Your search keyword '"Good-Jacobson, KL"' showing total 63 results

1. Influenza virus infection history shapes antibody responses to influenza vaccination

Author

Auladell, M, Hoang, VMP, Le, TQM, Tseng, Y-Y, Carolan, L, Wilks, S, Pham, QT, Price, D, Nguyen, TD, Nguyen, LKH, Le, TT, Nguyen, THT, Tran, TKH, Nguyen, TND, Vu, TNB, Khvorov, A, Hensen, L, Tran, ND, Kedzierska, K, Dang, DA, Wertheim, H, Boyd, SD, Good-Jacobson, KL, Smith, D, Barr, I, Sullivan, S, van Doorn, HR, Fox, A, Auladell, M, Hoang, VMP, Le, TQM, Tseng, Y-Y, Carolan, L, Wilks, S, Pham, QT, Price, D, Nguyen, TD, Nguyen, LKH, Le, TT, Nguyen, THT, Tran, TKH, Nguyen, TND, Vu, TNB, Khvorov, A, Hensen, L, Tran, ND, Kedzierska, K, Dang, DA, Wertheim, H, Boyd, SD, Good-Jacobson, KL, Smith, D, Barr, I, Sullivan, S, van Doorn, HR, and Fox, A

Abstract

Studies of successive vaccination suggest that immunological memory against past influenza viruses may limit responses to vaccines containing current strains. The impact of memory induced by prior infection is rarely considered and is difficult to ascertain, because infections are often subclinical. This study investigated influenza vaccination among adults from the Ha Nam cohort (Vietnam), who were purposefully selected to include 72 with and 28 without documented influenza A(H3N2) infection during the preceding 9 years (Australian New Zealand Clinical Trials Registry 12621000110886). The primary outcome was the effect of prior influenza A(H3N2) infection on hemagglutinin-inhibiting antibody responses induced by a locally available influenza vaccine administered in November 2016. Baseline and postvaccination sera were titrated against 40 influenza A(H3N2) strains spanning 1968-2018. At each time point (baseline, day 14 and day 280), geometric mean antibody titers against 2008-2018 strains were higher among participants with recent infection (34 (29-40), 187 (154-227) and 86 (72-103)) than among participants without recent infection (19 (17-22), 91 (64-130) and 38 (30-49)). On days 14 and 280, mean titer rises against 2014-2018 strains were 6.1-fold (5.0- to 7.4-fold) and 2.6-fold (2.2- to 3.1-fold) for participants with recent infection versus 4.8-fold (3.5- to 6.7-fold) and 1.9-fold (1.5- to 2.3-fold) for those without. One of 72 vaccinees with recent infection versus 4 of 28 without developed symptomatic A(H3N2) infection in the season after vaccination (P = 0.021). The range of A(H3N2) viruses recognized by vaccine-induced antibodies was associated with the prior infection strain. These results suggest that recall of immunological memory induced by prior infection enhances antibody responses to inactivated influenza vaccine and is important to attain protective antibody titers.

Published

2022

2. JEM career launchpad

Author

Bigas, A, Zanoni, I, Hepworth, MR, Eisenbarth, SC, Masters, SL, Kipnis, J, Vinuesa, CG, Good-Jacobson, KL, Tangye, SG, Yamazaki, S, Hivroz, C, Wojno, ET, Shulman, Z, Colonna, M, Bigas, A, Zanoni, I, Hepworth, MR, Eisenbarth, SC, Masters, SL, Kipnis, J, Vinuesa, CG, Good-Jacobson, KL, Tangye, SG, Yamazaki, S, Hivroz, C, Wojno, ET, Shulman, Z, and Colonna, M

Abstract

JEM has been a launching pad for scientific careers since its inception. Here is a collection of testimonials attesting to the diversity of the scientific community it serves.

Published

2021

3. Metabolic characteristics of CD8+ T cell subsets in young and aged individuals are not predictive of functionality

Author

Quinn, KM, Hussain, T, Kraus, F, Formosa, LE, Lam, WK, Dagley, MJ, Saunders, EC, Assmus, LM, Wynne-Jones, E, Loh, L, van de Sandt, CE, Cooper, L, Good-Jacobson, KL, Kedzierska, K, Mackay, LK, McConville, MJ, Ramm, G, Ryan, MT, La Gruta, NL, Quinn, KM, Hussain, T, Kraus, F, Formosa, LE, Lam, WK, Dagley, MJ, Saunders, EC, Assmus, LM, Wynne-Jones, E, Loh, L, van de Sandt, CE, Cooper, L, Good-Jacobson, KL, Kedzierska, K, Mackay, LK, McConville, MJ, Ramm, G, Ryan, MT, and La Gruta, NL

Abstract

Virtual memory T (TVM) cells are antigen-naïve CD8+ T cells that exist in a semi-differentiated state and exhibit marked proliferative dysfunction in advanced age. High spare respiratory capacity (SRC) has been proposed as a defining metabolic characteristic of antigen-experienced memory T (TMEM) cells, facilitating rapid functionality and survival. Given the semi-differentiated state of TVM cells and their altered functionality with age, here we investigate TVM cell metabolism and its association with longevity and functionality. Elevated SRC is a feature of TVM, but not TMEM, cells and it increases with age in both subsets. The elevated SRC observed in aged mouse TVM cells and human CD8+ T cells from older individuals is associated with a heightened sensitivity to IL-15. We conclude that elevated SRC is a feature of TVM, but not TMEM, cells, is driven by physiological levels of IL-15, and is not indicative of enhanced functionality in CD8+ T cells.

Published

2020

4. Metabolic characteristics of CD8+ T cell subsets in young and aged individuals are not predictive of functionality (vol 11, 2857, 2020)

Author

Quinn, KM, Hussain, T, Kraus, F, Formosa, LE, Lam, WK, Dagley, MJ, Saunders, EC, Assmus, LM, Wynne-Jones, E, Loh, L, van de Sandt, CE, Cooper, L, Good-Jacobson, KL, Kedzierska, K, Mackay, LK, McConville, MJ, Ramm, G, Ryan, MT, La Gruta, NL, Quinn, KM, Hussain, T, Kraus, F, Formosa, LE, Lam, WK, Dagley, MJ, Saunders, EC, Assmus, LM, Wynne-Jones, E, Loh, L, van de Sandt, CE, Cooper, L, Good-Jacobson, KL, Kedzierska, K, Mackay, LK, McConville, MJ, Ramm, G, Ryan, MT, and La Gruta, NL

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2020

5. The Histone Methyltransferase DOT1L Is Essential for Humoral Immune Responses

Author

Kealy, L, Di Pietro, A, Hailes, L, Scheer, S, Dalit, L, Groom, JR, Zaph, C, Good-Jacobson, KL, Kealy, L, Di Pietro, A, Hailes, L, Scheer, S, Dalit, L, Groom, JR, Zaph, C, and Good-Jacobson, KL

Abstract

Histone modifiers are essential for the ability of immune cells to reprogram their gene expression during differentiation. The recruitment of the histone methyltransferase DOT1L (disruptor of telomeric silencing 1-like) induces oncogenic gene expression in a subset of B cell leukemias. Despite its importance, its role in the humoral immune system is unclear. Here, we demonstrate that DOT1L is a critical regulator of B cell biology. B cell development is defective in Dot1lf/fMb1Cre/+ mice, culminating in a reduction of peripheral mature B cells. Upon immunization or influenza infection of Dot1lf/fCd23Cre/+ mice, class-switched antibody-secreting cells are significantly attenuated and germinal centers fail to form. Consequently, DOT1L is essential for B cell memory formation. Transcriptome, pathway, and histological analyses identified a role for DOT1L in reprogramming gene expression for appropriate localization of B cells during the initial stage of the response. Together, these results demonstrate an essential role for DOT1L in generating an effective humoral immune response.

