| Literature DB >> 28658630 |
Philipp Mertins1, Dariusz Przybylski1, Nir Yosef2, Jana Qiao1, Karl Clauser1, Raktima Raychowdhury1, Thomas M Eisenhaure1, Tanja Maritzen3, Volker Haucke3, Takashi Satoh4, Shizuo Akira4, Steven A Carr1, Aviv Regev5, Nir Hacohen6, Nicolas Chevrier7.
Abstract
Building an integrated view of cellular responses to environmental cues remains a fundamental challenge due to the complexity of intracellular networks in mammalian cells. Here, we introduce an integrative biochemical and genetic framework to dissect signal transduction events using multiple data types and, in particular, to unify signaling and transcriptional networks. Using the Toll-like receptor (TLR) system as a model cellular response, we generate multifaceted datasets on physical, enzymatic, and functional interactions and integrate these data to reveal biochemical paths that connect TLR4 signaling to transcription. We define the roles of proximal TLR4 kinases, identify and functionally test two dozen candidate regulators, and demonstrate a role for Ap1ar (encoding the Gadkin protein) and its binding partner, Picalm, potentially linking vesicle transport with pro-inflammatory responses. Our study thus demonstrates how deciphering dynamic cellular responses by integrating datasets on various regulatory layers defines key components and higher-order logic underlying signaling-to-transcription pathways.Entities:
Keywords: TLRs; Toll-like receptors; large-scale in vitro kinase assay; pathogen-sensing pathways; phosphoproteomics; protein-protein interactions; signaling; transcriptional network analysis
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Year: 2017 PMID: 28658630 PMCID: PMC5551420 DOI: 10.1016/j.celrep.2017.06.016
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423