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RNAi-based functional selection identifies novel cell migration determinants dependent on PI3K and AKT pathways

机译:基于RNAi的功能选择可确定依赖PI3K和AKT途径的新型细胞迁移决定因素

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摘要

Lentiviral short hairpin RNA (shRNA)-mediated genetic screening is a powerful tool for identifying loss-of-function phenotype in mammalian cells. Here, we report the identification of 91 cell migration-regulating genes using unbiased genome-wide functional genetic selection. Individual knockdown or cDNA overexpression of a set of 10 candidates reveals that most of these cell migration determinants are strongly dependent on the PI3K/PTEN/AKT pathway and on their downstream signals, such as FOXO1 and p70S6K1. ALK, one of the cell migration promoting genes, uniquely uses p55 gamma regulatory subunit of PI3K, rather than more common p85 subunit, to trigger the activation of the PI3K-AKT pathway. Our method enables the rapid and cost-effective genome-wide selection of cell migration regulators. Our results emphasize the importance of the PI3K/PTEN/AKT pathway as a point of convergence for multiple regulators of cell migration.
机译:慢病毒短发夹RNA(shRNA)介导的基因筛选是一种功能强大的工具,可用于识别哺乳动物细胞中功能丧失的表型。在这里,我们报告使用无偏见的全基因组功能遗传选择鉴定91个细胞迁移调控基因。一组10个候选基因的单独敲低或cDNA过表达揭示了大多数这些细胞迁移决定簇强烈依赖于PI3K / PTEN / AKT途径及其下游信号,例如FOXO1和p70S6K1。 ALK是一种促进细胞迁移的基因,它独特地利用PI3K的p55γ调节亚基而不是更常见的p85亚基来触发PI3K-AKT途径的激活。我们的方法可以快速,经济高效地在全基因组范围内选择细胞迁移调节剂。我们的结果强调了PI3K / PTEN / AKT途径作为细胞迁移的多个调节因子的汇合点的重要性。

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