Your search keyword '"Tarlinton DM"' showing total 172 results

1. IL-21 has a critical role in establishing germinal centers by amplifying early B cell proliferation.

Author

Dvorscek, AR, McKenzie, CI, Robinson, MJ, Ding, Z, Pitt, C, O'Donnell, K, Zotos, D, Brink, R, Tarlinton, DM, Quast, I, Dvorscek, AR, McKenzie, CI, Robinson, MJ, Ding, Z, Pitt, C, O'Donnell, K, Zotos, D, Brink, R, Tarlinton, DM, and Quast, I

Abstract

The proliferation and differentiation of antigen-specific B cells, including the generation of germinal centers (GC), are prerequisites for long-lasting, antibody-mediated immune protection. Affinity for antigen determines B cell recruitment, proliferation, differentiation, and competitiveness in the response, largely through determining access to T cell help. However, how T cell-derived signals contribute to these outcomes is incompletely understood. Here, we report how the signature cytokine of follicular helper T cells, IL-21, acts as a key regulator of the initial B cell response by accelerating cell cycle progression and the rate of cycle entry, increasing their contribution to the ensuing GC. This effect occurs over a wide range of initial B cell receptor affinities and correlates with elevated AKT and S6 phosphorylation. Moreover, the resultant increased proliferation can explain the IL-21-mediated promotion of plasma cell differentiation. Collectively, our data establish that IL-21 acts from the outset of a T cell-dependent immune response to increase cell cycle progression and fuel cyclic re-entry of B cells, thereby regulating the initial GC size and early plasma cell output.

Published

2022

2. The concerted change in the distribution of cell cycle phases and zone composition in germinal centers is regulated by IL-21

Author

Zotos, D, Quast, I, Li-Wai-Suen, CSN, McKenzie, CI, Robinson, MJ, Kan, A, Smyth, GK, Hodgkin, PD, Tarlinton, DM, Zotos, D, Quast, I, Li-Wai-Suen, CSN, McKenzie, CI, Robinson, MJ, Kan, A, Smyth, GK, Hodgkin, PD, and Tarlinton, DM

Abstract

Humoral immune responses require germinal centres (GC) for antibody affinity maturation. Within GC, B cell proliferation and mutation are segregated from affinity-based positive selection in the dark zone (DZ) and light zone (LZ) substructures, respectively. While IL-21 is known to be important in affinity maturation and GC maintenance, here we show it is required for both establishing normal zone representation and preventing the accumulation of cells in the G1 cell cycle stage in the GC LZ. Cell cycle progression of DZ B cells is unaffected by IL-21 availability, as is the zone phenotype of the most highly proliferative GC B cells. Collectively, this study characterises the development of GC zones as a function of time and B cell proliferation and identifies IL-21 as an important regulator of these processes. These data help explain the requirement for IL-21 in normal antibody affinity maturation.

Published

2021

3. Display of Native Antigen on cDC1 That Have Spatial Access to Both T and B Cells Underlies Efficient Humoral Vaccination.

Author

Kato, Y, Steiner, TM, Park, H-Y, Hitchcock, RO, Zaid, A, Hor, JL, Devi, S, Davey, GM, Vremec, D, Tullett, KM, Tan, PS, Ahmet, F, Mueller, SN, Alonso, S, Tarlinton, DM, Ploegh, HL, Kaisho, T, Beattie, L, Manton, JH, Fernandez-Ruiz, D, Shortman, K, Lahoud, MH, Heath, WR, Caminschi, I, Kato, Y, Steiner, TM, Park, H-Y, Hitchcock, RO, Zaid, A, Hor, JL, Devi, S, Davey, GM, Vremec, D, Tullett, KM, Tan, PS, Ahmet, F, Mueller, SN, Alonso, S, Tarlinton, DM, Ploegh, HL, Kaisho, T, Beattie, L, Manton, JH, Fernandez-Ruiz, D, Shortman, K, Lahoud, MH, Heath, WR, and Caminschi, I

Abstract

Follicular dendritic cells and macrophages have been strongly implicated in presentation of native Ag to B cells. This property has also occasionally been attributed to conventional dendritic cells (cDC) but is generally masked by their essential role in T cell priming. cDC can be divided into two main subsets, cDC1 and cDC2, with recent evidence suggesting that cDC2 are primarily responsible for initiating B cell and T follicular helper responses. This conclusion is, however, at odds with evidence that targeting Ag to Clec9A (DNGR1), expressed by cDC1, induces strong humoral responses. In this study, we reveal that murine cDC1 interact extensively with B cells at the border of B cell follicles and, when Ag is targeted to Clec9A, can display native Ag for B cell activation. This leads to efficient induction of humoral immunity. Our findings indicate that surface display of native Ag on cDC with access to both T and B cells is key to efficient humoral vaccination.

Published

2020

4. The Amount of BCL6 in B Cells Shortly after Antigen Engagement Determines Their Representation in Subsequent Germinal Centers

Author

Robinson, MJ, Ding, Z, Pitt, C, Brodie, EJ, Quast, I, Tarlinton, DM, Zotos, D, Robinson, MJ, Ding, Z, Pitt, C, Brodie, EJ, Quast, I, Tarlinton, DM, and Zotos, D

Abstract

It is unknown whether the incremental increases in BCL6 amounts in antigen-activated B cells influence the unfolding differentiation before germinal center (GC) formation. By comparing shortly after immunization the distribution of conventional B cells to those enforced to express BCL6 at the upper quartile of normal and those lacking BCL6 altogether, we determined that B cell representation in the stages before the GC compartment was related to BCL6 amounts. This was not by increased proliferation or suppression of early plasmablast differentiation, but rather by preferential recruitment and progression through these early stages of B cell activation, culminating in preferential transition into GC. Once established, this bias was stable in GC over several weeks; other BCL6-regulated GC B cell behaviors were unaffected. We propose that setting BCL6 amounts very early in activated B cells will be central in determining clonal representation in the GC and thus memory populations.

Published

2020

5. An Erg-driven transcriptional program controls B cell lymphopoiesis.

Author

Ng, AP, Coughlan, HD, Hediyeh-Zadeh, S, Behrens, K, Johanson, TM, Low, MSY, Bell, CC, Gilan, O, Chan, Y-C, Kueh, AJ, Boudier, T, Feltham, R, Gabrielyan, A, DiRago, L, Hyland, CD, Ierino, H, Mifsud, S, Viney, E, Willson, T, Dawson, MA, Allan, RS, Herold, MJ, Rogers, K, Tarlinton, DM, Smyth, GK, Davis, MJ, Nutt, SL, Alexander, WS, Ng, AP, Coughlan, HD, Hediyeh-Zadeh, S, Behrens, K, Johanson, TM, Low, MSY, Bell, CC, Gilan, O, Chan, Y-C, Kueh, AJ, Boudier, T, Feltham, R, Gabrielyan, A, DiRago, L, Hyland, CD, Ierino, H, Mifsud, S, Viney, E, Willson, T, Dawson, MA, Allan, RS, Herold, MJ, Rogers, K, Tarlinton, DM, Smyth, GK, Davis, MJ, Nutt, SL, and Alexander, WS

Abstract

B lymphoid development is initiated by the differentiation of hematopoietic stem cells into lineage committed progenitors, ultimately generating mature B cells. This highly regulated process generates clonal immunological diversity via recombination of immunoglobulin V, D and J gene segments. While several transcription factors that control B cell development and V(D)J recombination have been defined, how these processes are initiated and coordinated into a precise regulatory network remains poorly understood. Here, we show that the transcription factor ETS Related Gene (Erg) is essential for early B lymphoid differentiation. Erg initiates a transcriptional network involving the B cell lineage defining genes, Ebf1 and Pax5, which directly promotes expression of key genes involved in V(D)J recombination and formation of the B cell receptor. Complementation of Erg deficiency with a productively rearranged immunoglobulin gene rescued B lineage development, demonstrating that Erg is an essential and stage-specific regulator of the gene regulatory network controlling B lymphopoiesis.

Published

2020

6. Hhex regulates murine lymphoid progenitor survival independently of Stat5 and Cdkn2a

Author

Jackson, JT, O'Donnell, K, Light, A, Goh, W, Huntington, ND, Tarlinton, DM, McCormack, MP, Jackson, JT, O'Donnell, K, Light, A, Goh, W, Huntington, ND, Tarlinton, DM, and McCormack, MP

Abstract

The transcription factor Hhex (hematopoietically expressed homeobox gene) is critical for development of multiple lymphoid lineages beyond the common lymphoid progenitor. In addition, Hhex regulates hematopoietic stem cell (HSC) self-renewal, emergency hematopoiesis, and acute myeloid leukemia initiation and maintenance. Hhex mediates its effects on HSCs and acute myeloid leukemia stem cells via repression of the Cdkn2a tumor suppressor locus. However, we report here that loss of Cdkn2a does not rescue the failure of lymphoid development caused by loss of Hhex. As loss of Hhex causes apoptosis of lymphoid progenitors associated with impaired Bcl2 expression and defective Stat5b signaling, we tested the effects of rescuing these pathways using transgenic mice. Expression of the anti-apoptotic factor Bcl2, but not activated Stat5, rescued the development of T-, B-, and NK-cell lineages in the absence of Hhex. These results indicate that Bcl2 expression, but not Stat5b signaling or loss of Cdkn2a, can overcome the lymphoid deficiencies caused by the absence of Hhex, suggesting that the primary role of this transcription factor is to promote survival of lymphoid progenitors during early lymphoid development.

