Projects per year
Abstract
CD4+ T cells are key players in immune-mediated inflammatory diseases (IMIDs) through the production of inflammatory mediators including tumour necrosis factor (TNF). Anti-TNF therapy has revolutionized the treatment of several IMIDs and we previously demonstrated that in vitro treatment of human CD4+ T cells with anti-TNF promotes anti-inflammatory IL-10 expression in multiple subpopulations of CD4+ T cells. Here we investigated the transcriptional mechanisms underlying the IL-10 induction by TNF-blockade in CD4+ T cells, isolated from PBMCs of healthy volunteers, stimulated in vitro for 3 days with anti-CD3/CD28 mAb in the absence or presence of anti-TNF. After culture, CD45RA+ cells were depleted before performing gene expression profiling and chromatin accessibility analysis. Gene expression analysis of CD45RA-CD4+ T cells showed a distinct anti-TNF specific gene signature of 183 genes (q-value < 0.05). Pathway enrichment analysis of differentially expressed genes revealed multiple pathways related to cytokine signalling and regulation of cytokine production; in particular, IL10 was the most upregulated gene by anti-TNF, while the proinflammatory cytokines and chemokines IFNG, IL9, IL22, and CXCL10 were significantly downregulated (q-value < 0.05). Transcription factor motif analysis at the differentially open chromatin regions, after anti-TNF treatment, revealed 58 transcription factor motifs enriched at the IL10 locus. We identified seven transcription factor candidates for the anti-TNF mediated regulation of IL-10, which were either differentially expressed or whose locus was differentially accessible upon anti-TNF treatment. Correlation analysis between the expression of these transcription factors and IL10 suggests a role for MAF, PRDM1, and/or EOMES in regulating IL10 expression in CD4+ T cells upon anti-TNF treatment.
Original language | English |
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Article number | kyae013 |
Journal | Discovery Immunology |
Volume | 3 |
Issue number | 1 |
DOIs | |
Publication status | Published - 27 Jul 2024 |
Keywords
- IL-10, CD4+ T cell, anti-TNF, regulation, adalimumab
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- 2 Finished
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Determining the molecular mechanisms underlying IL-10 expression in human CD4+ T-cells following TNF blockade
Taams, L., Dionne, M. & Lavender, P.
1/04/2016 → 31/07/2023
Project: Research
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NIHR Biomedical Research Centre
Afzali, B., Antoniou, M., Barker, J., Barratt, B., Beighton, D., Bevan, S., Blower, P., Burchell, J., Cason, J., Chappell, L., Cope, A., Corrigan, C., Cunninghame Graham, D., Dontu, G., Edgeworth, J., Farzaneh, F., Gee, T., Gould, H., Green, P., Greenough, A., Grigoriadis, A., Hayday, A., Higginson, I., Kalra, L., Karagiannis, S., Kelly, F., Kemper, C., Lau-Walker, M., Lavender, P., Lee, T., Lempp, H., Lewis, C., Lombardi, G., Lord, G., Marber, M., Mason, J., Mathew, C., McGrath, J., Metcalfe, A., Molokhia, M., Mullen, G., Nagel, E., Neil, S., Nestle, F., Oakey, R., Parker, P., Peakman, M., Perera, D., Purushotham, A., Rasekh Ahmadi, K., Rashid, T., Razavi, R., Ridley, A., Robson, M., Sacks, S., Sanchez Fueyo, A., Santis, G., Sanz Moreno, V., Sawyer, E., Schaeffter, T., Shah, A., Sharpe, P., Simpson, M., Smith, R., Sorinola, I., Spector, T., Spicer, J., Taams, L., Tavassoli, M., Taylor, D., Tree, T., Trembath, R., Tribe, R., Tutt, A., Waltham, M., Watt, F., Webb, A., Wells, C., Whelan, K., Whitaker, J., Whittlesea, C., Williamson, C., Wolfe, C., Yu, V., academic, A., Hughes, S., Montana, G., Rhode, K., Schnabel, J. & Tziotzios, C.
NIHR National Institute For Health & Care Research, DHSC Department of Health and Social Care
1/04/2007 → 31/03/2017
Project: Research