Published

2020

6. Context-Dependent Role for T-bet in T Follicular Helper Differentiation and Germinal Center Function following Viral Infection

Author

Sheikh, AA, Cooper, L, Feng, M, Souza-Fonseca-Guimaraes, F, Lafouresse, F, Duckworth, BC, Huntington, ND, Moon, JJ, Pellegrini, M, Nutt, SL, Belz, GT, Good-Jacobson, KL, Groom, JR, Sheikh, AA, Cooper, L, Feng, M, Souza-Fonseca-Guimaraes, F, Lafouresse, F, Duckworth, BC, Huntington, ND, Moon, JJ, Pellegrini, M, Nutt, SL, Belz, GT, Good-Jacobson, KL, and Groom, JR

Abstract

Following infection, inflammatory cues upregulate core transcriptional programs to establish pathogen-specific protection. In viral infections, T follicular helper (TFH) cells express the prototypical T helper 1 transcription factor T-bet. Several studies have demonstrated essential but conflicting roles for T-bet in TFH biology. Understanding the basis of this controversy is crucial, as modulation of T-bet expression instructs TFH differentiation and ultimately protective antibody responses. Comparing influenza and LCMV viral infections, we demonstrate that the role of T-bet is contingent on the environmental setting of TFH differentiation, IL-2 signaling, and T cell competition. Furthermore, we demonstrate that T-bet expression by either TFH or GC B cells independently drives antibody isotype class switching. Specifically, T cell-specific loss of T-bet promotes IgG1, whereas B cell-specific loss of T-bet inhibits IgG2a/c switching. Combined, this work highlights that the context-dependent induction of T-bet instructs the development of protective, neutralizing antibodies following viral infection or vaccination.

Published

2019

7. Type I interferon induces CXCL13 to support ectopic germinal center formation

Author

Denton, AE, Innocentin, S, Carr, EJ, Bradford, BM, Lafouresse, F, Mabbott, NA, Morbe, U, Ludewig, B, Groom, JR, Good-Jacobson, KL, Linterman, MA, Denton, AE, Innocentin, S, Carr, EJ, Bradford, BM, Lafouresse, F, Mabbott, NA, Morbe, U, Ludewig, B, Groom, JR, Good-Jacobson, KL, and Linterman, MA

Abstract

Ectopic lymphoid structures form in a wide range of inflammatory conditions, including infection, autoimmune disease, and cancer. In the context of infection, this response can be beneficial for the host: influenza A virus infection-induced pulmonary ectopic germinal centers give rise to more broadly cross-reactive antibody responses, thereby generating cross-strain protection. However, despite the ubiquity of ectopic lymphoid structures and their role in both health and disease, little is known about the mechanisms by which inflammation is able to convert a peripheral tissue into one that resembles a secondary lymphoid organ. Here, we show that type I IFN produced after viral infection can induce CXCL13 expression in a phenotypically distinct population of lung fibroblasts, driving CXCR5-dependent recruitment of B cells and initiating ectopic germinal center formation. This identifies type I IFN as a novel inducer of CXCL13, which, in combination with other stimuli, can promote lung remodeling, converting a nonlymphoid tissue into one permissive to functional tertiary lymphoid structure formation.

Published

2019

8. Tailoring Immune Responses toward Autoimmunity: Transcriptional Regulators That Drive the Creation and Collusion of Autoreactive Lymphocytes

Author

Good-Jacobson, KL, Groom, JR, Good-Jacobson, KL, and Groom, JR

Abstract

T-dependent humoral immune responses to infection involve a collaboration between B and CD4 T cell activation, migration, and co-stimulation, thereby culminating in the formation of germinal centers (GCs) and eventual differentiation into memory cells and long-lived plasma cells (PCs). CD4 T cell-derived signals drive the formation of a tailored B cell response. Downstream of these signals are transcriptional regulators that are the critical enactors of immune cell programs. In particular, a core group of transcription factors regulate both B and T cell differentiation, identity, and function. The timing and expression levels of these transcription factors are tightly controlled, with dysregulated expression correlated to immune cell dysfunction in autoimmunity and lymphomagenesis. Recent studies have significantly advanced our understanding of both extrinsic and intrinsic regulators of autoreactive B cells and antibody-secreting PCs in systemic lupus erythematosus, rheumatoid arthritis, and other autoimmune conditions. Yet, there are still gaps in our understanding of the causative role these regulators play, as well as the link between lymphoid responses and peripheral damage. This review will focus on the genesis of immunopathogenic CD4 helper and GC B cells. In particular, we will detail the transcriptional regulation of cytokine and chemokine receptor signaling during the pathogenesis of GC-derived autoimmune conditions in both murine models and human patients.

Published

2018

9. Assessing the role of the T-box transcription factor Eomes in B cell differentiation during either Th1 or Th2 cell-biased responses

Author

Winslow, GM, Cooper, L, Hailes, L, Sheikh, A, Zaph, C, Belz, GT, Groom, JR, Good-Jacobson, KL, Winslow, GM, Cooper, L, Hailes, L, Sheikh, A, Zaph, C, Belz, GT, Groom, JR, and Good-Jacobson, KL

Abstract

Successful T-dependent humoral responses require the production of antibody-secreting plasmablasts, as well as the formation of germinal centers which eventually form high-affinity B cell memory. The ability of B cells to differentiate into germinal center and plasma cells, as well as the ability to tailor responses to different pathogens, is driven by transcription factors. In T cells, the T-box transcription factors T-bet and Eomesodermin (Eomes) regulate effector and memory T cell differentiation, respectively. While T-bet has a critical role in regulating anti-viral B cell responses, a role for Eomes in B cells has yet to be described. We therefore investigated whether Eomes was required for B cell differentiation during either Th1 or Th2 cell-biased immune responses. Here, we demonstrate that deletion of Eomes specifically in B cells did not affect B cell differentiation in response to vaccination, as well as following viral or helminth infection. In contrast to its established role in CD8+ T cells, Eomes did not influence memory B cell differentiation. Finally, the use of an Eomes reporter mouse confirmed the lack of Eomes expression during immune responses. Thus, germinal center and plasma cell differentiation and the formation of isotype-switched memory B cells in response to infection are independent of Eomes expression.

Published

2018

10. 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

11. Regulation of germinal center, B-cell memory, and plasma cell formation by histone modifiers

Author

Good-Jacobson, KL and Good-Jacobson, KL

Abstract

Understanding the regulation of antibody production and B-cell memory formation and function is core to finding new treatments for B-cell-derived cancers, antibody-mediated autoimmune disorders, and immunodeficiencies. Progression from a small number of antigen-specific B-cells to the production of a large number of antibody-secreting cells is tightly regulated. Although much progress has been made in revealing the transcriptional regulation of B-cell differentiation that occurs during humoral immune responses, there are still many questions that remain unanswered. Recent work on the expression and roles of histone modifiers in lymphocytes has begun to shed light on this additional level of regulation. This review will discuss the recent advancements in understanding how humoral immune responses, in particular germinal centers and memory cells, are modulated by histone modifiers.