Published

2020

7. Atypical chemokine receptor 4 shapes activated B cell fate

Author

Kara, EE, Bastow, CR, McKenzie, DR, Gregor, CE, Fenix, KA, Babb, R, Norton, TS, Zotos, D, Rodda, LB, Hermes, JR, Bourne, K, Gilchrist, DS, Nibbs, RJ, Alsharifi, M, Vinuesa, CG, Tarlinton, DM, Brink, R, Hill, GR, Cyster, JG, Comerford, I, McColl, SR, Kara, EE, Bastow, CR, McKenzie, DR, Gregor, CE, Fenix, KA, Babb, R, Norton, TS, Zotos, D, Rodda, LB, Hermes, JR, Bourne, K, Gilchrist, DS, Nibbs, RJ, Alsharifi, M, Vinuesa, CG, Tarlinton, DM, Brink, R, Hill, GR, Cyster, JG, Comerford, I, and McColl, SR

Abstract

Activated B cells can initially differentiate into three functionally distinct fates-early plasmablasts (PBs), germinal center (GC) B cells, or early memory B cells-by mechanisms that remain poorly understood. Here, we identify atypical chemokine receptor 4 (ACKR4), a decoy receptor that binds and degrades CCR7 ligands CCL19/CCL21, as a regulator of early activated B cell differentiation. By restricting initial access to splenic interfollicular zones (IFZs), ACKR4 limits the early proliferation of activated B cells, reducing the numbers available for subsequent differentiation. Consequently, ACKR4 deficiency enhanced early PB and GC B cell responses in a CCL19/CCL21-dependent and B cell-intrinsic manner. Conversely, aberrant localization of ACKR4-deficient activated B cells to the IFZ was associated with their preferential commitment to the early PB linage. Our results reveal a regulatory mechanism of B cell trafficking via an atypical chemokine receptor that shapes activated B cell fate.

Published

2018

8. Lyn, Lupus, and (B) Lymphocytes, a Lesson on the Critical Balance of Kinase Signaling in immunity

Author

Brodie, EJ, Infantino, S, Low, MSY, Tarlinton, DM, Brodie, EJ, Infantino, S, Low, MSY, and Tarlinton, DM

Abstract

Systemic lupus erythematosus (SLE) is a progressive autoimmune disease characterized by increased sensitivity to self-antigens, auto-antibody production, and systemic inflammation. B cells have been implicated in disease progression and as such represent an attractive therapeutic target. Lyn is a Src family tyrosine kinase that plays a major role in regulating signaling pathways within B cells as well as other hematopoietic cells. Its role in initiating negative signaling cascades is especially critical as exemplified by Lyn-/- mice developing an SLE-like disease with plasma cell hyperplasia, underscoring the importance of tightly regulating signaling within B cells. This review highlights recent advances in our understanding of the function of the Src family tyrosine kinase Lyn in B lymphocytes and its contribution to positive and negative signaling pathways that are dysregulated in autoimmunity.

Published

2018

9. Proapoptotic BIM Impacts B Lymphoid Homeostasis by Limiting the Survival of Mature B Cells in a Cell-Autonomous Manner

Author

Liu, R, King, A, Bouillet, P, Tarlinton, DM, Strasser, A, Heierhorst, J, Liu, R, King, A, Bouillet, P, Tarlinton, DM, Strasser, A, and Heierhorst, J

Abstract

The proapoptotic BH3-only protein BIM (Bcl2l11) plays key roles in the maintenance of multiple hematopoietic cell types. In mice, germline knockout or conditional pan-hematopoietic deletion of Bim results in marked splenomegaly and significantly increased numbers of B cells. However, it has remained unclear whether these abnormalities reflect the loss of cell-intrinsic functions of BIM within the B lymphoid lineage and, if so, which stages in the lifecycle of B cells are most impacted by the loss of BIM. Here, we show that B lymphoid-specific conditional deletion of Bim during early development (i.e., in pro-B cells using Mb1-Cre) or during the final differentiation steps (i.e., in transitional B cells using Cd23-Cre) led to a similar >2-fold expansion of the mature follicular B cell pool. Notably, while the expansion of mature B cells was quantitatively similar in conditional and germline Bim-deficient mice, the splenomegaly was significantly attenuated after B lymphoid-specific compared to global Bim deletion. In vitro, conditional loss of Bim substantially increased the survival of mature B cells that were refractory to activation by lipopolysaccharide. Finally, we also found that conditional deletion of just one Bim allele by Mb1-Cre dramatically accelerated the development of Myc-driven B cell lymphoma, in a manner that was comparable to the effect of germline Bim heterozygosity. These data indicate that, under physiological conditions, BIM regulates B cell homeostasis predominantly by limiting the life span of non-activated mature B cells, and that it can have additional effects on developing B cells under pathological conditions.

Published

2018

10. Dynein light chain regulates adaptive and innate B cell development by distinctive genetic mechanisms

Author

Roopenian, DC, King, A, Li, L, Wong, DM, Liu, R, Bamford, R, Strasser, A, Tarlinton, DM, Heierhorst, J, Roopenian, DC, King, A, Li, L, Wong, DM, Liu, R, Bamford, R, Strasser, A, Tarlinton, DM, and Heierhorst, J

Abstract

Mechanistic differences in the development and function of adaptive, high-affinity antibody-producing B-2 cells and innate-like, "natural" antibody-producing B-1a cells remain poorly understood. Here we show that the multi-functional dynein light chain (DYNLL1/LC8) plays important roles in the establishment of B-1a cells in the peritoneal cavity and in the ongoing development of B-2 lymphoid cells in the bone marrow of mice. Epistasis analyses indicate that Dynll1 regulates B-1a and early B-2 cell development in a single, linear pathway with its direct transcriptional activator ASCIZ (ATMIN/ZNF822), and that the two genes also have complementary functions during late B-2 cell development. The B-2 cell defects caused by loss of DYNLL1 were associated with lower levels of the anti-apoptotic protein BCL-2, and could be supressed by deletion of pro-apoptotic BIM which is negatively regulated by both DYNLL1 and BCL-2. Defects in B cell development caused by loss of DYNLL1 could also be partially suppressed by a pre-arranged SWHEL Igm-B cell receptor transgene. In contrast to the rescue of B-2 cell numbers, the B-1a cell deficiency in Dynll1-deleted mice could not be suppressed by the loss of Bim, and was further compounded by the SWHEL transgene. Conversely, oncogenic MYC expression, which is synthetic lethal with Dynll1 deletion in B-2 cells, did not further reduce B-1a cell numbers in Dynll1-defcient mice. Finally, we found that the ASCIZ-DYNLL1 axis was also required for the early-juvenile development of aggressive MYC-driven and p53-deficient B cell lymphomas. These results identify ASCIZ and DYNLL1 as the core of a transcriptional circuit that differentially regulates the development of the B-1a and B-2 B lymphoid cell lineages and plays a critical role in lymphomagenesis.

Published

2017

11. Environmental sensing by mature B cells is controlled by the transcription factors PU.1 and SpiB

Author

Willis, SN, Tellier, J, Liao, Y, Trezise, S, Light, A, O'Donnell, K, Garrett-Sinha, LA, Shi, W, Tarlinton, DM, Nutt, SL, Willis, SN, Tellier, J, Liao, Y, Trezise, S, Light, A, O'Donnell, K, Garrett-Sinha, LA, Shi, W, Tarlinton, DM, and Nutt, SL

Abstract

Humoral immunity requires B cells to respond to multiple stimuli, including antigen, membrane and soluble ligands, and microbial products. Ets family transcription factors regulate many aspects of haematopoiesis, although their functions in humoral immunity are difficult to decipher as a result of redundancy between the family members. Here we show that mice lacking both PU.1 and SpiB in mature B cells do not generate germinal centers and high-affinity antibody after protein immunization. PU.1 and SpiB double-deficient B cells have a survival defect after engagement of CD40 or Toll-like receptors (TLR), despite paradoxically enhanced plasma cell differentiation. PU.1 and SpiB regulate the expression of many components of the B cell receptor signaling pathway and the receptors for CD40L, BAFF and TLR ligands. Thus, PU.1 and SpiB enable B cells to appropriately respond to environmental cues.

Published

2017

12. Dynamic changes in Id3 and E-protein activity orchestrate germinal center and plasma cell development

Author

Gloury, R, Zotos, D, Zuidscherwoude, M, Masson, F, Liao, Y, Hasbold, J, Corcoran, LM, Hodgkin, PD, Belz, GT, Shi, W, Nutt, SL, Tarlinton, DM, Kallies, A, Gloury, R, Zotos, D, Zuidscherwoude, M, Masson, F, Liao, Y, Hasbold, J, Corcoran, LM, Hodgkin, PD, Belz, GT, Shi, W, Nutt, SL, Tarlinton, DM, and Kallies, A

Abstract

The generation of high-affinity antibodies requires germinal center (GC) development and differentiation of long-lived plasma cells in a multilayered process that is tightly controlled by the activity of multiple transcription factors. Here, we reveal a new layer of complexity by demonstrating that dynamic changes in Id3 and E-protein activity govern both GC and plasma cell differentiation. We show that down-regulation of Id3 in B cells is essential for releasing E2A and E2-2, which in a redundant manner are required for antigen-induced B cell differentiation. We demonstrate that this pathway controls the expression of multiple key factors, including Blimp1, Xbp1, and CXCR4, and is therefore critical for establishing the transcriptional network that controls GC B cell and plasma cell differentiation.

