Your search keyword '"Tartey, Sarang"' showing total 16 results

1. Ets-2 deletion in myeloid cells attenuates IL-1α-mediated inflammatory disease caused by a Ptpn6 point mutation

Author

Tartey, Sarang, Gurung, Prajwal, Karki, Rajendra, Burton, Amanda, Hertzog, Paul, and Kanneganti, Thirumala-Devi

Published

2021

2. ASK1/2 signaling promotes inflammation in a mouse model of neutrophilic dermatosis

Author

Tartey, Sarang, Gurung, Prajwal, Dasari, Tejasvi Krishna, Burton, Amanda, and Kanneganti, Thirumala-Devi

Subjects

Autoimmune diseases -- Development and progression -- Models, Inflammation -- Development and progression, Mitogen-activated protein kinases -- Physiological aspects -- Health aspects, Dermatitis -- Development and progression -- Models, Neutrophils -- Physiological aspects -- Health aspects, Health care industry

Abstract

Mice homozygous for the Tyr208Asn amino acid substitution in the carboxy terminus of Src homology region 2 (SH2) domain-containing phosphatase 1 (SHP-1) (referred to as [Ptpn6.sup.spin] mice) spontaneously develop a severe inflammatory disease resembling neutrophilic dermatosis in humans. Disease in [Ptpn6.sup.spin] mice is characterized by persistent footpad swelling and suppurative inflammation. Recently, in addition to IL-1[alpha] and IL-1R signaling, we demonstrated a pivotal role for several kinases such as SYK, RIPK1, and TAK1 in promoting inflammatory disease in [Ptpn6.sup.spin] mice. In order to identify new kinases involved in SHP-1-mediated inflammation, we took a genetic approach and discovered apoptosis signal-regulating kinases 1 and 2 (ASK1 and ASK2) as novel kinases regulating Ptpn6-mediated footpad inflammation. Double deletion of ASK1 and ASK2 abrogated cutaneous inflammatory disease in [Ptpn6.sup.spin] mice. This double deletion further rescued the splenomegaly and lymphomegaly caused by excessive neutrophil infiltration in [Ptpn6.sup.spin] mice. Mechanistically, ASK regulates [Ptpn6.sup.spin]-mediated disease by controlling proinflammatory signaling in the neutrophils. Collectively, the present study identifies SHP-1 and ASK signaling crosstalk as a critical regulator of IL-1[alpha]-driven inflammation and opens future avenues for finding novel drug targets to treat neutrophilic dermatosis in humans., Introduction Mutations in the PTPN6 gene that encodes for the protein tyrosine phosphatase Src homology region 2 (SH2) domain-containing phosphatase 1 (SHP-1) have been linked with autoinflammatory and autoimmune diseases [...]

Published

2018

3. Akirin2 is critical for inducing inflammatory genes by bridging IκB‐ζ and the SWI/SNF complex

Author

Tartey, Sarang, Matsushita, Kazufumi, Vandenbon, Alexis, Ori, Daisuke, Imamura, Tomoko, Mino, Takashi, Standley, Daron M, Hoffmann, Jules A, Reichhart, Jean‐Marc, Akira, Shizuo, and Takeuchi, Osamu

Published

2014

4. Cyclin J–CDK complexes limit innate immune responses by reducing proinflammatory changes in macrophage metabolism.

Author

Chong, Yee Kien, Tartey, Sarang, Yoshikawa, Yuki, Imami, Koshi, Li, Songling, Yoshinaga, Masanori, Hirabayashi, Ai, Liu, Guohao, Vandenbon, Alexis, Hia, Fabian, Uehata, Takuya, Mino, Takashi, Suzuki, Yutaka, Noda, Takeshi, Ferrandon, Dominique, Standley, Daron M., Ishihama, Yasushi, and Takeuchi, Osamu

Subjects

CYCLINS, CYCLIN-dependent kinases, IMMUNE response, GLYCOLYSIS, TYPE I interferons, MITOCHONDRIAL proteins, MACROPHAGE inflammatory proteins, HEAT shock proteins