Published

2014

12. CD80 and PD-L2 define functionally distinct memory B cell subsets that are independent of antibody isotype.

Author

Zuccarino-Catania, GV, Sadanand, S, Weisel, FJ, Tomayko, MM, Meng, H, Kleinstein, SH, Good-Jacobson, KL, Shlomchik, MJ, Zuccarino-Catania, GV, Sadanand, S, Weisel, FJ, Tomayko, MM, Meng, H, Kleinstein, SH, Good-Jacobson, KL, and Shlomchik, MJ

Abstract

Memory B cells (MBCs) are long-lived sources of rapid, isotype-switched secondary antibody-forming cell (AFC) responses. Whether MBCs homogeneously retain the ability to self-renew and terminally differentiate or if these functions are compartmentalized into MBC subsets has remained unclear. It has been suggested that antibody isotype controls MBC differentiation upon restimulation. Here we demonstrate that subcategorizing MBCs on the basis of their expression of CD80 and PD-L2, independently of isotype, identified MBC subsets with distinct functions upon rechallenge. CD80(+)PD-L2(+) MBCs differentiated rapidly into AFCs but did not generate germinal centers (GCs); conversely, CD80(-)PD-L2(-) MBCs generated few early AFCs but robustly seeded GCs. The gene-expression patterns of the subsets supported both the identity and function of these distinct MBC types. Hence, the differentiation and regeneration of MBCs are compartmentalized.

Published

2014

13. PD-1 regulates germinal center B cell survival and the formation and affinity of long-lived plasma cells.

Author

Good-Jacobson, KL, Szumilas, CG, Chen, L, Sharpe, AH, Tomayko, MM, Shlomchik, MJ, Good-Jacobson, KL, Szumilas, CG, Chen, L, Sharpe, AH, Tomayko, MM, and Shlomchik, MJ

Abstract

Memory B and plasma cells (PCs) are generated in the germinal center (GC). Because follicular helper T cells (T(FH) cells) have high expression of the immunoinhibitory receptor PD-1, we investigated the role of PD-1 signaling in the humoral response. We found that the PD-1 ligands PD-L1 and PD-L2 were upregulated on GC B cells. Mice deficient in PD-L2 (Pdcd1lg2(-/-)), PD-L1 and PD-L2 (Cd274(-/-)Pdcd1lg2(-/-)) or PD-1 (Pdcd1(-/-)) had fewer long-lived PCs. The mechanism involved more GC cell death and less T(FH) cell cytokine production in the absence of PD-1; the effect was selective, as remaining PCs had greater affinity for antigen. PD-1 expression on T cells and PD-L2 expression on B cells controlled T(FH) cell and PC numbers. Thus, PD-1 regulates selection and survival in the GC, affecting the quantity and quality of long-lived PCs.

Published

2010

14. 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

15. Type I interferons induce an epigenetically distinct memory B cell subset in chronic viral infection.

Author

Cooper L, Xu H, Polmear J, Kealy L, Szeto C, Pang ES, Gupta M, Kirn A, Taylor JJ, Jackson KJL, Broomfield BJ, Nguyen A, Gago da Graça C, La Gruta N, Utzschneider DT, Groom JR, Martelotto L, Parish IA, O'Keeffe M, Scharer CD, Gras S, and Good-Jacobson KL

Subjects

Animals, Mice, Mice, Inbred C57BL, Receptor, Interferon alpha-beta genetics, Immunologic Memory immunology, Chronic Disease, B-Lymphocyte Subsets immunology, Single-Cell Analysis, Interferon Type I metabolism, Interferon Type I immunology, Lymphocytic Choriomeningitis immunology, Lymphocytic Choriomeningitis virology, Lymphocytic choriomeningitis virus immunology, Memory B Cells immunology, Epigenesis, Genetic

Abstract

Memory B cells (MBCs) are key providers of long-lived immunity against infectious disease, yet in chronic viral infection, they do not produce effective protection. How chronic viral infection disrupts MBC development and whether such changes are reversible remain unknown. Through single-cell (sc)ATAC-seq and scRNA-seq during acute versus chronic lymphocytic choriomeningitis viral infection, we identified a memory subset enriched for interferon (IFN)-stimulated genes (ISGs) during chronic infection that was distinct from the T-bet + subset normally associated with chronic infection. Blockade of IFNAR-1 early in infection transformed the chromatin landscape of chronic MBCs, decreasing accessibility at ISG-inducing transcription factor binding motifs and inducing phenotypic changes in the dominating MBC subset, with a decrease in the ISG subset and an increase in CD11c + CD80 + cells. However, timing was critical, with MBCs resistant to intervention at 4 weeks post-infection. Together, our research identifies a key mechanism to instruct MBC identity during viral infection., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

16. A Touch of Immunology: improving accessibility to the science of antibodies for people with blindness, low vision and diverse needs.

Author

Polmear J, Kealy L, Xu H, and Good-Jacobson KL

Subjects

Animals, Humans, Allergy and Immunology, Antibodies immunology, Autoimmune Diseases immunology, Autoimmunity, Blindness immunology, Vision, Low immunology

Abstract

Immunology for all: Most scientific communication has historically been limited to visual imagery and the written or spoken word, often in the form of dense articles obscured by jargon. Clear communication of science is vital to enable the public to engage with important scientific discoveries and to limit medical distrust. However, scientific communication is often executed in a way which neglects people with blindness, low vision and diverse needs. Our aim for the exhibit at the Monash Sensory Science Exhibition on Autoimmunity 2023 at Monash University was to develop novel, tactile and informative models to help better communicate the scientific principles that underpin autoimmune disease and immunology. As B-cell biologists, we decided to focus our exhibit for this workshop on antibody-mediated autoimmunity. Antibodies are key components of the immune system, providing protection against a range of diverse pathogens. However, in the context of autoimmunity, they can also drive pathology., (© 2023 The Authors. Immunology & Cell Biology published by John Wiley & Sons Australia, Ltd on behalf of the Australian and New Zealand Society for Immunology, Inc.)

Published

2024

17. Visualizing Epigenetic Modifications and Nuclear Bodies by Immunofluorescence Staining in Naïve, Activated, and Memory B Cell Subsets.

Author

Chakma CR, Garvie A, Wong LH, and Good-Jacobson KL

Subjects

Animals, Mice, Humans, Cell Nucleus metabolism, B-Lymphocyte Subsets metabolism, B-Lymphocyte Subsets immunology, Immunologic Memory, Microscopy, Fluorescence methods, Histones metabolism, Lymphocyte Activation, Staining and Labeling methods, Fluorescent Antibody Technique methods, Epigenesis, Genetic

Abstract

Immunofluorescence microscopy is a powerful technique using fluorescently labelled antibodies which can be used to visualize proteins in the nucleus. A key advantage of this method is that it can provide insight into the spatial organization and the localization of nuclear proteins, which can provide elucidation of their function. Here, we provide a protocol for immunofluorescence staining in the nucleus, which has successfully been used to visualize histone modifications and nuclear bodies in human and mouse B lymphocytes, using as few as 1 × 10 4 -5 × 10 4 cells., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

18. Assessing the Survival of Human Plasma Cells Ex Vivo.

Author

Polmear J, Fletcher AL, and Good-Jacobson KL

Subjects

Humans, Cell Culture Techniques methods, Cells, Cultured, Flow Cytometry methods, Plasma Cells immunology, Plasma Cells cytology, Plasma Cells drug effects, Cell Survival drug effects