Published

2016

13. MCL-1 is required throughout B-cell development and its loss sensitizes specific B-cell subsets to inhibition of BCL-2 or BCL-XL

Author

Vikstrom, IB, Slomp, A, Carrington, EM, Moesbergen, LM, Chang, C, Kelly, GL, Glaser, SP, Jansen, JHM, Leusen, JHW, Strasser, A, Huang, DCS, Lew, AM, Peperzak, V, Tarlinton, DM, Vikstrom, IB, Slomp, A, Carrington, EM, Moesbergen, LM, Chang, C, Kelly, GL, Glaser, SP, Jansen, JHM, Leusen, JHW, Strasser, A, Huang, DCS, Lew, AM, Peperzak, V, and Tarlinton, DM

Abstract

Pro-survival BCL-2 family members protect cells from programmed cell death that can be induced by multiple internal or external cues. Within the haematopoietic lineages, the BCL-2 family members BCL-2, BCL-XL and MCL-1 are known to support cell survival but the individual and overlapping roles of these pro-survival BCL-2 proteins for the persistence of individual leukocyte subsets in vivo has not yet been determined. By combining inducible knockout mouse models with the BH3-mimetic compound ABT-737, which inhibits BCL-2, BCL-XL and BCL-W, we found that dependency on MCL-1, BCL-XL or BCL-2 expression changes during B-cell development. We show that BCL-XL expression promotes survival of immature B cells, expression of BCL-2 is important for survival of mature B cells and long-lived plasma cells (PC), and expression of MCL-1 is important for survival throughout B-cell development. These data were confirmed with novel highly specific BH3-mimetic compounds that target either BCL-2, BCL-XL or MCL-1. In addition, we observed that combined inhibition of these pro-survival proteins acts in concert to delete specific B-cell subsets. Reduced expression of MCL-1 further sensitized immature as well as transitional B cells and splenic PC to loss of BCL-XL expression. More markedly, loss of MCL-1 greatly sensitizes PC populations to BCL-2 inhibition using ABT-737, even though the total wild-type PC pool in the spleen is not significantly affected by this drug and the bone marrow (BM) PC population only slightly. Combined loss or inhibition of MCL-1 and BCL-2 reduced the numbers of established PC >100-fold within days. Our data suggest that combination treatment targeting these pro-survival proteins could be advantageous for treatment of antibody-mediated autoimmune diseases and B-cell malignancies.

Published

2016

14. c-Myb is required for plasma cell migration to bone marrow after immunization or infection

Author

Good-Jacobson, KL, O'Donnell, K, Belz, GT, Nutt, SL, Tarlinton, DM, Good-Jacobson, KL, O'Donnell, K, Belz, GT, Nutt, SL, and Tarlinton, DM

Abstract

Plasma cell migration is crucial to immunity, but little is known about the molecular regulators of their migratory programs. Here, we detail the critical role of the transcription factor c-Myb in determining plasma cell location. In the absence of c-Myb, no IgG(+) antigen-specific plasma cells were detected in the bone marrow after immunization or virus infection. This was correlated with a dramatic reduction of plasma cells in peripheral blood, mislocalization in spleen, and an inability of c-Myb-deficient plasma cells to migrate along a CXCL12 gradient. Therefore, c-Myb plays an essential, novel role in establishing the long-lived plasma cell population in the BM via responsiveness to chemokine migration cues.

Published

2015

15. The Tetraspanin CD37 Orchestrates the alpha4beta1 Integrin-Akt Signaling Axis and Supports Long-Lived Plasma Cell Survival

Author

van Spriel AB, de Keijzer S, van der Schaaf A, Gartlan KH, Sofi M, Light A, Linssen PC, Boezeman JB, Zuidscherwoude M, Reinieren-Beeren I, Cambi A, Mackay F, Tarlinton DM, Figdor CG, and Wright MD

Published

2012

16. The transcription factors IRF8 and PU.1 negatively regulate plasma cell differentiation

Author

Carotta, S, Willis, SN, Hasbold, J, Inouye, M, Pang, SHM, Emslie, D, Light, A, Chopin, M, Shi, W, Wang, H, Morse, HC, Tarlinton, DM, Corcoran, LM, Hodgkin, PD, Nutt, SL, Carotta, S, Willis, SN, Hasbold, J, Inouye, M, Pang, SHM, Emslie, D, Light, A, Chopin, M, Shi, W, Wang, H, Morse, HC, Tarlinton, DM, Corcoran, LM, Hodgkin, PD, and Nutt, SL

Abstract

Activated B cells undergo immunoglobulin class-switch recombination (CSR) and differentiate into antibody-secreting plasma cells. The distinct transcriptomes of B cells and plasma cells are maintained by the antagonistic influences of two groups of transcription factors: those that maintain the B cell program, including BCL6 and PAX5, and plasma cell-promoting factors, such as IRF4 and BLIMP-1. We show that the complex of IRF8 and PU.1 controls the propensity of B cells to undergo CSR and plasma cell differentiation by concurrently promoting the expression of BCL6 and PAX5 and repressing AID and BLIMP-1. As the PU.1-IRF8 complex functions in a reciprocal manner to IRF4, we propose that concentration-dependent competition between these factors controls B cell terminal differentiation.

Published

2014

17. The Zinc-finger protein ASCIZ regulates B cell development via DYNLL1 and Bim

Author

Jurado, S, Gleeson, K, O'Donnell, K, Izon, DJ, Walkley, CR, Strasser, A, Tarlinton, DM, Heierhorst, J, Jurado, S, Gleeson, K, O'Donnell, K, Izon, DJ, Walkley, CR, Strasser, A, Tarlinton, DM, and Heierhorst, J

Abstract

Developing B lymphocytes expressing defective or autoreactive pre-B or B cell receptors (BCRs) are eliminated by programmed cell death, but how the balance between death and survival signals is regulated to prevent immunodeficiency and autoimmunity remains incompletely understood. In this study, we show that absence of the essential ATM (ataxia telangiectasia mutated) substrate Chk2-interacting Zn(2+)-finger protein (ASCIZ; also known as ATMIN/ZNF822), a protein with dual functions in the DNA damage response and as a transcription factor, leads to progressive cell loss from the pre-B stage onwards and severely diminished splenic B cell numbers in mice. This lymphopenia cannot be suppressed by deletion of p53 or complementation with a prearranged BCR, indicating that it is not caused by impaired DNA damage responses or defective V(D)J recombination. Instead, ASCIZ-deficient B cell precursors contain highly reduced levels of DYNLL1 (dynein light chain 1; LC8), a recently identified transcriptional target of ASCIZ, and normal B cell development can be restored by ectopic Dynll1 expression. Remarkably, the B cell lymphopenia in the absence of ASCIZ can also be fully suppressed by deletion of the proapoptotic DYNLL1 target Bim. Our findings demonstrate a key role for ASCIZ in regulating the survival of developing B cells by activating DYNLL1 expression, which may then modulate Bim-dependent apoptosis.

Published

2012

18. B and T cells collaborate in antiviral responses via IL-6, IL-21, and transcriptional activator and coactivator, Oct2 and OBF-1

Author

Karnowski, A, Chevrier, S, Belz, GT, Mount, A, Emslie, D, D'Costa, K, Tarlinton, DM, Kallies, A, Corcoran, LM, Karnowski, A, Chevrier, S, Belz, GT, Mount, A, Emslie, D, D'Costa, K, Tarlinton, DM, Kallies, A, and Corcoran, LM

Abstract

A strong humoral response to infection requires the collaboration of several hematopoietic cell types that communicate via antigen presentation, surface coreceptors and their ligands, and secreted factors. The proinflammatory cytokine IL-6 has been shown to promote the differentiation of activated CD4(+) T cells into T follicular helper cells (T(FH) cells) during an immune response. T(FH) cells collaborate with B cells in the formation of germinal centers (GCs) during T cell-dependent antibody responses, in part through secretion of critical cytokines such as IL-21. In this study, we demonstrate that loss of either IL-6 or IL-21 has marginal effects on the generation of T(FH) cells and on the formation of GCs during the response to acute viral infection. However, mice lacking both IL-6 and IL-21 were unable to generate a robust T(FH) cell-dependent immune response. We found that IL-6 production in follicular B cells in the draining lymph node was an important early event during the antiviral response and that B cell-derived IL-6 was necessary and sufficient to induce IL-21 from CD4(+) T cells in vitro and to support T(FH) cell development in vivo. Finally, the transcriptional activator Oct2 and its cofactor OBF-1 were identified as regulators of Il6 expression in B cells.

Published

2012

19. B cell priming for extrafollicular antibody responses requires Bcl-6 expression by T cells

Author

Lee, SK, Rigby, RJ, Zotos, D, Tsai, LM, Kawamoto, S, Marshall, JL, Ramiscal, RR, Chan, TD, Gatto, D, Brink, R, Yu, D, Fagarasan, S, Tarlinton, DM, Cunningham, AF, Vinuesa, CG, Lee, SK, Rigby, RJ, Zotos, D, Tsai, LM, Kawamoto, S, Marshall, JL, Ramiscal, RR, Chan, TD, Gatto, D, Brink, R, Yu, D, Fagarasan, S, Tarlinton, DM, Cunningham, AF, and Vinuesa, CG

Abstract

T follicular helper cells (Tfh cells) localize to follicles where they provide growth and selection signals to mutated germinal center (GC) B cells, thus promoting their differentiation into high affinity long-lived plasma cells and memory B cells. T-dependent B cell differentiation also occurs extrafollicularly, giving rise to unmutated plasma cells that are important for early protection against microbial infections. Bcl-6 expression in T cells has been shown to be essential for the formation of Tfh cells and GC B cells, but little is known about its requirement in physiological extrafollicular antibody responses. We use several mouse models in which extrafollicular plasma cells can be unequivocally distinguished from those of GC origin, combined with antigen-specific T and B cells, to show that the absence of T cell-expressed Bcl-6 significantly reduces T-dependent extrafollicular antibody responses. Bcl-6(+) T cells appear at the T-B border soon after T cell priming and before GC formation, and these cells express low amounts of PD-1. Their appearance precedes that of Bcl-6(+) PD-1(hi) T cells, which are found within the GC. IL-21 acts early to promote both follicular and extrafollicular antibody responses. In conclusion, Bcl-6(+) T cells are necessary at B cell priming to form extrafollicular antibody responses, and these pre-GC Tfh cells can be distinguished phenotypically from GC Tfh cells.