Abstract

Toll-like receptor (TLR) stimulation induces glycolysis and the production of mitochondrial reactive oxygen species (ROS), both of which are critical for inflammatory responses in macrophages. Here, we demonstrated that cyclin J, a TLR-inducible member of the cyclin family, reduced cytokine production in macrophages by coordinately controlling glycolysis and mitochondrial functions. Cyclin J interacted with cyclin-dependent kinases (CDKs), which increased the phosphorylation of a subset of CDK substrates, including the transcription factor FoxK1 and the GTPase Drp1. Cyclin J–dependent phosphorylation of FoxK1 decreased the transcription of glycolytic genes and Hif-1α activation, whereas hyperactivation of Drp1 by cyclin J–dependent phosphorylation promoted mitochondrial fragmentation and impaired the production of mitochondrial ROS. In mice, cyclin J in macrophages limited the growth of tumor xenografts and protected against LPS-induced shock but increased the susceptibility to bacterial infection. Collectively, our findings indicate that cyclin J–CDK signaling promotes antitumor immunity and the resolution of inflammation by opposing the metabolic changes that drive inflammatory responses in macrophages. Cyclin macrophages off: The activation of macrophages stimulates metabolic changes that are critical for these cells to respond to infections and tumors. Chong et al. found that cyclin J suppressed macrophage activation through a cell cycle–independent mechanism. Stimulating mouse macrophages with lipopolysaccharide (LPS) or type I interferon induced the expression of the gene encoding cyclin J, and constitutive expression of cyclin J in macrophages attenuated LPS-induced metabolic reprogramming and inflammatory responses. Mechanistically, cyclin J interacted with cyclin-dependent kinases (CDKs) to promote phosphorylation of the transcription factor FoxK1 and the mitochondrial fission protein Drp1, leading to reductions in glycolysis and reactive oxygen species production and an increase in mitochondrial fragmentation. Macrophage-specific loss of cyclin J sensitized mice to LPS-induced shock and increased the growth of tumor xenografts but protected against infection. Cyclin J therefore restrains macrophage responses by dampening activation-induced metabolic reprogramming. [ABSTRACT FROM AUTHOR]

Published

2022

5. Inflammasomes in the pathophysiology of autoinflammatory syndromes.

Author

Tartey, Sarang and Kanneganti, Thirumala‐Devi

Subjects

INFLAMMASOMES, DISEASES, FAMILIAL Mediterranean fever, CRYOPYRIN-associated periodic syndromes, SYNDROMES

Abstract

Inflammasomes are a specialized group of intracellular sensors that are key components of the host innate immune system. Autoinflammatory diseases are disorders of the innate immune system that are characterized by recurrent inflammation and serious complications. Dysregulation of the inflammasome is associated with the onset and progression of several autoinflammatory and autoimmune diseases, including cryopyrin‐associated periodic fever syndrome, familial Mediterranean fever, rheumatoid arthritis, and systemic lupus erythematosus. In this review, we discuss the involvement of various inflammasome components in the regulation of autoinflammatory disorders and describe the manifestations of these autoinflammatory diseases caused by inflammasome activation. [ABSTRACT FROM AUTHOR]

Published

2020

6. Differential role of the NLRP3 inflammasome in infection and tumorigenesis.

Author

Tartey, Sarang and Kanneganti, Thirumala‐Devi

Subjects

*METABOLIC disorders, *INFLAMMATORY bowel diseases, *INFECTION

Abstract

Summary: Dysregulated inflammation is one of the hallmarks of cancer initiation and progression. Emerging evidence indicates that inflammasomes play a central role in regulating immune cell functions in various infections and cancer. Inflammasomes are multimeric complexes consisting of nucleotide‐binding oligomerization domain (NOD) ‐like receptors (NLRs). Among the NLRs, NOD1, NOD2 and NLRP3 respond to a variety of endogenous (i.e. damage‐associated molecular patterns) and exogenous (i.e. pathogen‐associated molecular patterns) stimuli. The NLRP3 inflammasome is associated with the onset and progression of autoinflammatory and autoimmune diseases, including metabolic disorders, multiple sclerosis, inflammatory bowel disease, and cryopyrin‐associated periodic fever syndrome. NLRP3 is also associated with a wide variety of infections and tumorigenesis that are closely correlated with chemotherapy response and prognosis. In this review, we explore the rapidly expanding body of research on the expression and functions of NLRP3 in infections and cancers and outline novel inhibitors targeting the NLRP3 inflammasome that could be developed as therapeutic alternatives to current anticancer treatment. "The NLRP3 inflammasome is important not only for fighting against bacterial, fungal and viral infections but also for mediating cancer initiation and progression. NLRP3 inflammasome activation can create a pro‐inflammatory microenvironment that induces malignant transformation and suppresses local immunity normally provided by natural killer or T cells. In this review, we summarize and discuss the current understanding of the role of NLRP3 inflammasome in infections and cancer". [ABSTRACT FROM AUTHOR]

Published

2019

7. Cutting Edge: Dysregulated CARD9 Signaling in Neutrophils Drives Inflammation in a Mouse Model of Neutrophilic Dermatoses.

