Your search keyword '"Gabrielle T. Belz"' showing total 11 results

1. c-Myb Regulates the T-Bet-Dependent Differentiation Program in B Cells to Coordinate Antibody Responses

Author

Dana Piovesan, Jessica Tempany, Andrea Di Pietro, Inge Baas, Callisthenis Yiannis, Kristy O’Donnell, Yunshun Chen, Victor Peperzak, Gabrielle T. Belz, Charles R. Mackay, Gordon K. Smyth, Joanna R. Groom, David M. Tarlinton, and Kim L. Good-Jacobson

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Humoral immune responses are tailored to the invading pathogen through regulation of key transcription factors and their networks. This is critical to establishing effective antibody-mediated responses, yet it is unknown how B cells integrate pathogen-induced signals to drive or suppress transcriptional programs specialized for each class of pathogen. Here, we detail the key role of the transcription factor c-Myb in regulating the T-bet-mediated anti-viral program. Deletion of c-Myb in mature B cells significantly increased serum IgG2c and CXCR3 expression by upregulating T-bet, normally suppressed during Th2-cell-mediated responses. Enhanced expression of T-bet resulted in aberrant plasma cell differentiation within the germinal center, mediated by CXCR3 expression. These findings identify a dual role for c-Myb in limiting inappropriate effector responses while coordinating plasma cell differentiation with germinal center egress. Identifying such intrinsic regulators of specialized antibody responses can assist in vaccine design and therapeutic intervention in B-cell-mediated immune disorders. : Piovesan et al. examine how B cells establish transcriptional programs that result in tailored responses to invading pathogens. The authors find that the transcription factor c-Myb represses the T-bet-mediated anti-viral program in B cells. c-Myb limits inappropriate effector responses while coordinating plasma cell differentiation with germinal center egress. Keywords: B cells, c-Myb, T-bet, immunoglobulin, CXCR3, plasma cell, germinal center

Published

2017

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

Author

Ann Ly, Yang Liao, Halina Pietrzak, Lisa J. Ioannidis, Tom Sidwell, Renee Gloury, Marcel Doerflinger, Tony Triglia, Raymond Z. Qin, Joanna R. Groom, Gabrielle T. Belz, Kim L. Good-Jacobson, Wei Shi, Axel Kallies, and Diana S. Hansen

Subjects

Biology (General), QH301-705.5

Abstract

Summary: 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 IgG2c 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. : Antibody responses play a pivotal role in clinical immunity to malaria. Ly et al. report that that germinal center (GC) B cells upregulate the transcription factor T-bet during infection. T-bet favors commitment of B cells to the GC dark zone, thereby augmenting immunoglobulin gene mutation rates and antibody affinity maturation. Keywords: malaria, T-bet, B cells, germinal center, antibodies, affinity maturation

Published

2019

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

Author

Amania A. Sheikh, Lucy Cooper, Meiqi Feng, Fernando Souza-Fonseca-Guimaraes, Fanny Lafouresse, Brigette C. Duckworth, Nicholas D. Huntington, James J. Moon, Marc Pellegrini, Stephen L. Nutt, Gabrielle T. Belz, Kim L. Good-Jacobson, and Joanna R. Groom

Subjects

Biology (General), QH301-705.5

Abstract

Summary: 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. : Shiekh et al. show that, in influenza and LCMV infections, the role of the transcription factor T-bet in TFH differentiation is contingent on environmental cues, IL-2 signaling, and T cell competition. Cell-specific T-bet expression independently drives antibody isotype class switching. Therefore T-bet instructs immune protection in a context-dependent manner. Keywords: T cell differentiation, T follicular helper, T helper 1, T-bet, germinal center, influenza, viral infection, transcriptional regulation, isotope switching

Published

2019

4. Deciphering the Innate Lymphoid Cell Transcriptional Program

Author

Cyril Seillet, Lisa A. Mielke, Daniela B. Amann-Zalcenstein, Shian Su, Jerry Gao, Francisca F. Almeida, Wei Shi, Matthew E. Ritchie, Shalin H. Naik, Nicholas D. Huntington, Sebastian Carotta, and Gabrielle T. Belz

Subjects

innate lymphoid cells, development, immunity, transcription factors, innate, Biology (General), QH301-705.5

Abstract

Innate lymphoid cells (ILCs) are enriched at mucosal surfaces, where they provide immune surveillance. All ILC subsets develop from a common progenitor that gives rise to pre-committed progenitors for each of the ILC lineages. Currently, the temporal control of gene expression that guides the emergence of these progenitors is poorly understood. We used global transcriptional mapping to analyze gene expression in different ILC progenitors. We identified PD-1 to be specifically expressed in PLZF+ ILCp and revealed that the timing and order of expression of the transcription factors NFIL3, ID2, and TCF-1 was critical. Importantly, induction of ILC lineage commitment required only transient expression of NFIL3 prior to ID2 and TCF-1 expression. These findings highlight the importance of the temporal program that permits commitment of progenitors to the ILC lineage, and they expand our understanding of the core transcriptional program by identifying potential regulators of ILC development.