Published

2011

20. IL-21 regulates germinal center B cell differentiation and proliferation through a B cell-intrinsic mechanism

Author

Zotos, D, Coquet, JM, Zhang, Y, Light, A, D'Costa, K, Kallies, A, Corcoran, LM, Godfrey, DI, Toellner, K-M, Smyth, MJ, Nutt, SL, Tarlinton, DM, Zotos, D, Coquet, JM, Zhang, Y, Light, A, D'Costa, K, Kallies, A, Corcoran, LM, Godfrey, DI, Toellner, K-M, Smyth, MJ, Nutt, SL, and Tarlinton, DM

Abstract

Germinal centers (GCs) are sites of B cell proliferation, somatic hypermutation, and selection of variants with improved affinity for antigen. Long-lived memory B cells and plasma cells are also generated in GCs, although how B cell differentiation in GCs is regulated is unclear. IL-21, secreted by T follicular helper cells, is important for adaptive immune responses, although there are conflicting reports on its target cells and mode of action in vivo. We show that the absence of IL-21 signaling profoundly affects the B cell response to protein antigen, reducing splenic and bone marrow plasma cell formation and GC persistence and function, influencing their proliferation, transition into memory B cells, and affinity maturation. Using bone marrow chimeras, we show that these activities are primarily a result of CD3-expressing cells producing IL-21 that acts directly on B cells. Molecularly, IL-21 maintains expression of Bcl-6 in GC B cells. The absence of IL-21 or IL-21 receptor does not abrogate the appearance of T cells in GCs or the appearance of CD4 T cells with a follicular helper phenotype. IL-21 thus controls fate choices of GC B cells directly.

Published

2010

21. Membrane-bound Fas ligand only is essential for Fas-induced apoptosis

Author

Reilly, LAO, Tai, L, Lee, L, Kruse, EA, Grabow, S, Fairlie, WD, Haynes, NM, Tarlinton, DM, Zhang, J-G, Belz, GT, Smyth, MJ, Bouillet, P, Robb, L, Strasser, A, Reilly, LAO, Tai, L, Lee, L, Kruse, EA, Grabow, S, Fairlie, WD, Haynes, NM, Tarlinton, DM, Zhang, J-G, Belz, GT, Smyth, MJ, Bouillet, P, Robb, L, and Strasser, A

Abstract

Fas ligand (FasL), an apoptosis-inducing member of the TNF cytokine family, and its receptor Fas are critical for the shutdown of chronic immune responses and prevention of autoimmunity. Accordingly, mutations in their genes cause severe lymphadenopathy and autoimmune disease in mice and humans. FasL function is regulated by deposition in the plasma membrane and metalloprotease-mediated shedding. Here we generated gene-targeted mice that selectively lack either secreted FasL (sFasL) or membrane-bound FasL (mFasL) to resolve which of these forms is required for cell killing and to explore their hypothesized non-apoptotic activities. Mice lacking sFasL (FasL(Deltas/Deltas)) appeared normal and their T cells readily killed target cells, whereas T cells lacking mFasL (FasL(Deltam/Deltam)) could not kill cells through Fas activation. FasL(Deltam/Deltam) mice developed lymphadenopathy and hyper-gammaglobulinaemia, similar to FasL(gld/gld) mice, which express a mutant form of FasL that cannot bind Fas, but surprisingly, FasL(Deltam/Deltam) mice (on a C57BL/6 background) succumbed to systemic lupus erythematosus (SLE)-like autoimmune kidney destruction and histiocytic sarcoma, diseases that occur only rarely and much later in FasL(gld/gld) mice. These results demonstrate that mFasL is essential for cytotoxic activity and constitutes the guardian against lymphadenopathy, autoimmunity and cancer, whereas excess sFasL appears to promote autoimmunity and tumorigenesis through non-apoptotic activities.

Published

2009

22. A requirement for CD45 distinguishes Ly49D-mediated cytokine and chemokine production from killing in primary natural killer cells

Author

Huntington, ND, Xu, YK, Nutt, SL, Tarlinton, DM, Huntington, ND, Xu, YK, Nutt, SL, and Tarlinton, DM

Abstract

Engagement of receptors on the surface of natural killer (NK) cells initiates a biochemical cascade ultimately triggering cytokine production and cytotoxicity, although the interrelationship between these two outcomes is currently unclear. In this study we investigate the role of the cell surface phosphatase CD45 in NK cell development and intracellular signaling from activating receptors. Stimulation via the major histocompatibility complex I-binding receptor, Ly49D on CD45(-/-) primary NK cells resulted in the activation of phosphoinositide-3-kinase and normal cytotoxicity but failed to elicit a range of cytokines and chemokines. This blockage is associated with impaired phosphorylation of Syk, Vav1, JNK, and p38, which mimics data obtained using inhibitors of the src-family kinases (SFK). These data, supported by analogous findings after CD16 and NKG2D stimulation of CD45(-/-) primary NK cells, place CD45 upstream of SFK in NK cells after stimulation via immunoreceptor tyrosine-based activation motif-containing receptors. Thus we identify CD45 as a pivotal enzyme in eliciting a precise subset of NK cell responses.

Published

2005

23. Differential requirement for OBF-1 during antibody-secreting cell differentiation

Author

Corcoran, LM, Hasbold, J, Dietrich, W, Hawkins, E, Kallies, A, Nutt, SL, Tarlinton, DM, Matthias, P, Hodgkin, PD, Corcoran, LM, Hasbold, J, Dietrich, W, Hawkins, E, Kallies, A, Nutt, SL, Tarlinton, DM, Matthias, P, and Hodgkin, PD

Abstract

Resting B cells can be cultured to induce antibody-secreting cell (ASC) differentiation in vitro. A quantitative analysis of cell behavior during such a culture allows the influences of different stimuli and gene products to be measured. The application of this analytical system revealed that the OBF-1 transcriptional coactivator, whose loss impairs antibody production in vivo, has two effects on ASC development. Although OBF-1 represses early T cell-dependent (TD) differentiation, it is also critical for the completion of the final stages of ASC development. Under these conditions, the loss of OBF-1 blocks the genetic program of ASC differentiation so that Blimp-1/prdm1 induction fails, and bcl-6, Pax5, and AID are not repressed as in control ASC. Retroviral complementation confirmed that OBF-1 was the critical entity. Surprisingly, when cells were cultured in lipopolysaccharide to mimic T cell-independent conditions, OBF-1-null B cells differentiated normally to ASC. In the OBF-1(-/-) ASC generated under either culture regimen, antibody production was normal or only modestly reduced, revealing that Ig genes are not directly dependent on OBF-1 for their expression. The differential requirement for OBF-1 in TD ASC generation was confirmed in vivo. These studies define a new regulatory role for OBF-1 in determining the cell-autonomous capacity of B cells to undergo terminal differentiation in response to different immunological signals.

Published

2005

24. Early appearance of germinal center-derived memory B cells and plasma cells in blood after primary immunization

Author

Blink, EJ, Light, A, Kallies, A, Nutt, SL, Hodgkin, PD, Tarlinton, DM, Blink, EJ, Light, A, Kallies, A, Nutt, SL, Hodgkin, PD, and Tarlinton, DM

Abstract

Immunization with a T cell-dependent antigen elicits production of specific memory B cells and antibody-secreting cells (ASCs). The kinetic and developmental relationships between these populations and the phenotypic forms they and their precursors may take remain unclear. Therefore, we examined the early stages of a primary immune response, focusing on the appearance of antigen-specific B cells in blood. Within 1 wk, antigen-specific B cells appear in the blood with either a memory phenotype or as immunoglobulin (Ig)G1 ASCs expressing blimp-1. The memory cells have mutated V(H) genes; respond to the chemokine CXCL13 but not CXCL12, suggesting recirculation to secondary lymphoid organs; uniformly express B220; show limited differentiation potential unless stimulated by antigen; and develop independently of blimp-1 expression. The antigen-specific IgG1 ASCs in blood show affinity maturation paralleling that of bone marrow ASCs, raising the possibility that this compartment is established directly by blood-borne ASCs. We find no evidence for a blimp-1-expressing preplasma memory compartment, suggesting germinal center output is restricted to ASCs and B220(+) memory B cells, and this is sufficient to account for the process of affinity maturation.

