Fate mapping quantifies the dynamics of B cell development and activation throughout life

SummaryFollicular mature (FM) and germinal centre (GC) B cells underpin humoral immunity but the dynamics of their generation and maintenance are not clearly defined. Here we exploited a fate-mapping system in mice that tracks B cells as they develop into peripheral subsets, together with a cell division fate reporter mouse and mathematical models. We find that FM cells are kinetically homogeneous, recirculate freely, continually replenished from transitional populations, and self-renew rarely. In contrast, GC B cell lineages persist for weeks with rapid turnover and site-specific dynamics. Those in the spleen derive from transitional cells and are kinetically homogeneous, while those in lymph nodes derive from FM B cells and comprise both transient and persistent clones. These differences likely derive from the nature of antigen exposure at the different sites. Our integrative approach also reveals how the host environment drives cell-extrinsic, age-related changes in B cell homeostasis.

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Faculty Opinions recommendation of Role of MHC class II on memory B cells in post-germinal center B cell homeostasis and memory response.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.1031339.363676 ◽

2006 ◽

Author(s):

David Tarlinton

Keyword(s):

B Cells ◽

B Cell ◽

Mhc Class Ii ◽

Germinal Center ◽

Memory B Cells ◽

Cell Homeostasis ◽

Memory Response ◽

Germinal Center B Cell ◽

B Cell Homeostasis

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WASP confers selective advantage for specific hematopoietic cell populations and serves a unique role in marginal zone B-cell homeostasis and function

Blood ◽

10.1182/blood-2008-02-140715 ◽

2008 ◽

Vol 112 (10) ◽

pp. 4139-4147 ◽

Cited By ~ 71

Author(s):

Lisa S. Westerberg ◽

Miguel A. de la Fuente ◽

Fredrik Wermeling ◽

Hans D. Ochs ◽

Mikael C. I. Karlsson ◽

...

Keyword(s):

T Cells ◽

B Cells ◽

B Cell ◽

Marginal Zone ◽

Hematopoietic Cells ◽

Selective Advantage ◽

Relative Contribution ◽

B Cell Homeostasis ◽

And Function

Abstract Development of hematopoietic cells depends on a dynamic actin cytoskeleton. Here we demonstrate that expression of the cytoskeletal regulator WASP, mutated in the Wiskott-Aldrich syndrome, provides selective advantage for the development of naturally occurring regulatory T cells, natural killer T cells, CD4+ and CD8+ T lymphocytes, marginal zone (MZ) B cells, MZ macrophages, and platelets. To define the relative contribution of MZ B cells and MZ macrophages for MZ development, we generated wild-type and WASP-deficient bone marrow chimeric mice, with full restoration of the MZ. However, even in the presence of MZ macrophages, only 10% of MZ B cells were of WASP-deficient origin. We show that WASP-deficient MZ B cells hyperproliferate in vivo and fail to respond to sphingosine-1-phosphate, a crucial chemoattractant for MZ B-cell positioning. Abnormalities of the MZ compartment in WASP−/− mice lead to aberrant uptake of Staphylococcus aureus and to a reduced immune response to TNP-Ficoll. Moreover, WASP-deficient mice have increased levels of “natural” IgM antibodies. Our findings reveal that WASP regulates both development and function of hematopoietic cells. We demonstrate that WASP deficiency leads to an aberrant MZ that may affect responses to blood-borne pathogens and peripheral B-cell tolerance.

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Cellular side of acquired immunity (B cells)

Oxford Textbook of Rheumatology ◽

10.1093/med/9780199642489.003.0050_update_001 ◽

2013 ◽

pp. 371-378

Author(s):

Thomas Dörner ◽

Peter E. Lipsky

Keyword(s):

B Cells ◽

B Cell ◽

T Cell Activation ◽

Cell Activation ◽

Plasma Cells ◽

Adaptive Immune System ◽

Adaptive Immune ◽

B Cell Homeostasis ◽

Anti Cd20 ◽

Antigen Presenting

B cells have gained interest in rheumatoid arthritis (RA) beyond being the precursors of antibody-producing plasma cells since they are also a broader component of the adaptive immune system. They are capable of functioning as antigen-presenting cells for T-cell activation and can produce an array of cytokines. Disturbances of peripheral B-cell homeostasis together with the formation of ectopic lymphoid neogenesis within the inflamed synovium appears to be a characteristic of patients with RA. Enhanced generation of memory B cells and autoreactive plasma cells producing IgM-RF and ACPA-IgG antibodies together with formation of immune complexes contribute to the maintenance of RA, whereas treatment with B-cell-directed anti-CD20 and CLTA4-Ig therapy provides clinical benefit.

