Cooperation of multiple signaling pathways in CD40-regulated gene expression in B lymphocytes

Dadgostar, Hajir; Zarnegar, Brian; Hoffmann, Alexander; Qin, F. Xiao-Feng; Truong, Uyen; Rao, Govinda; Baltimore, David; Cheng, Genhong

doi:10.1073/pnas.032665099

Cited by 110 publications

(104 citation statements)

References 57 publications

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“…Pharmacological inhibition of any of these pathways dramatically reduces the proliferation response induced by CD40 stimulation [37]. However, our data suggest that activation of these MAP kinase signaling pathways is not significantly affected in CARMA1 KO B cells and not likely a reason for the defective proliferation.…”

Section: Discussionmentioning

confidence: 52%

“…Proliferation of B cells upon CD40 stimulation requires NF-jB activation and NF-jBdependent induction genes such as cyclin-D2 [37,38]. However, our data indicated that activation of NF-jB is not defective in CD40-stimulated CARMA1 KO B cells (Fig.…”

Section: Discussionmentioning

confidence: 59%

“…CARMA1 KO B cells not only fail to activate NF-jB following BCR ligation but also fail to undergo activation and proliferation [20,23,24]. Moreover, biological response following CD40 stimulation in B cells requires both canonical (NF-jB1) B1) and non-canonical (NF-jB2) pathways [37,38]. Therefore, we asked whether activation of NF-jB is compromised in CARMA1 KO B cells upon CD40 stimulation.…”

Section: Nf-jb Activation Upon Cd40 Stimulation In Wt and Carma1 Ko Bmentioning

confidence: 99%

“…Inhibition of any of these pathways has been shown to dramatically reduce CD40-induced proliferation [37]. Moreover, p42/p44 (ERK1/2) phosphorylation upon CD40 stimulation stabilizes c-Myc protein and favors cell-cycle progression [43].…”

Section: Analysis Of Map Kinase Signaling Cascades Following Cd40 Stimentioning

confidence: 99%

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Potential role of CARMA1 in CD40‐induced splenic B cell proliferation and marginal zone B cell maturation

Pappu¹,

Lin²

2006

Eur J Immunol

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NF‐κB activation through B cell receptor (BCR) ligation is critical for B cell development, survival and antigen‐mediated activation of B cells. CARD domain and MAGUK‐domain containing protein‐1 (CARMA1), recently identified adaptor molecule, has been shown to play an essential role in BCR‐induced NF‐κB activation. CARMA1‐deficient B cells fail to proliferate upon BCR stimulation, leading to defective humoral responses. Surprisingly, CARMA1‐deficient B cells are also defective in CD40‐induced proliferation. The mechanisms responsible for CD40‐induced proliferation defect have not yet been characterized. In this study, we show that signaling cascades activated by CD40 stimulation are largely unaffected in CARMA1‐deficient B cells. Instead, we have found that the defective proliferation of CARMA1‐deficient B cells is due to two events. First, CARMA1‐deficient B cells show defective cell‐cycle progression. Secondly, the numbers of marginal zone (MZ) B cells, which are the main responders upon CD40 stimulation, are greatly diminished in CARMA1‐deficient mice. Since B cell maturation requires basal signaling through BCR and NF‐κB activation, we propose that impaired BCR signaling in CARMA1‐deficient mice leads to defective maturation of MZ B cell population, which in turn, contributes to impaired proliferation upon CD40 stimulation.

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Section: Discussionmentioning

confidence: 52%

Section: Discussionmentioning

confidence: 59%

Section: Nf-jb Activation Upon Cd40 Stimulation In Wt and Carma1 Ko Bmentioning

confidence: 99%

Section: Analysis Of Map Kinase Signaling Cascades Following Cd40 Stimentioning

confidence: 99%

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Potential role of CARMA1 in CD40‐induced splenic B cell proliferation and marginal zone B cell maturation

