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Predicting and affecting response to cancer therapy based on pathway-level biomarkers

机译:基于途径级生物标志物预测和影响对癌症治疗的反应

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Identifying robust, patient-specific, and predictive biomarkers presents a major obstacle in precision oncology. To optimize patient-specific therapeutic strategies, here we couple pathway knowledge with large-scale drug sensitivity, RNAi, and CRISPR-Cas9 screening data from 460 cell lines. Pathway activity levels are found to be strong predictive biomarkers for the essentiality of 15 proteins, including the essentiality of MAD2L1 in breast cancer patients with high BRCA-pathway activity. We also find strong predictive biomarkers for the sensitivity to 31 compounds, including BCL2 and microtubule inhibitors (MTIs). Lastly, we show that Bcl-xL inhibition can modulate the activity of a predictive biomarker pathway and re-sensitize lung cancer cells and tumors to MTI therapy. Overall, our results support the use of pathways in helping to achieve the goal of precision medicine by uncovering dozens of predictive biomarkers.
机译:识别稳健,患者特异性和预测生物标志物在精密肿瘤学中提出了一个主要障碍。为了优化特定的患者的治疗策略,在这里,我们对来自460个细胞系的大规模药物敏感性,RNAi和CRISPR-CAS9筛选数据致致衔接知识。发现途径活性水平是15个蛋白质的基本性的强预测生物标志物,包括乳腺癌患者的MAD2L1的基本性,具有高BRCA途径活性。我们还发现强烈的预测生物标志物,用于敏感性至31种化合物,包括BCl2和微管抑制剂(MTI)。最后,我们表明Bcl-XL抑制可以调节预测生物标志物途径的活性,并将肺癌细胞和肿瘤重新敏感到MTI治疗中。总体而言,我们的业绩支持通过揭示数十个预测生物标志物帮助实现精密药物的目标。

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