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Enhanced B Cell Activation in the Absence of CD81

Blood ◽

10.1182/blood.v112.11.2578.2578 ◽

2008 ◽

Vol 112 (11) ◽

pp. 2578-2578

Author(s):

Mrinmoy Sanyal ◽

Rosemary Fernandez ◽

Shoshana Levy

Keyword(s):

B Cells ◽

B Cell ◽

Cell Activation ◽

Cell Receptor ◽

Free Calcium ◽

B Cell Activation ◽

Membrane Reorganization ◽

A Cell

Abstract CD81 is a component of the CD19/CD21 coreceptor complex in B cells. This tetraspanin molecule was previously shown to enable membrane reorganization in B cells responding to complement-bound antigens. Here we stimulated B cells via their B cell receptor (BCR) and demonstrate that Cd81−/− B cells fluxed higher intracellular free calcium ion along with increased phosphorylation of PLCγ2 and Syk. The stimulated Cd81−/− B cells also proliferated faster and secreted higher amounts of antibodies. Moreover, activation of the TLR4 pathway in Cd81−/− B cells induced increased proliferation and antibody secretion. Furthermore, Cd81−/− mice mounted a significantly higher immune response to T-cell independent antigens than their wildtype counterparts. Finally, analysis of Cd81−/− B cells that were generated by bone marrow transplantation into Rag1−/− mice confirmed a cell intrinsic hyperactive phenotype. Taken together, these results indicate that CD81 plays a negative role in B cell activation in vitro and in vivo.

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Differential expression of CD21 identifies developmentally and functionally distinct subsets of human transitional B cells

Blood ◽

10.1182/blood-2009-07-234799 ◽

2010 ◽

Vol 115 (3) ◽

pp. 519-529 ◽

Cited By ~ 77

Author(s):

Santi Suryani ◽

David A. Fulcher ◽

Brigitte Santner-Nanan ◽

Ralph Nanan ◽

Melanie Wong ◽

...

Keyword(s):

B Cells ◽

B Cell ◽

Differential Expression ◽

Cell Development ◽

B Cell Development ◽

Cell Repertoire ◽

Molecular Features ◽

Transitional B Cells ◽

Transitional Cells

Abstract The transitional stage of B-cell development represents an important step where autoreactive cells are deleted, allowing the generation of a mature functional B-cell repertoire. In mice, 3 subsets of transitional B cells have been identified. In contrast, most studies of human transitional B cells have focused on a single subset defined as CD24hiCD38hi B cells. Here, we have identified 2 subsets of human transitional B cells based on the differential expression of CD21. CD21hi transitional cells displayed higher expression of CD23, CD44, and IgD, and exhibited greater proliferation and Ig secretion in vitro than CD21lo transitional B cells. In contrast, the CD21lo subset expressed elevated levels of LEF1, a transcription factor highly expressed by immature lymphocytes, and produced higher amounts of autoreactive Ab. These phenotypic, functional, and molecular features suggest that CD21lo transitional B cells are less mature than the CD21hi subset. This was confirmed by analyzing X-linked agammaglobulinemia patients and the kinetics of B-cell reconstitution after stem cell transplantation, which revealed that the development of CD21lo transitional B cells preceded that of CD21hi transitional cells. These findings provide important insights into the process of human B-cell development and have implications for understanding the processes underlying perturbed B-cell maturation in autoimmune and immunodeficient conditions.

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Global transcriptional coactivators CREB-binding protein and p300 are highly essential collectively but not individually in peripheral B cells

Blood ◽

10.1182/blood-2005-08-3263 ◽

2006 ◽

Vol 107 (11) ◽

pp. 4407-4416 ◽

Cited By ~ 44

Author(s):

Wu Xu ◽

Tomofusa Fukuyama ◽

Paul A. Ney ◽

Demin Wang ◽

Jerold Rehg ◽

...