Pappu¹,

Lin²

2006

Eur J Immunol

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“…Whether Ltb expression is up-regulated in later time points beyond 4 h is unknown. CD40L was previously shown to induce strong and sustained up-regulation of Ltb in B cells following 24 h of stimulation (61). It is possible that costimulation with CD40L is required to up-regulate Ltb in B cells during T-dependent immune response.…”

Section: Gene Expression Change Patterns Distinguishing Anti-igmentioning

confidence: 99%

Analysis of the Major Patterns of B Cell Gene Expression Changes in Response to Short-Term Stimulation with 33 Single Ligands

Zhu

Hart

Chang

et al. 2004

The Journal of Immunology

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We examined the major patterns of changes in gene expression in mouse splenic B cells in response to stimulation with 33 single ligands for 0.5, 1, 2, and 4 h. We found that ligands known to directly induce or costimulate proliferation, namely, anti-IgM (anti-Ig), anti-CD40 (CD40L), LPS, and, to a lesser extent, IL-4 and CpG-oligodeoxynucleotide (CpG), induced significant expression changes in a large number of genes. The remaining 28 single ligands produced changes in relatively few genes, even though they elicited measurable elevations in intracellular Ca2+ and cAMP concentration and/or protein phosphorylation, including cytokines, chemokines, and other ligands that interact with G protein-coupled receptors. A detailed comparison of gene expression responses to anti-Ig, CD40L, LPS, IL-4, and CpG indicates that while many genes had similar temporal patterns of change in expression in response to these ligands, subsets of genes showed unique expression patterns in response to IL-4, anti-Ig, and CD40L.

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Prolonged Ex vivo expansion and differentiation of naïve murine CD43⁻ B splenocytes

Zambrano

Jérôme

Freitag

et al. 2016

Biotechnology Progress

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Ex vivo expansion of naive primary B cells is still a challenge, yet would open new possibilities for in vitro studies of the immune response or the production of monoclonal antibodies. In our hands, unstimulated murine B cells did not expand in significant numbers, while culture viability decreased rapidly within a few days. Activation mimicking in vivo stimulation through either T cell-independent or T-cell dependent signaling, led to several division cycles, albeit accompanied by irreversible differentiation. By co-culturing B cells under moderate hypothermia (30°C) on live feeder fibroblasts expressing recombinant CD40 ligand (CD154) and by repeatedly transferring cultured B cells to new feeder cell cultures, we could extend the growth of primary mouse B cells compared to cultures maintained at 37°C. B cells under these conditions showed an activated phenotype as shown by the presence of AID and IRF4, two factors required for IgH class switch recombination in antigen-activated B cells. In contrast to cells cultured at 37°C, B cells under hyperthermia did surprisingly not differentiate into Blimp-1 expressing plasmablasts. Thus, the repeated batch process under hyperthermic conditions represents a first step towards the development of a continuous cultivation system for the expansion of primary B cells. © 2016 American Institute of Chemical Engineers Biotechnol. Prog., 32:978-989, 2016.

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Cooperation of multiple signaling pathways in CD40-regulated gene expression in B lymphocytes

Cited by 110 publications

References 57 publications

Potential role of CARMA1 in CD40‐induced splenic B cell proliferation and marginal zone B cell maturation

Potential role of CARMA1 in CD40‐induced splenic B cell proliferation and marginal zone B cell maturation

Analysis of the Major Patterns of B Cell Gene Expression Changes in Response to Short-Term Stimulation with 33 Single Ligands

Prolonged Ex vivo expansion and differentiation of naïve murine CD43⁻ B splenocytes

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Cooperation of multiple signaling pathways in CD40-regulated gene expression in B lymphocytes

Cited by 110 publications

References 57 publications

Potential role of CARMA1 in CD40‐induced splenic B cell proliferation and marginal zone B cell maturation

Potential role of CARMA1 in CD40‐induced splenic B cell proliferation and marginal zone B cell maturation

Analysis of the Major Patterns of B Cell Gene Expression Changes in Response to Short-Term Stimulation with 33 Single Ligands

Prolonged Ex vivo expansion and differentiation of naïve murine CD43− B splenocytes

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Prolonged Ex vivo expansion and differentiation of naïve murine CD43⁻ B splenocytes