Abstract

One way memory B cells provide protection is by rapidly differentiating into plasma cells. Plasma cells are vital in providing long-term protection against pathogens; however, they can also be detrimental to health in the case of antibody-mediated autoimmunity. Therefore, compounds which modulate the survival of plasma cells have been of interest for therapeutic intervention. Investigation of ex vivo plasma cell survival has previously been limited by the low frequency of plasma cells in the blood. Here we describe a novel ex vivo culture system that only requires 3000-5000 cells per condition. This method permits the assessment of human plasma cell survival derived from blood and can assess the impact of small molecule inhibitors on plasma cell viability., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

19. Detection of Lymphocytic Choriomeningitis Virus-Specific Memory B Cells Using Antigen Tetramers.

Author

Cooper L, Szeto C, Jayasinghe D, Taylor JJ, Gras S, and Good-Jacobson KL

Subjects

Animals, Mice, Immunologic Memory, B-Lymphocytes immunology, B-Lymphocytes metabolism, Lymphocytic choriomeningitis virus immunology, Lymphocytic Choriomeningitis immunology, Lymphocytic Choriomeningitis virology, Flow Cytometry methods, Antigens, Viral immunology, Memory B Cells immunology, Memory B Cells metabolism

Abstract

Memory B cells are central to the establishment of immunological memory, providing long-term protection against specific pathogens and playing a vital role in the efficacy of vaccines. Understanding how memory B cell formation is disrupted during persistent infection is essential for new therapeutics. Lymphocytic choriomeningitis virus (LCMV) is an ideal model for investigating memory B cells in acute versus chronic infection. This protocol details techniques to isolate, enrich, and examine LCMV-specific memory B cells in both acute and chronic LCMV infection. Using an antigen tetramer enrichment system and flow cytometry, this method assesses low-frequency, polyclonal antigen-specific memory B cells., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

20. Targeting BMI-1 to deplete antibody-secreting cells in autoimmunity.

Author

Polmear J, Hailes L, Olshansky M, Rischmueller M, L'Estrange-Stranieri E, Fletcher AL, Hibbs ML, Bryant VL, and Good-Jacobson KL

Abstract

Objectives: B cells drive the production of autoreactive antibody-secreting cells (ASCs) in autoimmune diseases such as Systemic Lupus Erythematosus (SLE) and Sjögren's syndrome, causing long-term organ damage. Current treatments for antibody-mediated autoimmune diseases target B cells or broadly suppress the immune system. However, pre-existing long-lived ASCs are often refractory to treatment, leaving a reservoir of autoreactive cells that continue to produce antibodies. Therefore, the development of novel treatment methods targeting ASCs is vital to improve patient outcomes. Our objective was to test whether targeting the epigenetic regulator BMI-1 could deplete ASCs in autoimmune conditions in vivo and in vitro ., Methods: Use of a BMI-1 inhibitor in both mouse and human autoimmune settings was investigated. Lyn -/- mice, a model of SLE, were treated with the BMI-1 small molecule inhibitor PTC-028, before assessment of ASCs, serum antibody and immune complexes. To examine human ASC survival, a novel human fibroblast-based assay was established, and the impact of PTC-028 on ASCs derived from Sjögren's syndrome patients was evaluated., Results: BMI-1 inhibition significantly decreased splenic and bone marrow ASCs in Lyn -/- mice. The decline in ASCs was linked to aberrant cell cycle gene expression and led to a significant decrease in serum IgG3, immune complexes and anti-DNA IgG. PTC-028 was also efficacious in reducing ex vivo plasma cell survival from both Sjögren's syndrome patients and age-matched healthy donors., Conclusion: These data provide evidence that inhibiting BMI-1 can deplete ASC in a variety of contexts and thus BMI-1 is a viable therapeutic target for antibody-mediated autoimmune diseases., Competing Interests: This study was supported in part by a GSK Fast Track Discovery Grant to KLG‐J. MR has received research funding for autoimmunity‐related clinical trials from BMS, Novartis, Servier Amgen and Astra Zeneca., (© 2023 The Authors. Clinical & Translational Immunology published by John Wiley & Sons Australia, Ltd on behalf of Australian and New Zealand Society for Immunology, Inc.)

Published

2023

21. Heterogeneous Tfh cell populations that develop during enteric helminth infection predict the quality of type 2 protective response.

Author

Zaini A, Dalit L, Sheikh AA, Zhang Y, Thiele D, Runting J, Rodrigues G, Ng J, Bramhall M, Scheer S, Hailes L, Groom JR, Good-Jacobson KL, and Zaph C

Abstract

T follicular helper (Tfh) cells are an important component of germinal center (GC)-mediated humoral immunity. Yet, how a chronic type 1 versus protective type 2 helminth infection modulates Tfh-GC responses remains poorly understood. Here, we employ the helminth Trichuris muris model and demonstrate that Tfh cell phenotypes and GC are differentially regulated in acute versus chronic infection. The latter failed to induce Tfh-GC B cell responses, with Tfh cells expressing Τ-bet and interferon-γ. In contrast, interleukin-4-producing Tfh cells dominate responses to an acute, resolving infection. Heightened expression and increased chromatin accessibility of T helper (Th)1- and Th2 cell-associated genes are observed in chronic and acute induced Tfh cells, respectively. Blockade of the Th1 cell response by T-cell-intrinsic T-bet deletion promoted Tfh cell expansion during chronic infection, pointing to a correlation between a robust Tfh cell response and protective immunity to parasites. Finally, blockade of Tfh-GC interactions impaired type 2 immunity, revealing the critical protective role of GC-dependent Th2-like Tfh cell responses during acute infection. Collectively, these results provide new insights into the protective roles of Tfh-GC responses and identify distinct transcriptional and epigenetic features of Tfh cells that emerge during resolving or chronic T. muris infection., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

22. New fibroblast network connections support lymphocytic cellular service.

Author

Fletcher AL and Good-Jacobson KL

Subjects

Lymphocytes, Brain

Published

2023

23. Requirements of IL-4 during the Generation of B Cell Memory.

Author

Chakma CR and Good-Jacobson KL

Subjects

B-Lymphocytes, Cell Differentiation, Germinal Center, Immunoglobulin Class Switching, Immunoglobulin Isotypes, Humans, Animals, Interleukin-4, Memory B Cells

Abstract

IL-4 has long been established as a key regulator of Th cells and for promoting effective B cell survival and isotype class switching. Yet, despite having been extensively studied, the specific role of IL-4 in generating humoral memory in vivo is unclear. In this review, we explore the recent studies that unravel the cellular sources and spatiotemporal production of IL-4, the relationship between IL-4 and IL-21 during germinal center responses and the formation of Ab-secreting cells, and the current understanding of whether IL-4 promotes or suppresses memory B cell generation in vitro and in vivo., (Copyright © 2023 by The American Association of Immunologists, Inc.)

Published

2023

24. Immunology at Monash University, Melbourne: celebrating 60 years of the Department of Immunology.

Author

Good-Jacobson KL

Subjects

Male, Humans, History, 20th Century, Australia, Universities

Abstract

Professor David Tarlinton is the Head of Department of Immunology, Monash University in Melbourne, Australia. His career has spanned research in the United States, Germany and Australia. As his department prepares to celebrate its 60th anniversary, he talks with Professor Kim Good-Jacobson about immunology in Melbourne, his career and advice for the next generation of researchers., (© 2023 the Australian and New Zealand Society for Immunology, Inc.)

Published

2023

25. Severe acute respiratory syndrome coronavirus-2 vaccine-induced B cells aspire to long-lived connections: Tracking B-cell memory over time.

