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Identification of distinct miRNA target regulation between breast cancer molecular subtypes using AGO2-PAR-CLIP and patient datasets

机译:使用AGO2-PAR-CLIP和患者数据集识别乳腺癌分子亚型之间不同的miRNA靶标调控

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摘要

Background: Various microRNAs (miRNAs) are up-or downregulated in tumors. However, the repression of cognate miRNA targets responsible for the phenotypic effects of this dysregulation in patients remains largely unexplored. To define miRNA targets and associated pathways, together with their relationship to outcome in breast cancer, we integrated patient-paired miRNA-mRNA expression data with a set of validated miRNA targets and pathway inference.
机译:背景:各种microRNA(miRNA)在肿瘤中上调或下调。然而,抑制miRNA靶标负责这种失调的表型效应在患者中仍未开发。为了定义miRNA靶标和相关途径,以及它们与乳腺癌预后的关系,我们将患者配对的miRNA-mRNA表达数据与一组经过验证的miRNA靶标和途径推论相结合。

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