Keyword(s):

B Cells ◽

B Cell ◽

Binding Protein ◽

Cell Receptor ◽

Conditional Knockout ◽

Creb Binding Protein ◽

Cell Stage ◽

Transcriptional Coactivators ◽

B Cell Homeostasis ◽

Peripheral B Cells

Abstract CREB-binding protein (CBP) and its para-log p300 are transcriptional coactivators that physically or functionally interact with over 320 mammalian and viral proteins, including 36 that are essential for B cells in mice. CBP and p300 are generally considered limiting for transcription, yet their roles in adult cell lineages are largely unknown since homozygous null mutations in either gene or compound heterozygosity cause early embryonic lethality in mice. We tested the hypotheses that CBP and p300 are limiting and that each has unique properties in B cells, by using mice with Cre/LoxP conditional knockout alleles for CBP (CBPflox) and p300 (p300flox), which carry CD19Cre that initiates floxed gene recombination at the pro–B-cell stage. CD19Cre-mediated loss of CBP or p300 led to surprisingly modest deficits in B-cell numbers, whereas inactivation of both genes was not tolerated by peripheral B cells. There was a moderate decrease in B-cell receptor (BCR)–responsive gene expression in CBP or p300 homozygous null B cells, suggesting that CBP and p300 are essential for this signaling pathway that is crucial for B-cell homeostasis. These results indicate that individually CBP and p300 are partially limiting beyond the pro-B-cell stage and that other coactivators in B cells cannot replace their combined loss.

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Absence of surface IgD does not impair naive B cell homeostasis and memory B cell formation in humans

10.1101/332361 ◽

2018 ◽

Author(s):

J. Nechvatalova ◽

S.J.W. Bartol ◽

Z. Chovancova ◽

L. Boon ◽

M. Vlkova ◽

...

Keyword(s):

B Cells ◽

B Cell ◽

Cell Activation ◽

Genetic Defect ◽

Memory B Cells ◽

Cell Homeostasis ◽

Human B Cells ◽

B Cell Homeostasis

One Sentence SummaryHuman B cells with a genetic defect in IGHD develop normally in vivo, and do not have a competitive disadvantage to IgD-expressing B cells for developing into memory B cells.AbstractSurface immunoglobulin D (IgD) is co-expressed with IgM on naive mature B cells. Still, the role of surface IgD remains enigmatic even 50 years after its initial discovery. We here examined the in vivo role of surface IgD in human B-cell homeostasis and antibody responses in four individuals with heterozygous nonsense mutations in IGHD. All IGHD heterozygous individuals had normal numbers of B cells and serum immunoglobulins, and did not show signs of immunodeficiency or immune dysregulation. IgD+ and IgD– naive mature B cells were present in equal numbers and showed similar immunophenotypes, except for decreased expression of CD79b in the IgD– subset. Furthermore, both IgD+ and IgD– naive mature B cells had normal replication histories, similar capacities to differentiate into plasma cells upon in vitro stimulation, and Ig switched memory B cells showed similar levels of somatic hypermutations. Thus human B cells lacking IgD expression develop normally and generate immunological memory in vivo, suggesting that surface IgD might function more restricted in regulating of B-cell activation to specific antigenic structures.

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The Antidepressant Mirtazapine Rapidly Shifts Hepatic B Cell Populations and Functional Cytokine Signatures in the Mouse

Frontiers in Immunology ◽

10.3389/fimmu.2021.622537 ◽

2021 ◽

Vol 12 ◽

Author(s):

Wagdi Almishri ◽

Rachelle P. Davis ◽

Abdel-Aziz Shaheen ◽

Mohammed O. Altonsy ◽

Craig N. Jenne ◽

...

Keyword(s):

B Cells ◽

B Cell ◽

Liver Diseases ◽

Normal Liver ◽

Cell Number ◽

Cell Populations ◽

Immune Mediated ◽

B Cell Homeostasis ◽

The Impact

IntroductionB cells are important regulators of both adaptive and innate immunity. The normal liver contains significant numbers of B cells, and their numbers increase dramatically in immune-mediated liver diseases. Our previous observations suggest a hepatoprotective effect of the antidepressant mirtazapine in human and experimental immune-mediated liver disease. Therefore, we performed a series of experiments to determine the impact of mirtazapine treatment on hepatic B cell homeostasis, as reflected by B cell number, trafficking and phenotype using flow cytometry (FCM) and intravital microscopy (IVM) analysis. Mirtazapine treatment rapidly induced a significant reduction in total hepatic B cell numbers, paralleled by a compositional shift in the predominant hepatic B cell subtype from B2 to B1. This shift in hepatic B cells induced by mirtazapine treatment was associated with a striking increase in total hepatic levels of the chemokine CXCL10, and increased production of CXCL10 by hepatic macrophages and dendritic cells. Furthermore, mirtazapine treatment led to an upregulation of CXCR3, the cognate chemokine receptor for CXCL10, on hepatic B cells that remained in the liver post-mirtazapine. A significant role for CXCR3 in the hepatic retention of B cells post-mirtazapine was confirmed using CXCR3 receptor blockade. In addition, B cells remaining in the liver post-mirtazapine produced lower amounts of the proinflammatory Th1-like cytokines IFNγ, TNFα, and IL-6, and increased amounts of the Th2-like cytokine IL-4, after stimulation in vitro.ConclusionMirtazapine treatment rapidly alters hepatic B cell populations, enhancing hepatic retention of CXCR3-expressing innate-like B cells that generate a more anti-inflammatory cytokine profile. Mirtazapine-induced hepatic B cell shifts could potentially represent a novel therapeutic approach to immune-mediated liver diseases characterized by B cell driven pathology.

