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Reverse engineering a hierarchical regulatory network downstream of oncogenic KRAS
Authors:Oleg Tchernitsa  Franziska Witzel  Bertram Klinger  Christine Sers  Hanspeter Herzel  Reinhold Schäfer
Affiliation:1. Laboratory of Molecular Tumour Pathology, Institute of Pathology, Charité Universit?tsmedizin Berlin, , Berlin, Germany;2. Laboratory of Functional Genomics, Charité Universit?tsmedizin Berlin, , Berlin, Germany;3. Institute for Theoretical Biology, Humboldt University, , Berlin, Germany
Abstract:RAS mutations are highly relevant for progression and therapy response of human tumours, but the genetic network that ultimately executes the oncogenic effects is poorly understood. Here, we used a reverse‐engineering approach in an ovarian cancer model to reconstruct KRAS oncogene‐dependent cytoplasmic and transcriptional networks from perturbation experiments based on gene silencing and pathway inhibitor treatments. We measured mRNA and protein levels in manipulated cells by microarray, RT–PCR and western blot analysis, respectively. The reconstructed model revealed complex interactions among the transcriptional and cytoplasmic components, some of which were confirmed by double pertubation experiments. Interestingly, the transcription factors decomposed into two hierarchically arranged groups. To validate the model predictions, we analysed growth parameters and transcriptional deregulation in the KRAS‐transformed epithelial cells. As predicted by the model, we found two functional groups among the selected transcription factors. The experiments thus confirmed the predicted hierarchical transcription factor regulation and showed that the hierarchy manifests itself in downstream gene expression patterns and phenotype.
Keywords:cancer systems biology  modular response analysis  oncogenes  ovarian carcinoma model  signal transduction
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