Author

Kealy L and Good-Jacobson KL

Subjects

Antibodies, Viral, B-Lymphocytes, BNT162 Vaccine, COVID-19 Vaccines, Humans, COVID-19, SARS-CoV-2

Abstract

It is vitally important that we understand whether mRNA vaccines are capable of generating high-affinity, longlived immune memory cells to SARS-CoV-2. To this end, a recent study by Ellebedy, Kim and colleagues provide much-needed insight into the production and quality of humoral immune cells generated by the BNT162b2 vaccine., (© 2022 Australian and New Zealand Society for Immunology Inc.)

Published

2022

26. Editorial overview: Collaboration in the immune system.

Author

Good-Jacobson KL and Groom JR

Subjects

Humans, Immune System

Published

2022

27. Antibody glycosylation directs innate and adaptive immune collaboration.

Author

Polmear J and Good-Jacobson KL

Subjects

Glycosylation, Humans, Immunity, Innate, Antibodies, Neutralizing, Polysaccharides

Abstract

Neutralizing antibody is fundamental for the effective clearance of many pathogens. In addition, non-neutralizing antibody functions have rapidly gained prominence. The N-glycan structure of antibody can help direct appropriate innate cell effector functions. Thus, dynamic communication between innate and adaptive arms via antibody glycosylation can be crucial for modulating between pro-inflammatory or anti-inflammatory responses. Antibody N-glycan profiles are increasingly used as biomarkers to distinguish between disease states and severity. Emerging evidence suggests that aberrant glycan profiles may impede effective immune responses, but whether they are a consequence or cause of pathology remains unclear. Untangling the role of antibody glycan profiles in pathogenesis and how they are modulated by the microenvironment will expand our ability to assess and modify disease outcomes., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2022

28. Influenza virus infection history shapes antibody responses to influenza vaccination.

Author

Auladell M, Phuong HVM, Mai LTQ, Tseng YY, Carolan L, Wilks S, Thai PQ, Price D, Duong NT, Hang NLK, Thanh LT, Thuong NTH, Huong TTK, Diep NTN, Bich VTN, Khvorov A, Hensen L, Duong TN, Kedzierska K, Anh DD, Wertheim H, Boyd SD, Good-Jacobson KL, Smith D, Barr I, Sullivan S, van Doorn HR, and Fox A

Subjects

Adult, Antibodies, Viral, Antibody Formation, Australia, Hemagglutination Inhibition Tests, Humans, Influenza A Virus, H3N2 Subtype, Vaccination, Vaccines, Inactivated, Influenza Vaccines, Influenza, Human prevention & control

Abstract

Studies of successive vaccination suggest that immunological memory against past influenza viruses may limit responses to vaccines containing current strains. The impact of memory induced by prior infection is rarely considered and is difficult to ascertain, because infections are often subclinical. This study investigated influenza vaccination among adults from the Ha Nam cohort (Vietnam), who were purposefully selected to include 72 with and 28 without documented influenza A(H3N2) infection during the preceding 9 years (Australian New Zealand Clinical Trials Registry 12621000110886). The primary outcome was the effect of prior influenza A(H3N2) infection on hemagglutinin-inhibiting antibody responses induced by a locally available influenza vaccine administered in November 2016. Baseline and postvaccination sera were titrated against 40 influenza A(H3N2) strains spanning 1968-2018. At each time point (baseline, day 14 and day 280), geometric mean antibody titers against 2008-2018 strains were higher among participants with recent infection (34 (29-40), 187 (154-227) and 86 (72-103)) than among participants without recent infection (19 (17-22), 91 (64-130) and 38 (30-49)). On days 14 and 280, mean titer rises against 2014-2018 strains were 6.1-fold (5.0- to 7.4-fold) and 2.6-fold (2.2- to 3.1-fold) for participants with recent infection versus 4.8-fold (3.5- to 6.7-fold) and 1.9-fold (1.5- to 2.3-fold) for those without. One of 72 vaccinees with recent infection versus 4 of 28 without developed symptomatic A(H3N2) infection in the season after vaccination (P = 0.021). The range of A(H3N2) viruses recognized by vaccine-induced antibodies was associated with the prior infection strain. These results suggest that recall of immunological memory induced by prior infection enhances antibody responses to inactivated influenza vaccine and is important to attain protective antibody titers., (© 2022. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2022

29. 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

30. Engraving our first B cell memories into the repertoire.

Author

Good-Jacobson KL

Subjects

Animals, Antibody Formation, B-Lymphocytes, Germinal Center, Humans, Immunologic Memory, Memory B Cells, Mice, B-Lymphocyte Subsets, Engraving and Engravings

Abstract

Memory B cells are central to effective protection against reinfection. Glaros et al. used single-cell techniques to illuminate how activated mouse B cells are diverted into forming memory cells a few days post-immunogenic exposure. Early memory subsets contribute to a crucial goal: building a diverse and agile humoral defense system., Competing Interests: Declaration of interests The author declares that there are no conflicts of interest, or copyright permissions required., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

31. Advances in understanding the formation and fate of B-cell memory in response to immunization or infection.

Author

Kealy L and Good-Jacobson KL

Abstract

Immunological memory has the potential to provide lifelong protection against recurrent infections. As such, it has been crucial to the success of vaccines. Yet, the recent pandemic has illuminated key gaps in our knowledge related to the factors influencing effective memory formation and the inability to predict the longevity of immune protection. In recent decades, researchers have acquired a number of novel and powerful tools with which to study the factors underpinning humoral memory. These tools have been used to study the B-cell fate decisions that occur within the germinal centre (GC), a site where responding B cells undergo affinity maturation and are one of the major routes for memory B cell and high-affinity long-lived plasma cell formation. The advent of single-cell sequencing technology has provided an enhanced resolution for studying fate decisions within the GC and cutting-edge techniques have enabled researchers to model this reaction with more accuracy both in vitro and in silico . Moreover, modern approaches to studying memory B cells have allowed us to gain a better appreciation for the heterogeneity and adaptability of this vital class of B cells. Together, these studies have facilitated important breakthroughs in our understanding of how these systems operate to ensure a successful immune response. In this review, we describe recent advances in the field of GC and memory B-cell biology in order to provide insight into how humoral memory is formed, as well as the potential for generating lasting immunity to novel pathogens such as severe acute respiratory syndrome coronavirus 2., (© The Author(s) 2021. Published by Oxford University Press.)

Published

2021

32. Homeostatic apoptosis prevents competition-induced atrophy in follicular B cells.

Author

Chappaz S, McArthur K, Kealy L, Law CW, Tailler M, Lane RM, Lieschke A, Ritchie ME, Good-Jacobson KL, Strasser A, and Kile BT

Subjects

Animals, Antibody Formation immunology, Atrophy, B-Cell Activating Factor metabolism, Cell Count, Cell Differentiation genetics, Cell Proliferation genetics, Cell Size, Cell Survival genetics, Cellular Senescence genetics, Gene Deletion, Gene Expression Regulation, Mice, Knockout, Sequence Analysis, RNA, Thymus Gland immunology, Transcription Factors metabolism, bcl-2 Homologous Antagonist-Killer Protein metabolism, bcl-2-Associated X Protein metabolism, Mice, Apoptosis, B-Lymphocytes pathology, Homeostasis