Published

2016

5. Acetylation of the Cd8 Locus by KAT6A Determines Memory T Cell Diversity

Author

Dane M. Newman, Shinya Sakaguchi, Aaron Lun, Simon Preston, Marc Pellegrini, Kseniya Khamina, Andreas Bergthaler, Stephen L. Nutt, Gordon K. Smyth, Anne K. Voss, Tim Thomas, Wilfried Ellmeier, Gabrielle T. Belz, and Rhys S. Allan

Subjects

T cells, virus, memory, histone acetylation, epigenetic, Biology (General), QH301-705.5

Abstract

How functionally diverse populations of pathogen-specific killer T cells are generated during an immune response remains unclear. Here, we propose that fine-tuning of CD8αβ co-receptor levels via histone acetylation plays a role in lineage fate. We show that lysine acetyltransferase 6A (KAT6A) is responsible for maintaining permissive Cd8 gene transcription and enabling robust effector responses during infection. KAT6A-deficient CD8+ T cells downregulated surface CD8 co-receptor expression during clonal expansion, a finding linked to reduced Cd8α transcripts and histone-H3 lysine 9 acetylation of the Cd8 locus. Loss of CD8 expression in KAT6A-deficient T cells correlated with reduced TCR signaling intensity and accelerated contraction of the effector-like memory compartment, whereas the long-lived memory compartment appeared unaffected, a result phenocopied by the removal of the Cd8 E8I enhancer element. These findings suggest a direct role of CD8αβ co-receptor expression and histone acetylation in shaping functional diversity within the cytotoxic T cell pool.

Published

2016

6. RUNX2 Mediates Plasmacytoid Dendritic Cell Egress from the Bone Marrow and Controls Viral Immunity

Author

Michaël Chopin, Simon P. Preston, Aaron T.L. Lun, Julie Tellier, Gordon K. Smyth, Marc Pellegrini, Gabrielle T. Belz, Lynn M. Corcoran, Jane E. Visvader, Li Wu, and Stephen L. Nutt

Subjects

Biology (General), QH301-705.5

Abstract

Plasmacytoid dendritic cells (pDCs) represent a unique immune cell type that responds to viral nucleic acids through the rapid production of type I interferons. Within the hematopoietic system, the transcription factor RUNX2 is exclusively expressed in pDCs and is required for their peripheral homeostasis. Here, we show that RUNX2 plays an essential role in promoting pDC localization and function. RUNX2 is required for the appropriate expression of the integrin-mediated adhesion machinery, as well as for the down-modulation of the chemokine receptor CXCR4, which allows pDC egress into the circulation. RUNX2 also facilitates the robust response to viral infection through the control of IRF7, the major regulator of type I interferon production. Mice lacking one copy of Runx2 have reduced numbers of peripheral pDCs and IFN-α expression, which might contribute to the reported difficulties of individuals with cleidocranial dysplasia, who are haploinsufficient for RUNX2, to clear viral infections.

Published

2016

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

Author

Raymond Z. Qin, Joanna R Groom, Halina M. Pietrzak, Kim L. Good-Jacobson, Lisa J Ioannidis, Tom Sidwell, Ann Ly, Diana S. Hansen, Marcel Doerflinger, Axel Kallies, Wei Shi, Gabrielle T. Belz, Renee Gloury, Tony Triglia, and Yang Liao

Subjects

0301 basic medicine, Receptors, CXCR3, Antibody Affinity, chemical and pharmacologic phenomena, Gene mutation, General Biochemistry, Genetics and Molecular Biology, Affinity maturation, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Animals, Avidity, Transcription factor, lcsh:QH301-705.5, B-Lymphocytes, biology, Chemistry, Germinal center, hemic and immune systems, Germinal Center, Malaria, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, lcsh:Biology (General), Mutation, Humoral immunity, biology.protein, Antibody, T-Box Domain Proteins, RGS Proteins, 030217 neurology & neurosurgery