Published

2005

25. Lyn-deficient mice develop severe, persistent asthma: Lyn is a critical negative regulator of Th2 immunity

Author

Beavitt, SJE, Harder, KW, Kemp, JM, Jones, J, Quilici, C, Casagranda, F, Lam, E, Turner, D, Brennan, S, Sly, PD, Tarlinton, DM, Anderson, GP, Hibbs, ML, Beavitt, SJE, Harder, KW, Kemp, JM, Jones, J, Quilici, C, Casagranda, F, Lam, E, Turner, D, Brennan, S, Sly, PD, Tarlinton, DM, Anderson, GP, and Hibbs, ML

Abstract

The etiology of asthma, a chronic inflammatory disorder of the airways, remains obscure, although T cells appear to be central disease mediators. Lyn tyrosine kinase has been implicated as both a facilitator and inhibitor of signaling pathways that play a role in allergic inflammation, although its role in asthma is unclear because Lyn is not expressed in T cells. We show in the present study that Lyn-/- mice develop a severe, persistent inflammatory asthma-like syndrome with lung eosinophilia, mast cell hyperdegranulation, intensified bronchospasm, hyper IgE, and Th2-polarizing dendritic cells. Dendritic cells from Lyn-/- mice have a more immature phenotype, exhibit defective inhibitory signaling pathways, produce less IL-12, and can transfer disease when adoptively transferred into wild-type recipients. Our results show that Lyn regulates the intensity and duration of multiple asthmatic traits and indicate that Lyn is an important negative regulator of Th2 immune responses.

Published

2005

26. Targeting plasma cells in autoimmune diseases

Author

Tarlinton, DM, Hodgkin, PD, Tarlinton, DM, and Hodgkin, PD

Abstract

Antibodies specific for self-antigens mediate life-threatening pathology in several autoimmune diseases. Clearly the ability to target the plasma cells (PCs) producing the autoantibodies would be of great clinical benefit. Current immunosuppressive therapies are based on the premise that autoreactive PCs are short-lived and replenished from ongoing immune responses. However, recent results question this assumption and suggest that optimizing the treatment of severe autoimmune conditions will require a significant investment in elucidating the details of PC biology.

Published

2004

27. Plasma cell ontogeny defined by quantitative changes in Blimp-1 expression

Author

Kallies, A, Hasbold, J, Tarlinton, DM, Dietrich, W, Corcoran, LM, Hodgkin, PD, Nutt, SL, Kallies, A, Hasbold, J, Tarlinton, DM, Dietrich, W, Corcoran, LM, Hodgkin, PD, and Nutt, SL

Abstract

Plasma cells comprise a population of terminally differentiated B cells that are dependent on the transcriptional regulator B lymphocyte--induced maturation protein 1 (Blimp-1) for their development. We have introduced a gfp reporter into the Blimp-1 locus and shown that heterozygous mice express the green fluorescent protein in all antibody-secreting cells (ASCs) in vivo and in vitro. In vitro, these cells display considerable heterogeneity in surface phenotype, immunoglobulin secretion rate, and Blimp-1 expression levels. Importantly, analysis of in vivo ASCs induced by immunization reveals a developmental pathway in which increasing levels of Blimp-1 expression define developmental stages of plasma cell differentiation that have many phenotypic and molecular correlates. Thus, maturation from transient plasmablast to long-lived ASCs in bone marrow is predicated on quantitative increases in Blimp-1 expression.

Published

2004

28. Generation and analysis of Siah2 mutant mice

Author

Frew, IJ, Hammond, VE, Dickins, RA, Quinn, JMW, Walkley, CR, Sims, NA, Schnall, R, Della, NG, Holloway, AJ, Digby, MR, Janes, PW, Tarlinton, DM, Purton, LE, Gillespie, MT, Bowtell, DDL, Frew, IJ, Hammond, VE, Dickins, RA, Quinn, JMW, Walkley, CR, Sims, NA, Schnall, R, Della, NG, Holloway, AJ, Digby, MR, Janes, PW, Tarlinton, DM, Purton, LE, Gillespie, MT, and Bowtell, DDL

Abstract

Siah proteins function as E3 ubiquitin ligase enzymes to target the degradation of diverse protein substrates. To characterize the physiological roles of Siah2, we have generated and analyzed Siah2 mutant mice. In contrast to Siah1a knockout mice, which are growth retarded and exhibit defects in spermatogenesis, Siah2 mutant mice are fertile and largely phenotypically normal. While previous studies implicate Siah2 in the regulation of TRAF2, Vav1, OBF-1, and DCC, we find that a variety of responses mediated by these proteins are unaffected by loss of Siah2. However, we have identified an expansion of myeloid progenitor cells in the bone marrow of Siah2 mutant mice. Consistent with this, we show that Siah2 mutant bone marrow produces more osteoclasts in vitro than wild-type bone marrow. The observation that combined Siah2 and Siah1a mutation causes embryonic and neonatal lethality demonstrates that the highly homologous Siah proteins have partially overlapping functions in vivo.

Published

2003

29. Loss of the pro-apoptotic BH3-only Bcl-2 family member Bim inhibits BCR stimulation-induced apoptosis and deletion of autoreactive B cells

Author

Enders, A, Bouillet, P, Puthalakath, H, Xu, YK, Tarlinton, DM, Strasser, A, Enders, A, Bouillet, P, Puthalakath, H, Xu, YK, Tarlinton, DM, and Strasser, A

Abstract

During development, the stochastic process assembling the genes encoding antigen receptors invariably generates B and T lymphocytes that can recognize self-antigens. Several mechanisms have evolved to prevent the activation of these cells and the concomitant development of autoimmune disease. One such mechanism is the induction of apoptosis in developing or mature B cells by engagement of the B cell antigen receptor (BCR) in the absence of T cell help. Here we report that B lymphocytes lacking the pro-apoptotic Bcl-2 family member Bim are refractory to apoptosis induced by BCR ligation in vitro. The loss of Bim also inhibited deletion of autoreactive B cells in vivo in two transgenic systems of B cell tolerance. Bim loss prevented deletion of autoreactive B cells induced by soluble self-antigen and promoted accumulation of self-reactive B cells developing in the presence of membrane-bound self-antigen, although their numbers were considerably lower compared with antigen-free mice. Mechanistically, we determined that BCR ligation promoted interaction of Bim with Bcl-2, inhibiting its survival function. These findings demonstrate that Bim is a critical player in BCR-mediated apoptosis and in B lymphocyte deletion.

Published

2003

30. Sustained activation of Lyn tyrosine kinase in vivo leads to autoimmunity

Author

Hibbs, ML, Harder, KW, Armes, J, Kountouri, N, Quilici, C, Casagranda, F, Dunn, AR, Tarlinton, DM, Hibbs, ML, Harder, KW, Armes, J, Kountouri, N, Quilici, C, Casagranda, F, Dunn, AR, and Tarlinton, DM

Abstract

Genetic ablation of the Lyn tyrosine kinase has revealed unique inhibitory roles in B lymphocyte signaling. We now report the consequences of sustained activation of Lyn in vivo using a targeted gain-of-function mutation (Lyn(up/up) mice). Lyn(up/up) mice have reduced numbers of conventional B lymphocytes, down-regulated surface immunoglobulin M and costimulatory molecules, and elevated numbers of B1a B cells. Lyn(up/up) B cells are characterized by the constitutive phosphorylation of negative regulators of B cell antigen receptor (BCR) signaling including CD22, SHP-1, and SHIP-1, and display attributes of lymphocytes rendered tolerant by constitutive engagement of the antigen receptor. However, exaggerated positive signaling is also apparent as evidenced by the constitutive phosphorylation of Syk and phospholipase Cgamma2 in resting Lyn(up/up) B cells. Similarly, Lyn(up/up) B cells show a heightened calcium flux in response to BCR stimulation. Surprisingly, Lyn(up/up) mice develop circulating autoreactive antibodies and lethal autoimmune glomerulonephritis, suggesting that enhanced positive signaling eventually overrides constitutive negative signaling. These studies highlight the difficulty in maintaining tolerance in the face of chronic stimulation and emphasize the pivotal role of Lyn in B cell signaling.

Published

2002

31. Defective gp130-mediated signal transducer and activator of transcription (STAT) signaling results in degenerative joint disease, gastrointestinal ulceration, and failure of uterine implantation

Author

Ernst, M, Inglese, M, Waring, P, Campbell, IK, Bao, SS, Clay, FJ, Alexander, WS, Wicks, IP, Tarlinton, DM, Novak, U, Heath, JK, Dunn, AR, Ernst, M, Inglese, M, Waring, P, Campbell, IK, Bao, SS, Clay, FJ, Alexander, WS, Wicks, IP, Tarlinton, DM, Novak, U, Heath, JK, and Dunn, AR

Abstract

The receptor subunit gp130 transduces multiple cell type-specific activities of the leukemia inhibitory factor (LIF)/interleukin (IL)-6 family of cytokines through the signal transducer and activator of transcription (STAT) and src homology 2 domain-bearing protein tyrosine phosphatase (SHP)-2/ras/Erk pathways. To define STAT-dependent physiological responses, we generated mice with a COOH-terminal gp130(DeltaSTAT) "knock-in" mutation which deleted all STAT-binding sites. gp130(DeltaSTAT) mice phenocopyed mice deficient for IL-6 (impaired humoral and mucosal immune and hepatic acute phase responses) and LIF (failure of blastocyst implantation). However, unlike mice with null mutations in any of the components in the gp130 signaling pathway, gp130(DeltaSTAT) mice also displayed gastrointestinal ulceration and a severe joint disease with features of chronic synovitis, cartilaginous metaplasia, and degradation of the articular cartilage. Mitogenic hyperresponsiveness of synovial cells to the LIF/IL-6 family of cyto-kines was caused by sustained gp130-mediated SHP-2/ras/Erk activation due to impaired STAT-mediated induction of suppressor of cytokine signaling (SOCS) proteins which normally limits gp130 signaling. Therefore, the joint pathology in gp130(DeltaSTAT) mice is likely to arise from the disturbance of the otherwise balanced activation of the SHP-2/ras/Erk and STAT signaling cascades emanating from gp130.

