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Distinct IL-1α-responsive enhancers promote acute and coordinated changes in chromatin topology in a hierarchical manner.

The EMBO journal (2019-11-09)
Sinah-Sophia Weiterer, Johanna Meier-Soelch, Theodore Georgomanolis, Athanasia Mizi, Anna Beyerlein, Hendrik Weiser, Lilija Brant, Christin Mayr-Buro, Liane Jurida, Knut Beuerlein, Helmut Müller, Axel Weber, Ulas Tenekeci, Oliver Dittrich-Breiholz, Marek Bartkuhn, Andrea Nist, Thorsten Stiewe, Wilfred Fj van IJcken, Tabea Riedlinger, M Lienhard Schmitz, Argyris Papantonis, Michael Kracht
RÉSUMÉ

How cytokine-driven changes in chromatin topology are converted into gene regulatory circuits during inflammation still remains unclear. Here, we show that interleukin (IL)-1α induces acute and widespread changes in chromatin accessibility via the TAK1 kinase and NF-κB at regions that are highly enriched for inflammatory disease-relevant SNPs. Two enhancers in the extended chemokine locus on human chromosome 4 regulate the IL-1α-inducible IL8 and CXCL1-3 genes. Both enhancers engage in dynamic spatial interactions with gene promoters in an IL-1α/TAK1-inducible manner. Microdeletions of p65-binding sites in either of the two enhancers impair NF-κB recruitment, suppress activation and biallelic transcription of the IL8/CXCL2 genes, and reshuffle higher-order chromatin interactions as judged by i4C interactome profiles. Notably, these findings support a dominant role of the IL8 "master" enhancer in the regulation of sustained IL-1α signaling, as well as for IL-8 and IL-6 secretion. CRISPR-guided transactivation of the IL8 locus or cross-TAD regulation by TNFα-responsive enhancers in a different model locus supports the existence of complex enhancer hierarchies in response to cytokine stimulation that prime and orchestrate proinflammatory chromatin responses downstream of NF-κB.

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