Abstract

Summary: 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 IgG2c 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. : Antibody responses play a pivotal role in clinical immunity to malaria. Ly et al. report that that germinal center (GC) B cells upregulate the transcription factor T-bet during infection. T-bet favors commitment of B cells to the GC dark zone, thereby augmenting immunoglobulin gene mutation rates and antibody affinity maturation. Keywords: malaria, T-bet, B cells, germinal center, antibodies, affinity maturation

Published

2019

8. c-Myb Regulates the T-Bet-Dependent Differentiation Program in B Cells to Coordinate Antibody Responses

Author

Charles R. Mackay, David M. Tarlinton, Inge Baas, Dana Piovesan, Andrea Di Pietro, Yunshun Chen, Kristy O'Donnell, Jessica C Tempany, Victor Peperzak, Gordon K. Smyth, Kim L. Good-Jacobson, Gabrielle T. Belz, Callisthenis Yiannis, and Joanna R Groom

Subjects

Male, 0301 basic medicine, Receptors, CXCR3, Transcription, Genetic, Cellular differentiation, Plasma Cells, Antibody Affinity, chemical and pharmacologic phenomena, Plasma cell, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, Proto-Oncogene Proteins c-myb, 03 medical and health sciences, 0302 clinical medicine, Plasma cell differentiation, medicine, Animals, Humans, lcsh:QH301-705.5, Transcription factor, Regulation of gene expression, B-Lymphocytes, CD40, Germinal center, Cell Differentiation, Germinal Center, 3. Good health, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, lcsh:Biology (General), Antibody Formation, Immunology, biology.protein, Female, Syndecan-1, T-Box Domain Proteins, Gene Deletion, 030215 immunology

Abstract

Summary: Humoral immune responses are tailored to the invading pathogen through regulation of key transcription factors and their networks. This is critical to establishing effective antibody-mediated responses, yet it is unknown how B cells integrate pathogen-induced signals to drive or suppress transcriptional programs specialized for each class of pathogen. Here, we detail the key role of the transcription factor c-Myb in regulating the T-bet-mediated anti-viral program. Deletion of c-Myb in mature B cells significantly increased serum IgG2c and CXCR3 expression by upregulating T-bet, normally suppressed during Th2-cell-mediated responses. Enhanced expression of T-bet resulted in aberrant plasma cell differentiation within the germinal center, mediated by CXCR3 expression. These findings identify a dual role for c-Myb in limiting inappropriate effector responses while coordinating plasma cell differentiation with germinal center egress. Identifying such intrinsic regulators of specialized antibody responses can assist in vaccine design and therapeutic intervention in B-cell-mediated immune disorders. : Piovesan et al. examine how B cells establish transcriptional programs that result in tailored responses to invading pathogens. The authors find that the transcription factor c-Myb represses the T-bet-mediated anti-viral program in B cells. c-Myb limits inappropriate effector responses while coordinating plasma cell differentiation with germinal center egress. Keywords: B cells, c-Myb, T-bet, immunoglobulin, CXCR3, plasma cell, germinal center

Published

2017

9. Deciphering the Innate Lymphoid Cell Transcriptional Program

Author

Wei Shi, Francisca F. Almeida, Daniela Amann-Zalcenstein, Lisa A. Mielke, Nicholas D. Huntington, Jerry Gao, Shalin H. Naik, Shian Su, Matthew E. Ritchie, Sebastian Carotta, Cyril Seillet, and Gabrielle T. Belz

Subjects

0301 basic medicine, Lineage (genetic), Cellular differentiation, Programmed Cell Death 1 Receptor, innate lymphoid cells, Bone Marrow Cells, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, transcription factors, innate, Animals, Cell Lineage, Hepatocyte Nuclear Factor 1-alpha, Lymphocytes, Progenitor cell, skin and connective tissue diseases, Transcription factor, development, lcsh:QH301-705.5, Progenitor, Regulation of gene expression, Genetics, NFIL3, Innate lymphoid cell, Cell Differentiation, immunity, Immunity, Innate, Cell biology, Killer Cells, Natural, body regions, Basic-Leucine Zipper Transcription Factors, 030104 developmental biology, Gene Expression Regulation, lcsh:Biology (General), 030215 immunology

Abstract

SummaryInnate lymphoid cells (ILCs) are enriched at mucosal surfaces, where they provide immune surveillance. All ILC subsets develop from a common progenitor that gives rise to pre-committed progenitors for each of the ILC lineages. Currently, the temporal control of gene expression that guides the emergence of these progenitors is poorly understood. We used global transcriptional mapping to analyze gene expression in different ILC progenitors. We identified PD-1 to be specifically expressed in PLZF+ ILCp and revealed that the timing and order of expression of the transcription factors NFIL3, ID2, and TCF-1 was critical. Importantly, induction of ILC lineage commitment required only transient expression of NFIL3 prior to ID2 and TCF-1 expression. These findings highlight the importance of the temporal program that permits commitment of progenitors to the ILC lineage, and they expand our understanding of the core transcriptional program by identifying potential regulators of ILC development.

