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Publication : A validated regulatory network for Th17 cell specification.

First Author  Ciofani M Year  2012
Journal  Cell Volume  151
Issue  2 Pages  289-303
PubMed ID  23021777 Mgi Jnum  J:188993
Mgi Id  MGI:5444043 Doi  10.1016/j.cell.2012.09.016
Citation  Ciofani M, et al. (2012) A validated regulatory network for th17 cell specification. Cell 151(2):289-303
abstractText  Th17 cells have critical roles in mucosal defense and are major contributors to inflammatory disease. Their differentiation requires the nuclear hormone receptor RORgammat working with multiple other essential transcription factors (TFs). We have used an iterative systems approach, combining genome-wide TF occupancy, expression profiling of TF mutants, and expression time series to delineate the Th17 global transcriptional regulatory network. We find that cooperatively bound BATF and IRF4 contribute to initial chromatin accessibility and, with STAT3, initiate a transcriptional program that is then globally tuned by the lineage-specifying TF RORgammat, which plays a focal deterministic role at key loci. Integration of multiple data sets allowed inference of an accurate predictive model that we computationally and experimentally validated, identifying multiple new Th17 regulators, including Fosl2, a key determinant of cellular plasticity. This interconnected network can be used to investigate new therapeutic approaches to manipulate Th17 functions in the setting of inflammatory disease.
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