EZH2 Represses the B Cell Transcriptional Program and Regulates Antibody-Secreting Cell Metabolism and Antibody Production

Guo, Mengzhou; Price, Madeline J.; Patterson, Dillon G.; Barwick, Benjamin G.; Haines, Robert R.; Kania, Anna; Bradley, John E.; Randall, Troy D.; Boss, Jeremy M.; Scharer, Christopher D.

doi:10.4049/jimmunol.1701470

Cited by 110 publications

(137 citation statements)

References 84 publications

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“…Accordingly, we saw a marked reduction in the accumulation of B cells in the presence of WDR5 inhibitor OICR9429 (Figure 3b), while the effect on proliferation as indicated by Ki67 expression was marginal (Figure 4). The transcriptional repressor EZH2 is required for maximal antibody secretion [31] and is overexpressed in SLE leukocytes [32]. While we show reduced antibody secretion in presence of the EZH2 inhibitor UNC1999 (Figure 3b), we see very little effects on proliferation (Figure 4) in contrast to other studies [33,34].…”

Section: Discussioncontrasting

confidence: 59%

Identifying novel B-cell targets for chronic inflammatory autoimmune disease by screening of chemical probes in a patient-derived cell assay

Sundström

Shang

Panda

et al. 2020

Preprint

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B-cell secretion of autoantibodies drives autoimmune diseases, including systemic lupus erythematosus and idiopathic inflammatory myositis. Few therapies are presently available for treatment of these patients, often resulting in unsatisfactory effects and helping only some of patients. We developed a screening assay for evaluation of novel targets suspending B-cell maturation into antibody secreting cells, which could contribute to future drug development. The assay was employed for testing 43 high quality chemical probes and compounds inhibiting under-explored protein targets, using primary cells from patients with autoimmune disease. Probes inhibiting bromodomain family proteins and histone methyl transferases demonstrated abrogation of B-cell functions to a degree comparable to a positive control, the JAK inhibitor tofacitinib. Inhibition of each target rendered a specific functional cell and potential disease modifying effect, indicating specific epigenetic protein targets as potential new intervention points for future drug discovery and development efforts.

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Section: Discussioncontrasting

confidence: 59%

Identifying novel B-cell targets for chronic inflammatory autoimmune disease by screening of chemical probes in a patient-derived cell assay

Sundström

Shang

Panda

et al. 2020

Preprint

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“…In order to regulate gene expression, BLIMP1 recruits epigenetic coregulators. 17, 21–27 While an important role for EZH2 has been identified, 17, 25 the relative contribution of G9A and in particular G9A in human cells has not been extensively studied. 66 Small molecule inhibitors of epigenetic regulators provide tool compounds for exploring functional biology.…”

Section: Discussionmentioning

confidence: 99%

A dichotomy in association of core transcription factors and gene regulation during the activated B-cell to plasmablast transition

Cocco

Care

Al-Maskari

et al. 2019

Preprint

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The activated B-cell (ABC) to plasmablast transition is the cusp of antibody secreting cell (ASC) differentiation but is incompletely defined. We apply expression time-courses, parsimonious gene correlation network analysis, and ChIP-seq to explore this in human cells. The transition initiates with input signal loss leading within hours from cell growth dominant programs to enhanced proliferation, accompanied from 24h by ER-stress response, secretory optimization and upregulation of ASC features. Clustering of genomic occupancy for ASC transcription factors (TFs) IRF4, BLIMP1 and XBP1 with CTCF and histone marks defines distinct patterns for each factor in plasmablasts. Integrating TF-associated clusters and modular gene expression identifies a dichotomy: XBP1 and IRF4 significantly link to gene modules induced in plasmablasts, but not to modules of repressed genes, while BLIMP1 links to modules of ABC genes repressed in plasmablasts but is not significantly associated with modules induced in plasmablasts. Pharmacological inhibition of the G9A (EHMT2) histone-methytransferase, a BLIMP1 co-factor that catalyzes repressive H3K9me2 marks, leaves functional ASC differentiation intact but de-represses ABC-state genes. Thus, in human plasmablasts IRF4 and XBP1 emerge as the dominant association with ASC gene expression, while BLIMP1 links to repressed modules with particular focus in repression of the B-cell activation state.

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“…Specifically, we determined whether conditional deletion of DOT1L would result in a reduction of global H3K79me2 in B cell subsets ( Figure S2A). As a control, we also tested polycomb repressive complex 2 (PRC2)-mediated H3K27me3, which has also been shown to be an important regulator of B cell biology (Beguelin et al, 2013;Caganova et al, 2013;Guo et al, 2018;Su et al, 2003).…”

Section: Dot1l Regulates Expression Of Genes Required For Effective Bmentioning

confidence: 99%

The histone methyltransferase DOT1L is essential for humoral immune responses

Kealy

Pietro

Scheer

et al. 2019

Preprint

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Short running title: B cell responses require DOT1L. Abbreviations used: AID -activation-induced cytidine deaminase; ASCs -antibody-secreting cells; BCL6 -B cell lymphoma-6; CPM -counts per million; CTV -cell trace violet; DOT1Ldisruptor of telomeric silencing 1-like, EZH2 -enhancer of zeste homolog 2; FVS -fixable viability stain; H3K27me3 -trimethylation of lysine 27 on histone H3; Ig -immunoglobulin; KLH -Keyhole Limpet Hemocyanin; MLLr-ALL -Mixed Lineage Leukaemia-rearranged acute lymphoblastic leukaemia; NP -(4-Hydroxy-3-nitrophenyl)-acetyl; PRC2 -polycomb repressive complex 2; S1PR -sphingosine-1-phosphate receptor; Th cells -T helper cells. ABSTRACT Histone modifiers are essential molecular regulators that underpin the ability of immune cells to reprogram their gene expression during differentiation. The recruitment of the histone methyltransferase DOT1L induces oncogenic gene expression in a subset of B cell leukemia. Despite its importance, little is known about its role in the humoral immune system. Herein, we demonstrate that DOT1L is a critical regulator of B cell biology. Dot1l f/f Mb1 Cre/+ mice had a block in B cell development, culminating in a significant reduction of mature B cells in the periphery. Upon immunization or influenza infection, germinal centers failed to form in Dot1l f/f Cd23 Cre/+ mice. Consequently, immunized mice revealed that DOT1L was essential for the formation of B cell memory populations. Dot1l deletion significantly attenuated the formation of class-switched antibody-secreting cells in both T-dependent and T-independent responses. Transcriptome, pathway and histological analysis identified a key role for DOT1L in reprogramming gene expression for migration and localization during the initial stages of a humoral response. Together, these results demonstrate an essential role for DOT1L in antigen-dependent B cell differentiation and hence, in generating an effective and lasting humoral immune response.

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EZH2 Represses the B Cell Transcriptional Program and Regulates Antibody-Secreting Cell Metabolism and Antibody Production

Cited by 110 publications

References 84 publications

Identifying novel B-cell targets for chronic inflammatory autoimmune disease by screening of chemical probes in a patient-derived cell assay

Identifying novel B-cell targets for chronic inflammatory autoimmune disease by screening of chemical probes in a patient-derived cell assay

A dichotomy in association of core transcription factors and gene regulation during the activated B-cell to plasmablast transition

The histone methyltransferase DOT1L is essential for humoral immune responses

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