Published

2001

32. Autoimmune regulator controls T cell help for pathogenetic autoantibody production in collagen-induced arthritis.

Author

Campbell IK, Kinkel SA, Drake SF, Nieuwenhuijze AV, Hubert FX, Tarlinton DM, Heath WR, Scott HS, and Wicks IP

Abstract

OBJECTIVE: Autoimmune regulator (Aire) promotes the ectopic expression of tissue-restricted antigens in medullary thymic epithelial cells (mTECs), leading to negative selection of autoreactive T cells. This study was undertaken to determine whether loss of central tolerance renders Aire-deficient (Aire(-/-)) mice more susceptible to the induction of autoimmune arthritis. METHODS: Medullary TECs were isolated from Aire(-/-) and wild-type C57BL/6 mice for gene expression analysis. Collagen-induced arthritis (CIA) was elicited by injection of chick type II collagen (CII) in adjuvant. Cellular and humoral immune responses to CII were evaluated. Chimeric mice were created by reconstituting lymphocyte-deficient mice with either Aire(-/-) or wild-type CD4 T cells and wild-type B cells. RESULTS: Wild-type, but not Aire(-/-), mTECs expressed the CII gene Col2a1. Aire(-/-) mice developed more rapid and severe CIA, showing elevated serum anti-CII IgG levels, with earlier switching to arthritogenic IgG subclasses. No evidence was found of enhanced T cell responsiveness to CII in Aire(-/-) mice; however, Aire(-/-) CD4 T cells were more efficient at stimulating wild-type B cells to produce anti-CII IgG following immunization of chimeric mice with CII. CONCLUSION: Our findings indicate that Aire-dependent expression of CII occurs in mTECs, implying that there is central tolerance to self antigens found in articular cartilage. Reduced central tolerance to CII in Aire(-/-) mice manifests as increased CD4 T cell help to B cells for cross-reactive autoantibody production and enhanced CIA. Aire and central tolerance help prevent cross-reactive autoimmune responses to CII initiated by environmental stimuli and limit spontaneous autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2009

33. Conversion of vaccines from low to high immunogenicity by antibodies with epitope complementarity.

Author

Dvorscek AR, McKenzie CI, Stäheli VC, Ding Z, White J, Fabb SA, Lim L, O'Donnell K, Pitt C, Christ D, Hill DL, Pouton CW, Burnett DL, Brink R, Robinson MJ, Tarlinton DM, and Quast I

Subjects

Animals, Mice, Vaccines immunology, Lymphocyte Activation immunology, Cell Differentiation immunology, Epitopes immunology, Mice, Inbred C57BL, Epitopes, B-Lymphocyte immunology, Immunogenicity, Vaccine, Antibodies, Monoclonal immunology, Immunity, Humoral immunology, Antibody Affinity immunology, Memory B Cells immunology, Receptors, Antigen, B-Cell immunology, Germinal Center immunology, B-Lymphocytes immunology

Abstract

Existing antibodies (Abs) have varied effects on humoral immunity during subsequent infections. Here, we leveraged in vivo systems that allow precise control of antigen-specific Abs and B cells to examine the impact of Ab dose, affinity, and specificity in directing B cell activation and differentiation. Abs competing with the B cell receptor (BCR) epitope showed affinity-dependent suppression. By contrast, Abs targeting a complementary epitope, not overlapping with the BCR, shifted B cell differentiation toward Ab-secreting cells. Such Abs allowed for potent germinal center (GC) responses to otherwise poorly immunogenic sites by promoting antigen capture and presentation by low-affinity B cells. These mechanisms jointly diversified the B cell repertoire by facilitating the recruitment of high- and low-affinity B cells into Ab-secreting cell, GC, and memory B cell fates. Incorporation of small amounts of monoclonal Abs into protein- or mRNA-based vaccines enhanced immunogenicity and facilitated sustained immune responses, with implications for vaccine design and our understanding of protective immunity., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

34. Ki67 deficiency impedes chromatin accessibility and BCR gene rearrangement.

Author

Ding Z, Hagan M, Yan F, Schroer NWY, Polmear J, Good-Jacobson KL, Dvorscek AR, Pitt C, O'Donnell K, Nutt SL, Zotos D, McKenzie C, Hill DL, Robinson MJ, Quast I, Koentgen F, and Tarlinton DM

Subjects

Animals, Lymphopoiesis genetics, Receptors, Antigen, B-Cell metabolism, Receptors, Antigen, B-Cell genetics, Mice, Gene Rearrangement, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, T-Lymphocytes metabolism, T-Lymphocytes immunology, Mice, Inbred C57BL, Cell Proliferation genetics, Ki-67 Antigen metabolism, Chromatin metabolism, Chromatin genetics, B-Lymphocytes metabolism, B-Lymphocytes immunology

Abstract

The proliferation marker Ki67 has been attributed critical functions in maintaining mitotic chromosome morphology and heterochromatin organization during the cell cycle, indicating a potential role in developmental processes requiring rigid cell-cycle control. Here, we discovered that despite normal fecundity and organogenesis, germline deficiency in Ki67 resulted in substantial defects specifically in peripheral B and T lymphocytes. This was not due to impaired cell proliferation but rather to early lymphopoiesis at specific stages where antigen-receptor gene rearrangements occurred. We identified that Ki67 was required for normal global chromatin accessibility involving regulatory regions of genes critical for checkpoint stages in B cell lymphopoiesis. In line with this, mRNA expression of Rag1 was diminished and gene rearrangement was less efficient in the absence of Ki67. Transgenes encoding productively rearranged immunoglobulin heavy and light chains complemented Ki67 deficiency, completely rescuing early B cell development. Collectively, these results identify a unique contribution from Ki67 to somatic antigen-receptor gene rearrangement during lymphopoiesis., (© 2024 Ding et al.)

Published

2024

35. Predicting plasma cell retention and loss over a lifetime.

Author

Robinson MJ and Tarlinton DM

Subjects

Plasma Cells

Abstract

Plasma cells (PCs) rely on external survival cues for persistence, which limits the size of the PC pool. How, then, are new specificities incorporated into a saturated system? In this issue of Immunity, Simons and Karin put forward a mathematical framework to explain PC retention that makes testable predictions about steady-state lifespan structure, withstands tests based on accrual and displaceability, and accounts for lifespan stratification with specificity., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

36. Intrinsically determined turnover underlies broad heterogeneity in plasma-cell lifespan.

Author

Robinson MJ, Ding Z, Dowling MR, Hill DL, Webster RH, McKenzie C, Pitt C, O'Donnell K, Mulder J, Brodie E, Hodgkin PD, Wong NC, Quast I, and Tarlinton DM

Subjects

Antibody-Producing Cells, Plasma Cells, Longevity

Abstract

Antibodies produced by antibody-secreting plasma cells (ASCs) underlie multiple forms of long-lasting immunity. Here we examined the mechanisms regulating ASC turnover and persistence using a genetic reporter to time-stamp ASCs. This approach revealed ASC lifespans as heterogeneous and falling on a continuum, with only a small fraction surviving for >60 days. ASC longevity past 60 days was independent of isotype but correlated with a phenotype that developed progressively and ultimately associated with an underlying "long-lived" ASC (LL ASC)-enriched transcriptional program. While some of the differences between LL ASCs and other ASCs appeared to be acquired with age, other features were shared with some younger ASCs, such as high CD138 and CD93. Turnover was unaffected by altered ASC production, arguing against competition for niches as a major driver of turnover. Thus, ASC turnover is set by intrinsic lifespan limits, with steady-state population dynamics governed by niche vacancy rather than displacement., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

37. B cell receptor ligation induces IgE plasma cell elimination.

Author

Wade-Vallance AK, Yang Z, Libang JB, Robinson MJ, Tarlinton DM, and Allen CDC

Subjects

Animals, Mice, Apoptosis, Cell Nucleus, Cell Survival, Immunosuppressive Agents, Receptors, Antigen, B-Cell immunology, Hypersensitivity, Plasma Cells

Abstract

The proper regulation of IgE production safeguards against allergic disease, highlighting the importance of mechanisms that restrict IgE plasma cell (PC) survival. IgE PCs have unusually high surface B cell receptor (BCR) expression, yet the functional consequences of ligating this receptor are unknown. Here, we found that BCR ligation induced BCR signaling in IgE PCs followed by their elimination. In cell culture, exposure of IgE PCs to cognate antigen or anti-BCR antibodies induced apoptosis. IgE PC depletion correlated with the affinity, avidity, amount, and duration of antigen exposure and required the BCR signalosome components Syk, BLNK, and PLCγ2. In mice with a PC-specific impairment of BCR signaling, the abundance of IgE PCs was selectively increased. Conversely, BCR ligation by injection of cognate antigen or anti-IgE depleted IgE PCs. These findings establish a mechanism for the elimination of IgE PCs through BCR ligation. This has important implications for allergen tolerance and immunotherapy as well as anti-IgE monoclonal antibody treatments., (© 2023 Wade-Vallance et al.)

