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A multivariate computational method to analyze high-content RNAi screening data

机译:分析高含量RNAi筛查数据的多元计算方法

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摘要

High-content screening (HCS) using RNA interference (RNAi) in combination with automated microscopy is a powerful investigative tool to explore complex biological processes. However, despite the plethora of data generated from these screens, little progress has been made in analyzing HC data using multivariate methods that exploit the full richness of multidimensional data. We developed a novel multivariate method for HCS, Multivariate Robust Analysis Method (M-RAM), integrating image feature selection with ranking of perturbations for hit identification, and applied this method to a HC RNAi screen to discover novel components of the DNA damage response in an osteosarcoma cell line. M-RAM automatically selects the most informative phenotypic readouts and time points to facilitate the more efficient design of follow-up experiments and enhance biological understanding. Our method outperforms univariate hit identification and identifies relevant genes that these approaches would have missed. We found that statistical cell-to-cell variation in phenotypic responses is an important predictor of ‘hits’ in RNAi-directed image-based screens. Genes that we identified as modulators of DNA damage signaling in U2OS cells include B-Raf, a cancer driver gene in multiple tumor types, whose role in DNA damage signaling we confirm experimentally, and multiple subunits of protein kinase A.
机译:使用RNA干扰(RNAi)与自动显微镜相结合的高内涵筛选(HCS)是探索复杂生物学过程的强大研究工具。但是,尽管从这些屏幕生成的数据过多,但是使用利用多维数据的全部丰富性的多元方法分析HC数据的进展甚微。我们开发了一种用于HCS的新颖的多元方法,即多元稳健分析方法(M-RAM),将图像特征选择与扰动等级相结合以进行命中识别,并将该方法应用于HC RNAi筛选以发现DNA损伤反应的新成分。骨肉瘤细胞系。 M-RAM自动选择最有用的表型读数和时间点,以促进更高效的后续实验设计并增强生物学理解。我们的方法优于单变量命中识别,并能识别出这些方法可能会遗漏的相关基因。我们发现,表型反应中统计性的细胞间差异是RNAi定向图像筛选中“命中”的重要预测因子。我们确定为U2OS细胞中DNA损伤信号传导调节剂的基因包括B-Raf,B-Raf是多种肿瘤类型的癌症驱动基因,我们通过实验确定了其在DNA损伤信号传导中的作用,以及蛋白激酶A的多个亚基。

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