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Human B cell lineages associated with germinal centers following influenza vaccination are measurably evolving

eLife ◽

10.7554/elife.70873 ◽

2021 ◽

Vol 10 ◽

Author(s):

Kenneth B Hoehn ◽

Jackson S Turner ◽

Frederick I Miller ◽

Ruoyi Jiang ◽

Oliver G Pybus ◽

...

Keyword(s):

Influenza Virus ◽

B Cells ◽

Influenza Vaccination ◽

B Cell ◽

Seasonal Influenza ◽

Germinal Centers ◽

Cell Lineages ◽

Cell Evolution ◽

The Poor ◽

Poor Efficacy

The poor efficacy of seasonal influenza virus vaccines is often attributed to pre-existing immunity interfering with the persistence and maturation of vaccine-induced B cell responses. We previously showed that a subset of vaccine-induced B cell lineages are recruited into germinal centers (GCs) following vaccination, suggesting that affinity maturation of these lineages against vaccine antigens can occur. However, it remains to be determined whether seasonal influenza vaccination stimulates additional evolution of vaccine-specific lineages, and previous work has found no significant increase in somatic hypermutation (SHM) among influenza-binding lineages sampled from the blood following seasonal vaccination in humans. Here, we investigate this issue using a phylogenetic test of measurable immunoglobulin sequence evolution. We first validate this test through simulations and survey measurable evolution across multiple conditions. We find significant heterogeneity in measurable B cell evolution across conditions, with enrichment in primary response conditions such as HIV infection and early childhood development. We then show that measurable evolution following influenza vaccination is highly compartmentalized: while lineages in the blood are rarely measurably evolving following influenza vaccination, lineages containing GC B cells are frequently measurably evolving. Many of these lineages appear to derive from memory B cells. We conclude from these findings that seasonal influenza virus vaccination can stimulate additional evolution of responding B cell lineages, and imply that the poor efficacy of seasonal influenza vaccination is not due to a complete inhibition of vaccine-specific B cell evolution.

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A single-cell atlas of lymphocyte adaptive immune repertoires and transcriptomes reveals age-related differences in convalescent COVID-19 patients

10.1101/2021.02.12.430907 ◽

2021 ◽

Author(s):

Florian Bieberich ◽

Rodrigo Vazquez-Lombardi ◽

Alexander Yermanos ◽

Roy A. Ehling ◽

Derek M. Mason ◽

...

Keyword(s):

T Cell ◽

B Cells ◽

B Cell ◽

Single Cell ◽

Somatic Hypermutation ◽

Critical Role ◽

Young Patients ◽

Cell Receptors ◽

Adaptive Immune ◽

Age Related

AbstractCOVID-19 disease outcome is highly dependent on adaptive immunity from T and B lymphocytes, which play a critical role in the control, clearance and long-term protection against SARS-CoV-2. To date, there is limited knowledge on the composition of the T and B cell immune receptor repertoires [T cell receptors (TCRs) and B cell receptors (BCRs)] and transcriptomes in convalescent COVID-19 patients of different age groups. Here, we utilize single-cell sequencing (scSeq) of lymphocyte immune repertoires and transcriptomes to quantitatively profile the adaptive immune response in COVID-19 patients of varying age. We discovered highly expanded T and B cells in multiple patients, with the most expanded clonotypes coming from the effector CD8+ T cell population. Highly expanded CD8+ and CD4+ T cell clones show elevated markers of cytotoxicity (CD8: PRF1, GZMH, GNLY; CD4: GZMA), whereas clonally expanded B cells show markers of transition into the plasma cell state and activation across patients. By comparing young and old convalescent COVID-19 patients (mean ages = 31 and 66.8 years, respectively), we found that clonally expanded B cells in young patients were predominantly of the IgA isotype and their BCRs had incurred higher levels of somatic hypermutation than elderly patients. In conclusion, our scSeq analysis defines the adaptive immune repertoire and transcriptome in convalescent COVID-19 patients and shows important age-related differences implicated in immunity against SARS-CoV-2.

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