Published

2023

38. Making sense of plasma cell heterogeneity.

Author

Tarlinton DM, Ding Z, Tellier J, and Nutt SL

Subjects

Humans, Vaccination, Lymph Nodes, Plasma Cells, Bone Marrow

Abstract

Plasma cells (PCs) are essential for the quality and longevity of protective immunity. The canonical humoral response to vaccination involves induction of germinal centers in lymph nodes followed by maintenance by bone marrow-resident PCs, although there are many variations of this theme. Recent studies have highlighted the importance of PCs in nonlymphoid organs, including the gut, central nervous system, and skin. These sites harbor PCs with distinct isotypes and possible immunoglobulin-independent functions. Indeed, bone marrow now appears unique in housing PCs derived from multiple other organs. The mechanisms through which the bone marrow maintains PC survival long-term and the impact of their diverse origins on this process remain very active areas of research., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

39. Long-lived plasma cells accumulate in the bone marrow at a constant rate from early in an immune response.

Author

Robinson MJ, Dowling MR, Pitt C, O'Donnell K, Webster RH, Hill DL, Ding Z, Dvorscek AR, Brodie EJ, Hodgkin PD, Quast I, and Tarlinton DM

Subjects

Animals, Mice, Germinal Center, Antibodies, Immunity, Plasma Cells, Bone Marrow

Abstract

Vaccines work largely by generating long-lived plasma cells (LLPCs), but knowledge of how such cells are recruited is sparse. Although it is clear that LLPCs preferentially originate in germinal centers (GCs) and relocate to survival niches in bone marrow where they can persist for decades, the issues of the timing of LLPC recruitment and the basis of their retention remain uncertain. Here, using a genetic timestamping system in mice, we show that persistent PCs accrue in bone marrow at an approximately constant rate of one cell per hour over a period spanning several weeks after a single immunization with a model antigen. Affinity-based selection was evident in persisting PCs, reflecting a relative and dynamic rather than absolute affinity threshold as evidenced by the changing pattern of V H gene somatic mutations conveying increased affinity for antigen. We conclude that the life span of persistent, antigen-specific PCs is in part intrinsic, preprogrammed, and varied and that their final number is related to the duration of the response in a predictable way. This implies that modulating vaccines to extend the duration of the GC reaction will enhance antibody-mediated protective immunity.

Published

2022

40. CD137L and CD4 T cells limit BCL6-expressing pre-germinal center B cell expansion and BCL6-driven B cell malignancy.

Author

Ding Z, Quast I, Yan F, Liao Y, Pitt C, O-Donnell K, Robinson MJ, Shi W, Kallies A, Zotos D, and Tarlinton DM

Subjects

Animals, CD4-Positive T-Lymphocytes metabolism, Germinal Center metabolism, Humans, Immunoglobulin Heavy Chains, Mice, Proto-Oncogene Proteins c-bcl-6 genetics, Proto-Oncogene Proteins c-bcl-6 metabolism, 4-1BB Ligand metabolism, Lymphoma, Large B-Cell, Diffuse genetics, Lymphoma, Large B-Cell, Diffuse metabolism, Lymphoma, Large B-Cell, Diffuse pathology

Abstract

Aberrant expression of the proto-oncogene BCL6 is a driver of tumorigenesis in diffuse large B cell lymphoma (DLBCL). Mice overexpressing BCL6 from the B cell-specific immunoglobulin heavy chain μ intron promoter (Iμ-Bcl6 Tg/+ ) develop B cell lymphomas with features typical of human DLBCL. While the development of B cell lymphoma in these mice is tightly controlled by T cells, the mechanisms of this immune surveillance are poorly understood. Here we show that CD4 T cells contribute to the control of lymphoproliferative disease in lymphoma-prone Iμ-Bcl6 Tg/+ mice. We reveal that this CD4 T cell immuno-surveillance requires signaling by the co-stimulatory molecule CD137 ligand (CD137L; also known as 4-1BBL), which may promote the transition of pre-malignant B cells with an activated phenotype into the germinal center stage via reverse signaling, preventing their hazardous accumulation. Thus, CD137L-mediated CD4 T cell immuno-surveillance adds another layer of protection against B cell malignancy to that provided by CD8 T cell cytotoxicity., (© 2022 The Authors. Immunology & Cell Biology published by John Wiley & Sons Australia, Ltd on behalf of Australian and New Zealand Society for Immunology, Inc.)

Published

2022

41. IL-21 has a critical role in establishing germinal centers by amplifying early B cell proliferation.

Author

Dvorscek AR, McKenzie CI, Robinson MJ, Ding Z, Pitt C, O'Donnell K, Zotos D, Brink R, Tarlinton DM, and Quast I

Subjects

Antigens, Cell Differentiation, Cell Proliferation, Interleukins, Germinal Center, T-Lymphocytes, Helper-Inducer metabolism

Abstract

The proliferation and differentiation of antigen-specific B cells, including the generation of germinal centers (GC), are prerequisites for long-lasting, antibody-mediated immune protection. Affinity for antigen determines B cell recruitment, proliferation, differentiation, and competitiveness in the response, largely through determining access to T cell help. However, how T cell-derived signals contribute to these outcomes is incompletely understood. Here, we report how the signature cytokine of follicular helper T cells, IL-21, acts as a key regulator of the initial B cell response by accelerating cell cycle progression and the rate of cycle entry, increasing their contribution to the ensuing GC. This effect occurs over a wide range of initial B cell receptor affinities and correlates with elevated AKT and S6 phosphorylation. Moreover, the resultant increased proliferation can explain the IL-21-mediated promotion of plasma cell differentiation. Collectively, our data establish that IL-21 acts from the outset of a T cell-dependent immune response to increase cell cycle progression and fuel cyclic re-entry of B cells, thereby regulating the initial GC size and early plasma cell output., (© 2022 The Authors. Published under the terms of the CC BY 4.0 license.)

Published

2022

42. Interleukin-21, acting beyond the immunological synapse, independently controls T follicular helper and germinal center B cells.

Author

Quast I, Dvorscek AR, Pattaroni C, Steiner TM, McKenzie CI, Pitt C, O'Donnell K, Ding Z, Hill DL, Brink R, Robinson MJ, Zotos D, and Tarlinton DM

Subjects

Cell Differentiation, Germinal Center, Interleukins, Immunological Synapses, T-Lymphocytes, Helper-Inducer

Abstract

Germinal centers (GCs), transient structures within B cell follicles and central to affinity maturation, require the coordinated behavior of T and B cells. IL-21, a pleiotropic T cell-derived cytokine, is key to GC biology through incompletely understood mechanisms. By genetically restricting production and receipt of IL-21 in vivo, we reveal how its independent actions on T and B cells combine to regulate the GC. IL-21 established the magnitude of the GC B cell response by promoting CD4 + T cell expansion and differentiation in a dose-dependent manner and with paracrine activity. Within GC, IL-21 specifically promoted B cell centroblast identity and, when bioavailability was high, plasma cell differentiation. Critically, these actions may occur irrespective of cognate T-B interactions, making IL-21 a general promoter of growth as distinct to a mediator of affinity-driven selection via synaptic delivery. This promiscuous activity of IL-21 explains the consequences of IL-21 deficiency on antibody-based immunity., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

43. Targeting BMI-1 in B cells restores effective humoral immune responses and controls chronic viral infection.

Author

Di Pietro A, Polmear J, Cooper L, Damelang T, Hussain T, Hailes L, O'Donnell K, Udupa V, Mi T, Preston S, Shtewe A, Hershberg U, Turner SJ, La Gruta NL, Chung AW, Tarlinton DM, Scharer CD, and Good-Jacobson KL

Subjects

Adaptive Immunity immunology, Animals, Antibodies, Neutralizing immunology, Antibodies, Viral immunology, Antibody Formation immunology, Female, Germinal Center immunology, Male, Mice, Mice, Inbred C57BL, B-Lymphocytes immunology, Immunity, Humoral immunology, Lymphocytic Choriomeningitis immunology, Lymphocytic choriomeningitis virus immunology, Polycomb Repressive Complex 1 immunology, Proto-Oncogene Proteins immunology

Abstract

Ineffective antibody-mediated responses are a key characteristic of chronic viral infection. However, our understanding of the intrinsic mechanisms that drive this dysregulation are unclear. Here, we identify that targeting the epigenetic modifier BMI-1 in mice improves humoral responses to chronic lymphocytic choriomeningitis virus. BMI-1 was upregulated by germinal center B cells in chronic viral infection, correlating with changes to the accessible chromatin landscape, compared to acute infection. B cell-intrinsic deletion of Bmi1 accelerated viral clearance, reduced splenomegaly and restored splenic architecture. Deletion of Bmi1 restored c-Myc expression in B cells, concomitant with improved quality of antibody and coupled with reduced antibody-secreting cell numbers. Specifically, BMI-1-deficiency induced antibody with increased neutralizing capacity and enhanced antibody-dependent effector function. Using a small molecule inhibitor to murine BMI-1, we could deplete antibody-secreting cells and prohibit detrimental immune complex formation in vivo. This study defines BMI-1 as a crucial immune modifier that controls antibody-mediated responses in chronic infection., (© 2021. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2022

44. The concerted change in the distribution of cell cycle phases and zone composition in germinal centers is regulated by IL-21.

Author

Zotos D, Quast I, Li-Wai-Suen CSN, McKenzie CI, Robinson MJ, Kan A, Smyth GK, Hodgkin PD, and Tarlinton DM

Subjects

Animals, Cell Proliferation, Interleukins genetics, Interleukins immunology, Mice, Inbred C57BL, Mice, Knockout, Mice, B-Lymphocytes cytology, B-Lymphocytes immunology, Cell Cycle, Cell Differentiation, Germinal Center immunology

Abstract

Humoral immune responses require germinal centres (GC) for antibody affinity maturation. Within GC, B cell proliferation and mutation are segregated from affinity-based positive selection in the dark zone (DZ) and light zone (LZ) substructures, respectively. While IL-21 is known to be important in affinity maturation and GC maintenance, here we show it is required for both establishing normal zone representation and preventing the accumulation of cells in the G1 cell cycle stage in the GC LZ. Cell cycle progression of DZ B cells is unaffected by IL-21 availability, as is the zone phenotype of the most highly proliferative GC B cells. Collectively, this study characterises the development of GC zones as a function of time and B cell proliferation and identifies IL-21 as an important regulator of these processes. These data help explain the requirement for IL-21 in normal antibody affinity maturation., (© 2021. The Author(s).)

