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Two high-yield complementary methods to sort cell populations by their 2D or 3D migration speed

机译:通过其2D或3D迁移速度对小区群进行分类小区群的两种高产互补方法

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摘要

The potential to migrate is one of the most fundamental functions for various epithelial, mesenchymal, and immune cells. Image analysis of motile cell populations, both primary and cultured, typically reveals an intercellular variability in migration speeds. However, cell migration chromatography, the sorting of large populations of cells based on their migratory characteristics, cannot be easily performed. The lack of such methods has hindered our understanding of the direct correlation between the capacity to migrate and other cellular properties. Here, we report two novel, easily implementable and readily scalable methods to sort millions of live migratory cancer and immune cells based on their spontaneous migration in two-dimensional and three-dimensional microenvironments, respectively. Correlative downstream transcriptomic, molecular and functional tests reveal marked differences between the fast and slow subpopulations in patient-derived cancer cells. We further employ our method to reveal that sorting the most migratory cytotoxic T lymphocytes yields a pool of cells with enhanced cytotoxicity against cancer cells. This phenotypic assay opens new avenues for the precise characterization of the mechanisms underlying hither to unexplained heterogeneities in migratory phenotypes within a cell population, and for the targeted enrichment of the most potent migratory leukocytes in immunotherapies.
机译:迁移的可能性是各种上皮,间充质和免疫细胞的最基本的功能之一。初级和培养的运动细胞群图像分析通常揭示了迁移速度的细胞间变异性。然而,细胞迁移色谱法,基于其迁移特性的大量细胞的分类不能容易地进行。缺乏这些方法阻碍了我们对迁移能力与其他细胞性能之间的直接相关性的理解。在这里,我们报告了两种新颖,易于可实现的和易于可扩展的方法,分别分别基于其在二维和三维微环境中的自发迁移来分析数百万实时迁徙癌症和免疫细胞。相关下游转录组,分子和功能试验显示患者衍生的癌细胞中快速和缓慢群之间的显着差异。我们进一步采用我们的方法来揭示对大多数迁徙细胞毒性T淋巴细胞进行分类,产生具有增强的细胞毒性对癌细胞的细胞库。该表型测定开启了新的途径,以确切地表征在细胞群中的迁移表型中的迁移表型中的未解释的异质性的精确表征,以及用于靶向迁移白细胞的富含免疫检查中最有效的迁徙白细胞。

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