Abstract

While the intrinsic apoptosis pathway is thought to play a central role in shaping the B cell lineage, its precise role in mature B cell homeostasis remains elusive. Using mice in which mature B cells are unable to undergo apoptotic cell death, we show that apoptosis constrains follicular B (FoB) cell lifespan but plays no role in marginal zone B (MZB) cell homeostasis. In these mice, FoB cells accumulate abnormally. This intensifies intercellular competition for BAFF, resulting in a contraction of the MZB cell compartment, and reducing the growth, trafficking, and fitness of FoB cells. Diminished BAFF signaling dampens the non-canonical NF-κB pathway, undermining FoB cell growth despite the concurrent triggering of a protective p53 response. Thus, MZB and FoB cells exhibit a differential requirement for the intrinsic apoptosis pathway. Homeostatic apoptosis constrains the size of the FoB cell compartment, thereby preventing competition-induced FoB cell atrophy., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2021

33. Context-dependent roles of B cells during intestinal helminth infection.

Author

Zaini A, Good-Jacobson KL, and Zaph C

Subjects

Animals, Anthelmintics therapeutic use, Germinal Center immunology, Helminthiasis drug therapy, Helminthiasis parasitology, Helminths drug effects, Humans, Intestinal Diseases, Parasitic drug therapy, Intestinal Diseases, Parasitic parasitology, Mice, Protozoan Vaccines immunology, Reinfection parasitology, Reinfection prevention & control, T-Lymphocytes, Helper-Inducer immunology, Antibodies, Helminth immunology, B-Lymphocytes immunology, Helminthiasis immunology, Helminths immunology, Intestinal Diseases, Parasitic immunology

Abstract

The current approaches to reduce the burden of chronic helminth infections in endemic areas are adequate sanitation and periodic administration of deworming drugs. Yet, resistance against some deworming drugs and reinfection can still rapidly occur even after treatment. A vaccine against helminths would be an effective solution at preventing reinfection. However, vaccines against helminth parasites have yet to be successfully developed. While T helper cells and innate lymphoid cells have been established as important components of the protective type 2 response, the roles of B cells and antibodies remain the most controversial. Here, we review the roles of B cells during intestinal helminth infection. We discuss the potential factors that contribute to the context-specific roles for B cells in protection against diverse intestinal helminth parasite species, using evidence from well-defined murine model systems. Understanding the precise roles of B cells during resistance and susceptibility to helminth infection may offer a new perspective of type 2 protective immunity., Competing Interests: The authors have declared that no competing interests exist.

Published

2021

34. JEM career launchpad.

Author

Bigas A, Zanoni I, Hepworth MR, Eisenbarth SC, Masters SL, Kipnis J, Vinuesa CG, Good-Jacobson KL, Tangye SG, Yamazaki S, Hivroz C, Tait Wojno E, Shulman Z, and Colonna M

Subjects

Humans, Publications, Laboratory Personnel organization & administration, Publishing organization & administration

Published

2021

35. The Histone Methyltransferase DOT1L Is Essential for Humoral Immune Responses.

Author

Kealy L, Di Pietro A, Hailes L, Scheer S, Dalit L, Groom JR, Zaph C, and Good-Jacobson KL

Subjects

Animals, Disease Models, Animal, Humans, Mice, Histone-Lysine N-Methyltransferase immunology, Immunity, Humoral immunology, Methyltransferases immunology

Abstract

Histone modifiers are essential for the ability of immune cells to reprogram their gene expression during differentiation. The recruitment of the histone methyltransferase DOT1L (disruptor of telomeric silencing 1-like) induces oncogenic gene expression in a subset of B cell leukemias. Despite its importance, its role in the humoral immune system is unclear. Here, we demonstrate that DOT1L is a critical regulator of B cell biology. B cell development is defective in Dot1l f/f Mb1 Cre/+ mice, culminating in a reduction of peripheral mature B cells. Upon immunization or influenza infection of Dot1l f/f Cd23 Cre/+ mice, class-switched antibody-secreting cells are significantly attenuated and germinal centers fail to form. Consequently, DOT1L is essential for B cell memory formation. Transcriptome, pathway, and histological analyses identified a role for DOT1L in reprogramming gene expression for appropriate localization of B cells during the initial stage of the response. Together, these results demonstrate an essential role for DOT1L in generating an effective humoral immune response., 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

36. Hhex drives B cells down memory lane.

Author

Good-Jacobson KL and Groom JR

Subjects

B-Lymphocytes metabolism, Co-Repressor Proteins, Gene Expression Regulation, Homeodomain Proteins genetics, Transcription Factors genetics

Published

2020

37. Publisher Correction: Metabolic characteristics of CD8 + T cell subsets in young and aged individuals are not predictive of functionality.

Author

Quinn KM, Hussain T, Kraus F, Formosa LE, Lam WK, Dagley MJ, Saunders EC, Assmus LM, Wynne-Jones E, Loh L, van de Sandt CE, Cooper L, Good-Jacobson KL, Kedzierska K, Mackay LK, McConville MJ, Ramm G, Ryan MT, and La Gruta NL

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2020

38. Dysregulation of humoral immunity in chronic infection.

Author

Cooper L and Good-Jacobson KL

Subjects

Antibodies, Neutralizing immunology, Chronic Disease, Germinal Center immunology, Humans, Vaccines, Viral Load, B-Lymphocytes immunology, Immunity, Humoral, Immunologic Memory, Virus Diseases immunology

Abstract

Chronic viral infections disrupt the ability of the humoral immune response to produce neutralizing antibody or form effective immune memory, preventing viral clearance and making vaccine design difficult. Multiple components of the B-cell response are affected by pathogens that are not cleared from the host. Changes in the microenvironment shift production of B cells to short-lived plasma cells early in the response. Polyclonal B cells are recruited into both the plasma cell and germinal center compartments, inhibiting the formation of a targeted, high-affinity response. Finally, memory B cells shift toward an "atypical" phenotype, which may in turn result in changes to the functional properties of this population. While similar properties of B-cell dysregulation have been described across different types of persistent infections, key questions about the underlying mechanisms remain. This review will discuss the recent advances in this field, as well as highlight the critical questions about the interplay between viral load, microenvironment, the polyclonal response and atypical memory B cells that are yet to be answered. Design of new preventative treatments will rely on identifying the extrinsic and intrinsic modulators that push B cells toward an ineffective response, and thus identify new ways to guide them back onto the best path for clearance of virus and formation of effective immune memory., (© 2020 Australian and New Zealand Society for Immunology Inc.)

Published

2020

39. Metabolic characteristics of CD8 + T cell subsets in young and aged individuals are not predictive of functionality.

Author

Quinn KM, Hussain T, Kraus F, Formosa LE, Lam WK, Dagley MJ, Saunders EC, Assmus LM, Wynne-Jones E, Loh L, van de Sandt CE, Cooper L, Good-Jacobson KL, Kedzierska K, Mackay LK, McConville MJ, Ramm G, Ryan MT, and La Gruta NL

Subjects

Adult, Aged, Animals, CD8-Positive T-Lymphocytes cytology, CD8-Positive T-Lymphocytes metabolism, CD8-Positive T-Lymphocytes ultrastructure, Cell Differentiation immunology, Cell Proliferation, Disease Models, Animal, Female, Humans, Influenza A virus immunology, Influenza, Human blood, Influenza, Human immunology, Influenza, Human virology, Male, Mice, Microscopy, Electron, Transmission, Mitochondria metabolism, Mitochondria ultrastructure, T-Lymphocyte Subsets cytology, T-Lymphocyte Subsets metabolism, T-Lymphocyte Subsets ultrastructure, Young Adult, Aging immunology, CD8-Positive T-Lymphocytes immunology, Immunologic Memory, T-Lymphocyte Subsets immunology

Abstract

Virtual memory T (T VM ) cells are antigen-naïve CD8 + T cells that exist in a semi-differentiated state and exhibit marked proliferative dysfunction in advanced age. High spare respiratory capacity (SRC) has been proposed as a defining metabolic characteristic of antigen-experienced memory T (T MEM ) cells, facilitating rapid functionality and survival. Given the semi-differentiated state of T VM cells and their altered functionality with age, here we investigate T VM cell metabolism and its association with longevity and functionality. Elevated SRC is a feature of T VM , but not T MEM , cells and it increases with age in both subsets. The elevated SRC observed in aged mouse T VM cells and human CD8 + T cells from older individuals is associated with a heightened sensitivity to IL-15. We conclude that elevated SRC is a feature of T VM , but not T MEM , cells, is driven by physiological levels of IL-15, and is not indicative of enhanced functionality in CD8 + T cells.

