Inhibition of Super-Enhancer Activity in Autoinflammatory Site-Derived T Cells Reduces Disease-Associated Gene Expression

Publication date

2015-09-29

Authors

Peeters, J.
Vervoort, StephinISNI 0000000419538134
Tan, Sander C
Mijnheer, Gerdien
de Roock, SytzeISNI 0000000391194594
Vastert, BasISNI 000000039657238X
Nieuwenhuis, EESISNI 0000000393345368
van Wijk, FemkeORCID 0000-0001-8343-1356ISNI 0000000391770491
Prakken, BerentISNI 0000000389886890
Creyghton, M.P.

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Abstract

The underlying molecular mechanisms for many autoimmune diseases are poorly understood. Juvenile idiopathic arthritis (JIA) is an exceptionally well-suited model for studying autoimmune diseases due to its early onset and the possibility to analyze cells derived from the site of inflammation. Epigenetic profiling, utilizing primary JIA patient-derived cells, can contribute to the understanding of autoimmune diseases. With H3K27ac chromatin immunoprecipitation, we identified a disease-specific, inflammation-associated, typical enhancer and super-enhancer signature in JIA patient synovial-fluid-derived CD4(+) memory/effector T cells. RNA sequencing of autoinflammatory site-derived patient T cells revealed that BET inhibition, utilizing JQ1, inhibited immune-related super-enhancers and preferentially reduced disease-associated gene expression, including cytokine-related processes. Altogether, these results demonstrate the potential use of enhancer profiling to identify disease mediators and provide evidence for BET inhibition as a possible therapeutic approach for the treatment of autoimmune diseases.

Keywords

BET BROMODOMAIN INHIBITION, SELECTIVE-INHIBITION, C-MYC, TRANSCRIPTION, AUTOIMMUNITY, ARTHRITIS, VARIANTS, IDENTITY, TARGET, Journal Article, Research Support, Non-U.S. Gov't

Citation

Peeters, J G C, Vervoort, S J, Tan, S C, Mijnheer, G, de Roock, S, Vastert, S J, Nieuwenhuis, E E S, van Wijk, F, Prakken, B J, Creyghton, M P, Coffer, P J, Mokry, M & van Loosdregt, J 2015, 'Inhibition of Super-Enhancer Activity in Autoinflammatory Site-Derived T Cells Reduces Disease-Associated Gene Expression', Cell Reports [E], vol. 12, no. 12, pp. 1986-1996. https://doi.org/10.1016/j.celrep.2015.08.046