Published

2016

10. RUNX2 Mediates Plasmacytoid Dendritic Cell Egress from the Bone Marrow and Controls Viral Immunity

Author

Simon Preston, Julie Tellier, Marc Pellegrini, Jane E. Visvader, Aaron T. L. Lun, Gabrielle T. Belz, Stephen L. Nutt, Michael Chopin, Gordon K. Smyth, Lynn M. Corcoran, and Li Wu

Subjects

0301 basic medicine, Chemokine, Cell type, musculoskeletal, neural, and ocular physiology, hemic and immune systems, Plasmacytoid dendritic cell, Biology, Type I interferon production, CXCR4, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Chemokine receptor, 030104 developmental biology, 0302 clinical medicine, Immune system, lcsh:Biology (General), stomatognathic system, 030220 oncology & carcinogenesis, Immunology, biology.protein, IRF7, lcsh:QH301-705.5

Abstract

SummaryPlasmacytoid dendritic cells (pDCs) represent a unique immune cell type that responds to viral nucleic acids through the rapid production of type I interferons. Within the hematopoietic system, the transcription factor RUNX2 is exclusively expressed in pDCs and is required for their peripheral homeostasis. Here, we show that RUNX2 plays an essential role in promoting pDC localization and function. RUNX2 is required for the appropriate expression of the integrin-mediated adhesion machinery, as well as for the down-modulation of the chemokine receptor CXCR4, which allows pDC egress into the circulation. RUNX2 also facilitates the robust response to viral infection through the control of IRF7, the major regulator of type I interferon production. Mice lacking one copy of Runx2 have reduced numbers of peripheral pDCs and IFN-α expression, which might contribute to the reported difficulties of individuals with cleidocranial dysplasia, who are haploinsufficient for RUNX2, to clear viral infections.

Published

2016

11. Acetylation of the Cd8 Locus by KAT6A Determines Memory T Cell Diversity

Author

Simon Preston, Wilfried Ellmeier, Stephen L. Nutt, Kseniya Khamina, Anne K. Voss, Dane M. Newman, Tim Thomas, Rhys S. Allan, Andreas Bergthaler, Aaron T. L. Lun, Gabrielle T. Belz, Gordon K. Smyth, Marc Pellegrini, and Shinya Sakaguchi

Subjects

0301 basic medicine, Cellular differentiation, CD8 Antigens, T cells, virus, CD8-Positive T-Lymphocytes, Lymphocytic Choriomeningitis, General Biochemistry, Genetics and Molecular Biology, memory, 03 medical and health sciences, Mice, 0302 clinical medicine, Transcriptional regulation, medicine, Animals, Cell Lineage, Enhancer, lcsh:QH301-705.5, Histone Acetyltransferases, Mice, Knockout, biology, Effector, T-cell receptor, histone acetylation, Acetylation, Cell Differentiation, Molecular biology, Mice, Inbred C57BL, 030104 developmental biology, Histone, medicine.anatomical_structure, lcsh:Biology (General), 030220 oncology & carcinogenesis, biology.protein, Memory T cell, Immunologic Memory, Protein Processing, Post-Translational, epigenetic, T-Lymphocytes, Cytotoxic

Abstract

SummaryHow functionally diverse populations of pathogen-specific killer T cells are generated during an immune response remains unclear. Here, we propose that fine-tuning of CD8αβ co-receptor levels via histone acetylation plays a role in lineage fate. We show that lysine acetyltransferase 6A (KAT6A) is responsible for maintaining permissive Cd8 gene transcription and enabling robust effector responses during infection. KAT6A-deficient CD8+ T cells downregulated surface CD8 co-receptor expression during clonal expansion, a finding linked to reduced Cd8α transcripts and histone-H3 lysine 9 acetylation of the Cd8 locus. Loss of CD8 expression in KAT6A-deficient T cells correlated with reduced TCR signaling intensity and accelerated contraction of the effector-like memory compartment, whereas the long-lived memory compartment appeared unaffected, a result phenocopied by the removal of the Cd8 E8I enhancer element. These findings suggest a direct role of CD8αβ co-receptor expression and histone acetylation in shaping functional diversity within the cytotoxic T cell pool.