BET bromodomain inhibition reduces maturation and enhances tolerogenic properties of human and mouse dendritic cells

Schilderink, Ronald; Bell, Matthew; Reginato, Eleonora; Patten, Chris; Rioja, Inmaculada; Hilbers, Francisca W.; Kabala, Pawel A.; Reedquist, Kris A.; Tough, David F.; Tak, Paul P.; Prinjha, Rab K.; Jonge, Wouter J. de

doi:10.1016/j.molimm.2016.09.010

Cited by 32 publications

(44 citation statements)

References 30 publications

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“…In recent years, BET inhibitors have attracted attention as a novel class of drug candidates not only for cancer but also for various inflammatory diseases [13, 14]. Several studies demonstrated that BET inhibitors were effective in the models of arthritis, vascular inflammation, acute pancreatitis, hepatic fibrosis and renal damage [23, 29–32], as well as in T cell-transfer colitis models [21, 22]. In the present study, we demonstrated that a novel quinazoline-based bromodomain inhibitor, CN210, inhibited CBP and p300 in addition to BET proteins and that CN210 potently attenuated indomethacin-induced CD-like ileitis in mice.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, it is known that BET proteins regulate gene transcriptions during the differentiation of naïve CD4 + cells to mature helper-T cells, and that BET inhibitors, such as JQ1, attenuated the differentiation of Th1, Th2, and Th17 cells [35, 36]. BET inhibitors have also reported to suppress inflammatory cytokine production and T-cell activation via inhibition of dendritic cell maturation and promotion of regulatory T-cell differentiation [22].…”

Section: Discussionmentioning

confidence: 99%

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Ameliorative effect of a quinazoline-based bromodomain inhibitor, CN210, on experimentally-induced Crohn’s disease-like murine ileitis via inhibition of inflammatory cytokine expression

Noguchi

Hidaka

Kobayashi

et al. 2020

Preprint

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SK) ¶ These authors contributed equally to this work 1 Abstract 2 3 Inhibitors of bromodomain and extra-terminal motif proteins ("BET inhibitors") are emerging 4 epigenetic therapeutics that exert their effects by suppressing the expression of genes that drive 5 cancer and inflammation. The present study examined the anti-inflammatory effects of a 6 quinazoline-based BET inhibitor, CN210, which also inhibits bromodomains of two paralogous 7 histone acetyltransferases (HATs), such as cAMP-responsive element binding protein-binding 8 protein (CBP) and p300. To assess its effectiveness against inflammatory bowel disease (IBD), 9 CN210 was tested in an experimentally-induced murine Crohn's disease (CD)-like ileitis model.10 Ileitis was induced in mice by subcutaneous administration of indomethacin and CN210 was 11 given orally 30 min before and 24 h after the indomethacin administration. Whilst indomethacin 12 produced severe ileitis accompanied by an increase in ileal mucosal myeloperoxidase (MPO) 13 activity, administration of CN210 reduced the severity of ileitis in a dose-dependent manner 14 and suppressed the MPO activity. Similarly, upregulation of inflammatory cytokines was 15 observed in ileitis mucosa after indomethacin injection but this response was significantly 16 attenuated by CN210 administration. To further characterize the effects of CN210 on 17 inflammatory pathways, monocyte/macrophage-like cell line RAW264 treated with 18 lipopolysaccharide (LPS) was exposed to CN210. CN210 significantly attenuated the 19 expression of inflammatory cytokines and reversed the activation of NF-κB and MAP kinases 20 induced by LPS. These findings suggest that CN210 ameliorates indomethacin-induced ileitis 21 due at least in part to the inhibition of inflammatory cytokine expression via attenuation of NF-22 κB and MAP kinase pathways, thus representing a new mode of therapy for CD. 23 Introduction 24 25 Bromodomain and extra-terminal motif (BET) proteins, including BRD2, BRD3, BRD4 26 and BRDT, are epigenetic 'reader' proteins that bind to acetylated lysine residues on proteins, 27 including histones, by means of their bromodomains [1, 2]. Of the four BET proteins, BRD4 28 associates with general transcription cofactor complex 'Mediator' and is a key structural 29 component of extensive transcription factor complexes formed at the genomic regions termed 30 Super-Enhancers (SEs) [2-4]. Small-molecule inhibitors of BRD4 was shown to suppress the 31 expression of MYC oncogene and the genes that encode pro-inflammatory cytokines, such as 32 IL-6, IFN-β, IL-1β, IL-12α, CXCL9 and CCL12 in mice [5-7], and showed efficacy in a wide 33 range of cancer models including pancreatic, breast, ovarian, and colon cancers [8-12]. 34 Accordingly, small molecule inhibitors of BET proteins ("BET inhibitors") are now considered 35 as promising drug candidates for both cancer and inflammatory diseases [13, 14]. 36 Whilst several BET inhibitors currently are evaluated clinically [15], early results showed 37 mixed results with undesirable s...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Ameliorative effect of a quinazoline-based bromodomain inhibitor, CN210, on experimentally-induced Crohn’s disease-like murine ileitis via inhibition of inflammatory cytokine expression

Noguchi

Hidaka

Kobayashi

et al. 2020

Preprint

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“…Treatment with I-BET151 reduces maturation marker and pro-inflammatory cytokine expression in dendritic cells and inhibits mature dendritic cell–mediated, antigen-dependent proliferation of naïve CD4 + T cells. 91 Dendritic cells treated with I-BET151 remain immature, and this led to increased generation of immunosuppressive Foxp3 + Tregs in vitro. Disappointingly, mice (Rag1 -/- mice transferred with CD45RB high sorted T cells) experiencing chronic colitis due to impaired Treg function displayed only modest improvement in disease symptoms when treated with I-BET151.…”