Published

2021

45. Complement-in' the germinal center response.

Author

Robinson MJ, Quast I, and Tarlinton DM

Subjects

Germinal Center

Published

2021

46. Display of Native Antigen on cDC1 That Have Spatial Access to Both T and B Cells Underlies Efficient Humoral Vaccination.

Author

Kato Y, Steiner TM, Park HY, Hitchcock RO, Zaid A, Hor JL, Devi S, Davey GM, Vremec D, Tullett KM, Tan PS, Ahmet F, Mueller SN, Alonso S, Tarlinton DM, Ploegh HL, Kaisho T, Beattie L, Manton JH, Fernandez-Ruiz D, Shortman K, Lahoud MH, Heath WR, and Caminschi I

Subjects

Animals, Antigen Presentation, Autoantigens immunology, Autoantigens metabolism, Cell Differentiation, Cells, Cultured, Cytokines metabolism, Immunity, Humoral, Lectins, C-Type genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, Receptors, Immunologic genetics, Vaccination, B-Lymphocytes immunology, Dendritic Cells immunology, Lectins, C-Type metabolism, Receptors, Immunologic metabolism, Th1 Cells immunology, Th2 Cells immunology

Abstract

Follicular dendritic cells and macrophages have been strongly implicated in presentation of native Ag to B cells. This property has also occasionally been attributed to conventional dendritic cells (cDC) but is generally masked by their essential role in T cell priming. cDC can be divided into two main subsets, cDC1 and cDC2, with recent evidence suggesting that cDC2 are primarily responsible for initiating B cell and T follicular helper responses. This conclusion is, however, at odds with evidence that targeting Ag to Clec9A (DNGR1), expressed by cDC1, induces strong humoral responses. In this study, we reveal that murine cDC1 interact extensively with B cells at the border of B cell follicles and, when Ag is targeted to Clec9A, can display native Ag for B cell activation. This leads to efficient induction of humoral immunity. Our findings indicate that surface display of native Ag on cDC with access to both T and B cells is key to efficient humoral vaccination., (Copyright © 2020 by The American Association of Immunologists, Inc.)

Published

2020

47. How intrinsic and extrinsic regulators of plasma cell survival might intersect for durable humoral immunity.

Author

Robinson MJ, Webster RH, and Tarlinton DM

Subjects

Animals, Antibody Formation genetics, Antibody Formation immunology, Bone Marrow immunology, Bone Marrow metabolism, Cell Survival genetics, Cell Survival immunology, Cellular Microenvironment immunology, Humans, Immunity, Humoral, Immunologic Memory, Immunomodulation genetics, Plasma Cells immunology, Plasma Cells metabolism

Abstract

Plasma cells (PC) are key to protective immunity because they secrete antibodies. Surviving for periods ranging from days to decades in mammals, PC possess varying survival times that cannot be entirely stochastic or extrinsically set, as presumed half-lives vary with antigenic specificity. Here, we review the signals that impart survival potential to PC. These include signals provided during formation, and signals experienced once generated and embedded in the so-called long-lived niche. These signals all feed into survival by maintaining PC expression of MCL1, potentially synergistically with influences of other BCL2 family members. Herein, we propose that each formed PC has a capacity to respond to extrinsic cues that sets an upper maximum to its lifespan, but survival is also affected by variable availability of signals provided in BM survival niches. PC survival thus becomes a function of immunogen characteristics and niche anatomy, determined by the weighted survival benefit ascribed to each involved factor. Most factors, such as supporting cell types and secreted proteins, are predicted to influence survival times varying temporally by orders of magnitude, rather than absolute PC abundances measured at a single time, which may account for the variation in PC lifespan evident in the literature., (© 2020 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2020

48. Hhex regulates murine lymphoid progenitor survival independently of Stat5 and Cdkn2a.

Author

Jackson JT, O'Donnell K, Light A, Goh W, Huntington ND, Tarlinton DM, and McCormack MP

Subjects

Animals, Apoptosis genetics, Apoptosis immunology, Cell Survival genetics, Cell Survival immunology, Cyclin-Dependent Kinase Inhibitor p16 genetics, Homeodomain Proteins genetics, Lymphoid Progenitor Cells cytology, Mice, Mice, Knockout, Proto-Oncogene Proteins c-bcl-2 genetics, Proto-Oncogene Proteins c-bcl-2 immunology, STAT5 Transcription Factor genetics, Signal Transduction genetics, Transcription Factors genetics, Cyclin-Dependent Kinase Inhibitor p16 immunology, Homeodomain Proteins immunology, Lymphoid Progenitor Cells immunology, STAT5 Transcription Factor immunology, Signal Transduction immunology, Transcription Factors immunology

Abstract

The transcription factor Hhex (hematopoietically expressed homeobox gene) is critical for development of multiple lymphoid lineages beyond the common lymphoid progenitor. In addition, Hhex regulates hematopoietic stem cell (HSC) self-renewal, emergency hematopoiesis, and acute myeloid leukemia initiation and maintenance. Hhex mediates its effects on HSCs and acute myeloid leukemia stem cells via repression of the Cdkn2a tumor suppressor locus. However, we report here that loss of Cdkn2a does not rescue the failure of lymphoid development caused by loss of Hhex. As loss of Hhex causes apoptosis of lymphoid progenitors associated with impaired Bcl2 expression and defective Stat5b signaling, we tested the effects of rescuing these pathways using transgenic mice. Expression of the anti-apoptotic factor Bcl2, but not activated Stat5, rescued the development of T-, B-, and NK-cell lineages in the absence of Hhex. These results indicate that Bcl2 expression, but not Stat5b signaling or loss of Cdkn2a, can overcome the lymphoid deficiencies caused by the absence of Hhex, suggesting that the primary role of this transcription factor is to promote survival of lymphoid progenitors during early lymphoid development., (© 2020 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2020

49. An Erg-driven transcriptional program controls B cell lymphopoiesis.

Author

Ng AP, Coughlan HD, Hediyeh-Zadeh S, Behrens K, Johanson TM, Low MSY, Bell CC, Gilan O, Chan YC, Kueh AJ, Boudier T, Feltham R, Gabrielyan A, DiRago L, Hyland CD, Ierino H, Mifsud S, Viney E, Willson T, Dawson MA, Allan RS, Herold MJ, Rogers K, Tarlinton DM, Smyth GK, Davis MJ, Nutt SL, and Alexander WS

Subjects

Animals, B-Lymphocytes cytology, Cell Lineage genetics, Cells, Cultured, Gene Regulatory Networks genetics, Hematopoietic Stem Cells cytology, Mice, Inbred C57BL, Mice, Knockout, Oncogene Proteins metabolism, PAX5 Transcription Factor genetics, PAX5 Transcription Factor metabolism, Transcription Factors genetics, Transcription Factors metabolism, Transcriptional Regulator ERG metabolism, V(D)J Recombination genetics, B-Lymphocytes metabolism, Cell Differentiation genetics, Hematopoietic Stem Cells metabolism, Lymphopoiesis genetics, Oncogene Proteins genetics, Transcription, Genetic, Transcriptional Regulator ERG genetics

Abstract

B lymphoid development is initiated by the differentiation of hematopoietic stem cells into lineage committed progenitors, ultimately generating mature B cells. This highly regulated process generates clonal immunological diversity via recombination of immunoglobulin V, D and J gene segments. While several transcription factors that control B cell development and V(D)J recombination have been defined, how these processes are initiated and coordinated into a precise regulatory network remains poorly understood. Here, we show that the transcription factor ETS Related Gene (Erg) is essential for early B lymphoid differentiation. Erg initiates a transcriptional network involving the B cell lineage defining genes, Ebf1 and Pax5, which directly promotes expression of key genes involved in V(D)J recombination and formation of the B cell receptor. Complementation of Erg deficiency with a productively rearranged immunoglobulin gene rescued B lineage development, demonstrating that Erg is an essential and stage-specific regulator of the gene regulatory network controlling B lymphopoiesis.

Published

2020

50. The Amount of BCL6 in B Cells Shortly after Antigen Engagement Determines Their Representation in Subsequent Germinal Centers.

Author

Robinson MJ, Ding Z, Pitt C, Brodie EJ, Quast I, Tarlinton DM, and Zotos D

Subjects

Animals, Cell Proliferation, Lymphocyte Activation, Mice, Inbred C57BL, Phenotype, Spleen metabolism, Transcription Factors metabolism, Antigens metabolism, B-Lymphocytes metabolism, Germinal Center metabolism, Proto-Oncogene Proteins c-bcl-6 metabolism

Abstract

It is unknown whether the incremental increases in BCL6 amounts in antigen-activated B cells influence the unfolding differentiation before germinal center (GC) formation. By comparing shortly after immunization the distribution of conventional B cells to those enforced to express BCL6 at the upper quartile of normal and those lacking BCL6 altogether, we determined that B cell representation in the stages before the GC compartment was related to BCL6 amounts. This was not by increased proliferation or suppression of early plasmablast differentiation, but rather by preferential recruitment and progression through these early stages of B cell activation, culminating in preferential transition into GC. Once established, this bias was stable in GC over several weeks; other BCL6-regulated GC B cell behaviors were unaffected. We propose that setting BCL6 amounts very early in activated B cells will be central in determining clonal representation in the GC and thus memory populations., Competing Interests: Declaration of Interests The authors declare no competing interests., (Copyright © 2020 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2020