Published

2020

40. Transcription Factor T-bet in B Cells Modulates Germinal Center Polarization and Antibody Affinity Maturation in Response to Malaria.

Author

Ly A, Liao Y, Pietrzak H, Ioannidis LJ, Sidwell T, Gloury R, Doerflinger M, Triglia T, Qin RZ, Groom JR, Belz GT, Good-Jacobson KL, Shi W, Kallies A, and Hansen DS

Subjects

Animals, Antibody Affinity genetics, Antibody Affinity physiology, Malaria immunology, Mice, Mice, Inbred C57BL, Mutation genetics, RGS Proteins genetics, RGS Proteins metabolism, Receptors, CXCR3 genetics, Receptors, CXCR3 metabolism, T-Box Domain Proteins genetics, B-Lymphocytes metabolism, Germinal Center cytology, Germinal Center metabolism, Malaria metabolism, T-Box Domain Proteins metabolism

Abstract

Despite the key role that antibodies play in protection, the cellular processes mediating the acquisition of humoral immunity against malaria are not fully understood. Using an infection model of severe malaria, we find that germinal center (GC) B cells upregulate the transcription factor T-bet during infection. Molecular and cellular analyses reveal that T-bet in B cells is required not only for IgG 2c switching but also favors commitment of B cells to the dark zone of the GC. T-bet was found to regulate the expression of Rgs13 and CXCR3, both of which contribute to the impaired GC polarization observed in the absence of T-bet, resulting in reduced IghV gene mutations and lower antibody avidity. These results demonstrate that T-bet modulates GC dynamics, thereby promoting the differentiation of B cells with increased affinity for antigen., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

41. B Cells Hit a Class Ceiling in the Germinal Center.

Author

Cooper L and Good-Jacobson KL

Subjects

B-Lymphocytes, Germinal Center, Immunoglobulin Class Switching

Abstract

Class-switch recombination (CSR) provides diverse effector functions to B cells. In this issue of Immunity, Roco et al. (2019) refute long-standing dogma that germinal centers are the principal location for CSR; instead, CSR predominantly occurs early post immunization and declines during germinal center formation., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

42. Context-Dependent Role for T-bet in T Follicular Helper Differentiation and Germinal Center Function following Viral Infection.

Author

Sheikh AA, Cooper L, Feng M, Souza-Fonseca-Guimaraes F, Lafouresse F, Duckworth BC, Huntington ND, Moon JJ, Pellegrini M, Nutt SL, Belz GT, Good-Jacobson KL, and Groom JR

Subjects

Animals, Antibodies, Viral immunology, Arenaviridae Infections immunology, Arenaviridae Infections metabolism, Arenaviridae Infections virology, B-Lymphocytes immunology, B-Lymphocytes metabolism, B-Lymphocytes virology, Female, Germinal Center metabolism, Germinal Center virology, Immunoglobulin G metabolism, Lymphocyte Activation, Lymphocytic Choriomeningitis immunology, Lymphocytic Choriomeningitis metabolism, Lymphocytic Choriomeningitis virology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Orthomyxoviridae Infections immunology, Orthomyxoviridae Infections metabolism, Orthomyxoviridae Infections virology, Signal Transduction, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Helper-Inducer virology, Antibody Formation immunology, Cell Differentiation, Germinal Center immunology, Lymphocytic choriomeningitis virus immunology, Orthomyxoviridae immunology, T-Box Domain Proteins physiology, T-Lymphocytes, Helper-Inducer cytology

Abstract

Following infection, inflammatory cues upregulate core transcriptional programs to establish pathogen-specific protection. In viral infections, T follicular helper (TFH) cells express the prototypical T helper 1 transcription factor T-bet. Several studies have demonstrated essential but conflicting roles for T-bet in TFH biology. Understanding the basis of this controversy is crucial, as modulation of T-bet expression instructs TFH differentiation and ultimately protective antibody responses. Comparing influenza and LCMV viral infections, we demonstrate that the role of T-bet is contingent on the environmental setting of TFH differentiation, IL-2 signaling, and T cell competition. Furthermore, we demonstrate that T-bet expression by either TFH or GC B cells independently drives antibody isotype class switching. Specifically, T cell-specific loss of T-bet promotes IgG1, whereas B cell-specific loss of T-bet inhibits IgG2a/c switching. Combined, this work highlights that the context-dependent induction of T-bet instructs the development of protective, neutralizing antibodies following viral infection or vaccination., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

43. Type I interferon induces CXCL13 to support ectopic germinal center formation.

Author

Denton AE, Innocentin S, Carr EJ, Bradford BM, Lafouresse F, Mabbott NA, Mörbe U, Ludewig B, Groom JR, Good-Jacobson KL, and Linterman MA

Subjects

Animals, B-Lymphocytes metabolism, B-Lymphocytes pathology, Chemokine CXCL13 genetics, Female, Fibroblasts metabolism, Fibroblasts pathology, Fibroblasts virology, Germinal Center drug effects, Germinal Center metabolism, Interferon-beta pharmacology, Lung metabolism, Lung pathology, Lung virology, Male, Mice, Inbred C57BL, Mice, Transgenic, Orthomyxoviridae Infections metabolism, Receptors, CXCR5 genetics, Receptors, CXCR5 metabolism, T-Lymphocytes, Regulatory metabolism, T-Lymphocytes, Regulatory pathology, Chemokine CXCL13 metabolism, Germinal Center pathology, Interferon Type I metabolism, Orthomyxoviridae Infections pathology

Abstract

Ectopic lymphoid structures form in a wide range of inflammatory conditions, including infection, autoimmune disease, and cancer. In the context of infection, this response can be beneficial for the host: influenza A virus infection-induced pulmonary ectopic germinal centers give rise to more broadly cross-reactive antibody responses, thereby generating cross-strain protection. However, despite the ubiquity of ectopic lymphoid structures and their role in both health and disease, little is known about the mechanisms by which inflammation is able to convert a peripheral tissue into one that resembles a secondary lymphoid organ. Here, we show that type I IFN produced after viral infection can induce CXCL13 expression in a phenotypically distinct population of lung fibroblasts, driving CXCR5-dependent recruitment of B cells and initiating ectopic germinal center formation. This identifies type I IFN as a novel inducer of CXCL13, which, in combination with other stimuli, can promote lung remodeling, converting a nonlymphoid tissue into one permissive to functional tertiary lymphoid structure formation., (© 2019 Denton et al.)

