Christine M. Cote scite author profile

We examined the unique contributions of the cytokines IL-21 and IL-4 on germinal center (GC) B cell initiation and subsequent maturation in a murine model system. Similar to other reports, we found T follicular helper cell (Tfh) expression of IL-21 begins prior to Tfh migration into the B cell follicle and precedes that of IL-4. Consistent with this timing, IL-21 signaling has a greater influence on the peri-follicular pre-GC B cell transition to the intra-follicular stage. Notably, Bcl6hi B cells can form in the combined absence of IL21R and STAT6 derived signals, however these nascent GC B cells cease to proliferate and are more prone to apoptosis. When B cells lack either IL21R or STAT6, aberrant GCs form atypical centroblast and centrocytes that differ in their phenotypic maturation and co-stimulatory molecule expression. Thus IL-4 and IL-21 play non-redundant roles in the phased progression of GC B cell development that can initiate in the combined absence of these cytokine signals.

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The BCL6 RD2 Domain Governs Commitment of Activated B Cells to Form Germinal Centers

Huang

Gonzalez

Cote

et al. 2014

Cell Reports

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Summary To understand how the Bcl6 transcriptional repressor functions in the immune system we disrupted its RD2 repression domain in mice. Bcl6RD2MUT mice exhibit a complete loss of GC formation but retain normal extrafollicular responses. Bcl6RD2MUT antigen-engaged B-cells migrate to the interfollicular zone and interact with cognate T helper cells. However, these cells fail to complete early GC-commitment differentiation and coalesce as nascent GC aggregates. Bcl6 directly binds and represses trafficking receptors S1pr1 and Gpr183 by recruiting Hdac2 through the RD2 domain. Deregulation of these genes impairs B-cell migration and may contribute to GC failure in Bcl6RD2MUT mice. The development of functional GC-TFH cells was partially impaired in Bcl6RD2MUT mice. In contrast to Bcl6−/− mice, Bcl6RD2MUT animals experience no inflammatory disease or macrophage deregulation. These results reveal an essential role for RD2 repression in early GC commitment and striking biochemical specificity in Bcl6 control of humoral and innate immune-cell phenotypes.

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Germinal center B cell development has distinctly regulated stages completed by disengagement from T cell help

Zhang

Gonzalez

Cote

et al. 2017

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To reconcile conflicting reports on the role of CD40 signaling in germinal center (GC) formation, we examined the earliest stages of murine GC B cell differentiation. Peri-follicular GC precursors first expressed intermediate levels of BCL6 while co-expressing the transcription factors RelB and IRF4, the latter known to repress Bcl6 transcription. Transition of GC precursors to the BCL6hi follicular state was associated with cell division, although the number of required cell divisions was immunogen dose dependent. Potentiating T cell help or CD40 signaling in these GC precursors actively repressed GC B cell maturation and diverted their fate towards plasmablast differentiation, whereas depletion of CD4+ T cells promoted this initial transition. Thus while CD40 signaling in B cells is necessary to generate the immediate precursors of GC B cells, transition to the BCL6hi follicular state is promoted by a regional and transient diminution of T cell help.DOI: http://dx.doi.org/10.7554/eLife.19552.001

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Platelet P-selectin initiates cross-presentation and dendritic cell differentiation in blood monocytes

et al. 2020

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Dendritic cells (DCs) are adept at cross-presentation and initiation of antigen-specific immunity. Clinically, however, DCs produced by in vitro differentiation of monocytes in the presence of exogenous cytokines have been met with limited success. We hypothesized that DCs produced in a physiological manner may be more effective and found that platelets activate a cross-presentation program in peripheral blood monocytes with rapid (18 hours) maturation into physiological DCs (phDCs). Differentiation of monocytes into phDCs was concomitant with the formation of an “adhesion synapse,” a biophysical junction enriched with platelet P-selectin and monocyte P-selectin glycoprotein ligand 1, followed by intracellular calcium fluxing and nuclear localization of nuclear factor κB. phDCs were more efficient than cytokine-derived DCs in generating tumor-specific T cell immunity. Our findings demonstrate that platelets mediate a cytokine-independent, physiologic maturation of DC and suggest a novel strategy for DC-based immunotherapies.

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Author response: Germinal center B cell development has distinctly regulated stages completed by disengagement from T cell help

Zhang

Gonzalez

Cote

et al. 2016

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To reconcile conflicting reports on the role of CD40 signaling in germinal center (GC) formation, we examined the earliest stages of murine GC B cell differentiation. Peri-follicular GC precursors first expressed intermediate levels of BCL6 while co-expressing the transcription factors RelB and IRF4, the latter known to repress Bcl6 transcription. Transition of GC precursors to the BCL6 hi follicular state was associated with cell division, although the number of required cell divisions was immunogen dose dependent. Potentiating T cell help or CD40 signaling in these GC precursors actively repressed GC B cell maturation and diverted their fate towards plasmablast differentiation, whereas depletion of CD4+ T cells promoted this initial transition. Thus while CD40 signaling in B cells is necessary to generate the immediate precursors of GC B cells, transition to the BCL6 hi follicular state is promoted by a regional and transient diminution of T cell help.

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Christine M. Cote

Nonredundant Roles of IL-21 and IL-4 in the Phased Initiation of Germinal Center B Cells and Subsequent Self-Renewal Transitions

The BCL6 RD2 Domain Governs Commitment of Activated B Cells to Form Germinal Centers

Germinal center B cell development has distinctly regulated stages completed by disengagement from T cell help

Platelet P-selectin initiates cross-presentation and dendritic cell differentiation in blood monocytes

Author response: Germinal center B cell development has distinctly regulated stages completed by disengagement from T cell help

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