘要

Stem and progenitor cells that exhibit significant regenerative potential and critical roles in cancer initiation and progression remain difficult to characterize. Cell fates are determined by reciprocal signaling between the cell microenvironment and the nucleus; hence parameters derived from nuclear remodeling are ideal candidates for stem/progenitor cell characterization. Here we applied high-content, single cell analysis of nuclear shape and organization to examine stem and progenitor cells destined to distinct differentiation endpoints, yet undistinguishable by conventional methods. Nuclear descriptors defined through image informatics classified mesenchymal stem cells poised to either adipogenic or osteogenic differentiation, and oligodendrocyte precursors isolated from different regions of the brain and destined to distinct astrocyte subtypes. Nuclear descriptors also revealed early changes in stem cells after chemical oncogenesis, allowing the identification of a class of cancer-mitigating biomaterials. To capture the metrology of nuclear changes, we developed a simple and quantitative “imaging-derived” parsing index, which reflects the dynamic evolution of the high-dimensional space of nuclear organizational features. A comparative analysis of parsing outcomes via either nuclear shape or textural metrics of the nuclear structural protein NuMA indicates the nuclear shape alone is a weak phenotypic predictor. In contrast, variations in the NuMA organization parsed emergent cell phenotypes and discerned emergent stages of stem cell transformation, supporting a prognosticating role for this protein in the outcomes of nuclear functions.
机译:在癌症的发生和发展中表现出显着的再生潜力和关键作用的干细胞和祖细胞仍然难以表征。细胞命运是通过细胞微环境和细胞核之间的相互信号来确定的;因此,从核重塑得到的参数是干/祖细胞表征的理想候选者。在这里,我们对核的形状和组织进行了高含量的单细胞分析,以检查以不同分化终点为目标的干细胞和祖细胞,而这些干细胞和祖细胞无法通过常规方法进行区分。通过图像信息学定义的核描述符将间充质干细胞分为成脂性或成骨性分化,以及从脑部不同区域分离并注定为不同星形胶质细胞亚型的少突胶质细胞前体。核描述符还揭示了化学致癌后干细胞的早期变化,从而可以鉴定出一类减轻癌症的生物材料。为了捕获核变化的度量,我们开发了一种简单且定量的“成像派生”解析索引,该索引反映了核组织特征的高维空间的动态演变。通过核结构蛋白NuMA的核形状或组织结构度量解析结果的比较分析表明,仅核形状是一个弱的表型预测因子。相比之下,NuMA组织中的变异解析了新兴细胞表型和干细胞转化的新兴阶段,从而支持了该蛋白在核功能结局中的预后作用。

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