Section: Histone Readers As Therapeutic Targets For Ibdmentioning

confidence: 99%

“…Disappointingly, mice (Rag1 -/- mice transferred with CD45RB high sorted T cells) experiencing chronic colitis due to impaired Treg function displayed only modest improvement in disease symptoms when treated with I-BET151. 91 One explanation could be timing; I-BET151 administration in these mice occurred after colitis symptoms appeared and after priming of naïve T cells by dendritic cells had already occurred. Since earlier experiments negatively implicated I-BET151 in dendritic cell maturation and T cell activation, treatment with I-BET151 at an earlier stage could lead to higher Treg levels by immature dendritic cells, which might make a difference in ameliorating colitis.…”

Section: Histone Readers As Therapeutic Targets For Ibdmentioning

confidence: 99%

Epigenetics, DNA Organization, and Inflammatory Bowel Disease

Ray

Longworth

2018

Inflammatory Bowel Diseases

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Inflammatory bowel diseases (IBDs) are chronic inflammatory disorders affecting the gastrointestinal tract. The incidence of IBD is increasing, with more cases occurring in developed countries. Multiple factors such as genetics, environmental changes, gut microbiota, and immune abnormalities have been associated with development of IBD. In recent years, it has become increasingly apparent that epigenetic modifications of chromatin and the manner in which chromatin is organized in the nucleus are additionally important elements that can influence responses induced by the factors described above, and may therefore contribute to the onset and pathogenesis of IBD. Epigenetics and chromatin organization regulate diverse functions that include maintenance of homeostasis in the intestinal epithelium, the development and differentiation of immune cells, and modulation of responses generated by the immune system to defend against potential pathogens. Furthermore, changes in epigenetic chromatin marks and in chromatin organization have now been linked to differential gene expression in IBD patient cells. Although direct evidence for a role of histone modifications in IBD is currently very limited, in this review, we summarize the links between various epigenetic modifications, the proteins that catalyze or recognize these modifications, and the development or progression of IBD in human and experimental IBD. We also discuss how epigenetics influence the organization of DNA contacts to regulate gene expression and the implications this may have for diagnosing and treating IBD.

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“…Murine cDC1s (identified as CD11b − CD103 + XCR1 + ), equivalent to CD103 + Sirpα − DCs in humans, are dependent on transcription factors (TFs) Id2, Irf8, and Batf3 and induce anti-viral/bacterial IFNγ (Th1) CD4 + T cell responses (10). In contrast, CD11b + CD103 + intestinal cDC2s are related to CD103 + Sirpα + DCs in human intestines, depend on TFs Irf4 and Notch2 (10) and are important for induction of IL-17 (Th17) and IL-4/IL-5/IL-13 (Th2) CD4 + T cell responses (11). Whether epigenetic gene regulation is important in controlling immune responses of these subsets in the gut is unknown.…”

Section: Introductionmentioning

confidence: 99%

The Methyl-CpG-Binding Protein Mbd2 Regulates Susceptibility to Experimental Colitis via Control of CD11c+ Cells and Colonic Epithelium

et al. 2020

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Methyl-CpG-binding domain-2 (Mbd2) acts as an epigenetic regulator of gene expression, by linking DNA methylation to repressive chromatin structure. Although Mbd2 is widely expressed in gastrointestinal immune cells and is implicated in regulating intestinal cancer, anti-helminth responses and colonic inflammation, the Mbd2expressing cell types that control these responses are incompletely defined. Indeed, epigenetic control of gene expression in cells that regulate intestinal immunity is generally poorly understood, even though such mechanisms may explain the inability of standard genetic approaches to pinpoint the causes of conditions like inflammatory bowel disease. In this study we demonstrate a vital role for Mbd2 in regulating murine colonic inflammation. Mbd2 −/− mice displayed dramatically worse pathology than wild type controls during dextran sulfate sodium (DSS) induced colitis, with increased inflammatory (IL-1β +) monocytes. Profiling of mRNA from innate immune and epithelial cell (EC) populations suggested that Mbd2 suppresses inflammation and pathology via control of innate-epithelial cell crosstalk and T cell recruitment. Consequently, restriction of Mbd2 deficiency to CD11c + dendritic cells and macrophages, or to ECs, resulted in increased DSS colitis severity. Our identification of this dual role for Mbd2 in regulating the inflammatory capacity of both CD11c + cells and ECs highlights how epigenetic control mechanisms may limit intestinal inflammatory responses.

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BET bromodomain inhibition reduces maturation and enhances tolerogenic properties of human and mouse dendritic cells

Cited by 32 publications

References 30 publications

Ameliorative effect of a quinazoline-based bromodomain inhibitor, CN210, on experimentally-induced Crohn’s disease-like murine ileitis via inhibition of inflammatory cytokine expression

Ameliorative effect of a quinazoline-based bromodomain inhibitor, CN210, on experimentally-induced Crohn’s disease-like murine ileitis via inhibition of inflammatory cytokine expression

Epigenetics, DNA Organization, and Inflammatory Bowel Disease

The Methyl-CpG-Binding Protein Mbd2 Regulates Susceptibility to Experimental Colitis via Control of CD11c+ Cells and Colonic Epithelium

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