Published

2019

44. Epigenetic regulation of B cell fate and function during an immune response.

Author

Zhang Y and Good-Jacobson KL

Subjects

Animals, Antibody Formation, Cell Differentiation genetics, DNA Methylation, Gene Expression Regulation, Humans, B-Lymphocyte Subsets immunology, B-Lymphocytes immunology, Epigenesis, Genetic immunology, Germinal Center immunology

Abstract

The humoral immune response requires coordination of molecular programs to mediate differentiation into unique B cell subsets that help clear the infection and form immune memory. Epigenetic modifications are crucial for ensuring that the appropriate genes are transcribed or repressed during B cell differentiation. Recent studies have illuminated the changes in DNA methylation and histone post-translational modifications that accompany the formation of germinal center and antibody-secreting cells during an immune response. In particular, the B cell subset-specific expression and function of DNA methyltransferases and histone-modifying complexes that mediate epigenome changes have begun to be unravelled. This review will discuss the recent advances in this field, as well as highlight critical questions about the relationship between epigenetic regulation and B cell fate and function that are yet to be answered., (© 2019 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2019

45. B cells turn on, tune in with LSD1.

Author

Good-Jacobson KL

Subjects

B-Lymphocytes, Germinal Center, Histone Demethylases, Histones

Published

2019

46. Assessing the role of the T-box transcription factor Eomes in B cell differentiation during either Th1 or Th2 cell-biased responses.

Author

Cooper L, Hailes L, Sheikh A, Zaph C, Belz GT, Groom JR, and Good-Jacobson KL

Subjects

Animals, Cell Differentiation genetics, Cell Differentiation physiology, Lymphocyte Activation, Mice, T-Box Domain Proteins genetics, B-Lymphocytes cytology, B-Lymphocytes metabolism, T-Box Domain Proteins metabolism, Th1 Cells metabolism, Th2 Cells metabolism

Abstract

Successful T-dependent humoral responses require the production of antibody-secreting plasmablasts, as well as the formation of germinal centers which eventually form high-affinity B cell memory. The ability of B cells to differentiate into germinal center and plasma cells, as well as the ability to tailor responses to different pathogens, is driven by transcription factors. In T cells, the T-box transcription factors T-bet and Eomesodermin (Eomes) regulate effector and memory T cell differentiation, respectively. While T-bet has a critical role in regulating anti-viral B cell responses, a role for Eomes in B cells has yet to be described. We therefore investigated whether Eomes was required for B cell differentiation during either Th1 or Th2 cell-biased immune responses. Here, we demonstrate that deletion of Eomes specifically in B cells did not affect B cell differentiation in response to vaccination, as well as following viral or helminth infection. In contrast to its established role in CD8+ T cells, Eomes did not influence memory B cell differentiation. Finally, the use of an Eomes reporter mouse confirmed the lack of Eomes expression during immune responses. Thus, germinal center and plasma cell differentiation and the formation of isotype-switched memory B cells in response to infection are independent of Eomes expression., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

47. Disrupting the Code: Epigenetic Dysregulation of Lymphocyte Function during Infectious Disease and Lymphoma Development.

Author

Di Pietro A and Good-Jacobson KL

Subjects

Animals, Cell Differentiation, Communicable Diseases immunology, DNA Methylation, Gene Expression Regulation, Humans, Immunity, Cellular, Lymphoma immunology, Communicable Diseases genetics, Epigenesis, Genetic, Lymphocytes physiology, Lymphoma genetics

Abstract

Lymphocyte differentiation and identity are controlled by signals in the microenvironment that ultimately mediate gene expression in the nucleus. Although much focus has centered on the strategic and often unique roles transcription factors play within lymphocyte subsets, it is increasingly clear that another level of molecular regulation is crucial for regulating gene expression programs. In particular, epigenetic regulation is critical for appropriately regulated temporal and cell-type-specific gene expression during immune responses. As such, mutations in epigenetic modifiers are linked with lymphomagenesis. Furthermore, certain infections can remodel the epigenome in host cells, either through the microenvironment or by directly co-opting host epigenetic mechanisms, leading to inappropriate gene expression and/or ineffective cellular behavior. This review will focus on how histone modifications and DNA methylation, and the enzymes that regulate the epigenome, underpin lymphocyte differentiation and function in health and disease., (Copyright © 2018 by The American Association of Immunologists, Inc.)

Published

2018

48. Strength in diversity: Phenotypic, functional, and molecular heterogeneity within the memory B cell repertoire.

Author

Good-Jacobson KL

Subjects

B-Lymphocyte Subsets cytology, CD4-Positive T-Lymphocytes immunology, Cell Differentiation immunology, Germinal Center cytology, Humans, Immunologic Memory genetics, Plasma Cells immunology, B-Lymphocyte Subsets immunology, Germinal Center immunology, Immunologic Memory immunology, Receptors, Antigen, B-Cell immunology

Abstract

The vast majority of vaccines exploit antibody memory to induce lasting immunity. Memory B cells are generated during the initial response to infection, but persist long after the infection has cleared. Immune memory success relies on its adaptability: in response to different pathogens, variants of a single pathogen, and in balancing persistence with reactivation and plasma cell differentiation. This is likely achieved by producing a B cell memory population that is highly diverse, and recent work has highlighted the importance of memory B cell subsets in mediating the dichotomous roles of the population. This review will detail the characterization, function and both intrinsic and extrinsic regulation of different memory B cell subsets: memory B cell precursors within the germinal center, phenotypic, and functional heterogeneity of the memory B cell population, and memory B cell subsets that reside in tissues. In particular, understanding the genetic and epigenetic regulation of memory B diversity may be critical for gaining insight into B cell memory responses to pathogens that have evaded effective vaccine design. Therefore, there is a vital need to understand the mechanisms underlying the origin, function and translational potential of the heterogeneity within the memory B cell population., (© 2018 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2018

49. Tailoring Immune Responses toward Autoimmunity: Transcriptional Regulators That Drive the Creation and Collusion of Autoreactive Lymphocytes.

Author

Good-Jacobson KL and Groom JR

Subjects

Animals, Autoantibodies immunology, Humans, Lupus Erythematosus, Systemic pathology, Plasma Cells pathology, T-Lymphocytes, Helper-Inducer pathology, Autoimmunity, Cell Differentiation immunology, Lupus Erythematosus, Systemic immunology, Plasma Cells immunology, Signal Transduction immunology, T-Lymphocytes, Helper-Inducer immunology, Transcription Factors immunology

Abstract

T-dependent humoral immune responses to infection involve a collaboration between B and CD4 T cell activation, migration, and co-stimulation, thereby culminating in the formation of germinal centers (GCs) and eventual differentiation into memory cells and long-lived plasma cells (PCs). CD4 T cell-derived signals drive the formation of a tailored B cell response. Downstream of these signals are transcriptional regulators that are the critical enactors of immune cell programs. In particular, a core group of transcription factors regulate both B and T cell differentiation, identity, and function. The timing and expression levels of these transcription factors are tightly controlled, with dysregulated expression correlated to immune cell dysfunction in autoimmunity and lymphomagenesis. Recent studies have significantly advanced our understanding of both extrinsic and intrinsic regulators of autoreactive B cells and antibody-secreting PCs in systemic lupus erythematosus, rheumatoid arthritis, and other autoimmune conditions. Yet, there are still gaps in our understanding of the causative role these regulators play, as well as the link between lymphoid responses and peripheral damage. This review will focus on the genesis of immunopathogenic CD4 helper and GC B cells. In particular, we will detail the transcriptional regulation of cytokine and chemokine receptor signaling during the pathogenesis of GC-derived autoimmune conditions in both murine models and human patients.

Published

2018

50. Preparing for re-entry: is sequential switching the result of recurrent secondary responses?

Author

Good-Jacobson KL

Subjects

Humans, Phenotype, Time Factors, B-Lymphocytes, Immunoglobulin G

Published

2017