Author

Tartey, Sarang, Gurung, Prajwal, Samir, Parimal, Burton, Amanda, and Kanneganti, Thirumala-Devi

Subjects

*NEUTROPHILS, *INFLAMMATION, *SKIN diseases, *INTERLEUKIN-1, *DELETION mutation

Abstract

Mice homozygous for the Y208N amino acid substitution in the carboxy terminus of SHP-1 (referred to as Ptpn6spin mice) spontaneously develop a severe inflammatory disease resembling neutrophilic dermatosis in humans. Disease in Ptpn6spin mice is characterized by persistent footpad swelling and suppurative inflammation. Recently, in addition to IL-1α and IL-1R signaling, we demonstrated a pivotal role for RIPK1, TAK1, and ASK1 in promoting inflammatory disease in Ptpn6spin mice. In the current study we have identified a previously unknown role for CARD9 signaling as a critical regulator for Ptpn6spin-mediated footpad inflammation. Genetic deletion of CARD9 significantly rescued the Ptpn6spin -mediated footpad inflammation. Mechanistically, enhanced IL-1α--mediated signaling in Ptpn6spin mice neutrophils was dampened in Ptpn6spin Card9-/- mice. Collectively, this study identifies SHP-1 and CARD9 cross-talk as a novel regulator of IL-1α--driven inflammation and opens future avenues for finding novel drug targets to treat neutrophilic dermatosis in humans. [ABSTRACT FROM AUTHOR]

Published

2018

8. Pathogen recognition and Toll-like receptor targeted therapeutics in innate immune cells.

Author

Tartey, Sarang and Takeuchi, Osamu

Subjects

*NATURAL immunity, *TOLL-like receptors, *CARCINOGENESIS, *TARGETED drug delivery, *DRUG development

Abstract

The innate immune system deploys a variety of pattern-recognition receptors (PRRs) which include Toll-like receptors (TLRs), RIG-I-like receptors, NOD-like receptors, and C-type lectin receptors to detect the invasion of pathogens and initiate protective responses. The intercellular and intracellular orchestration of signals from different PRRs, their endogenous or microbial ligands and accessory molecules determine the stimulatory or inhibitory responses. Progressing over the last two decades, considerable research on the molecular mechanisms underlying host–pathogen interactions has led to a paradigm shift of our understanding of TLR signaling in the innate immune system. Given that a significant amount of evidence implicates TLRs in the pathogenesis of immune diseases and cancer, and their activation occurs early in the inflammatory cascade, they are attractive targets for novel therapeutic agents. In this review, we discuss the recent advances in TLR signaling cross talks and the mechanism of pathogen recognition with special emphasis on the role of TLRs in tumor immunity and TLR-targeted therapeutics. [ABSTRACT FROM PUBLISHER]

Published

2017

9. Chromatin Remodeling and Transcriptional Control in Innate Immunity: Emergence of Akirin2 as a Novel Player.

Author

Tartey, Sarang and Takeuchi, Osamu

Subjects

*CHROMATIN, *TRANSCRIPTION factors, *NATURAL immunity, *MACROPHAGES

Abstract

Transcriptional regulation of inflammatory gene expression has been at the forefront of studies of innate immunity and is coordinately regulated by transcription factors, including NF-kB, and chromatin modifiers. The growing evidence for involvement of chromatin in the regulation of gene expression in innate immune cells, has uncovered an evolutionarily conserved role of microbial sensing and chromatin remodeling. Toll-like receptors and RIG-I-like receptors trigger these signaling pathways leading to transcriptional expression of a set of genes involved in inflammation. Tightly regulated control of this gene expression is a paramount, and often foremost, goal of most biological endeavors. In this review, we will discuss the recent progress about the molecular mechanisms governing control of pro-inflammatory gene expression by an evolutionarily conserved novel nuclear protein Akirin2 in macrophages and its emergence as an essential link between NF-kB and chromatin remodelers for transcriptional regulation. [ABSTRACT FROM AUTHOR]

Published

2015

10. Akirin2 is critical for inducing inflammatory genes by bridging IκB-ζ and the SWI/ SNF complex.

Author

Tartey, Sarang, Matsushita, Kazufumi, Vandenbon, Alexis, Ori, Daisuke, Imamura, Tomoko, Mino, Takashi, Standley, Daron M, Hoffmann, Jules A, Reichhart, Jean‐Marc, Akira, Shizuo, and Takeuchi, Osamu

Subjects

TRANSCRIPTION factors, INFLAMMATION, GENETIC regulation, CYTOKINES, NATURAL immunity, CHROMATIN

Abstract

Transcription of inflammatory genes in innate immune cells is coordinately regulated by transcription factors, including NF-κB, and chromatin modifiers. However, it remains unclear how microbial sensing initiates chromatin remodeling. Here, we show that Akirin2, an evolutionarily conserved nuclear protein, bridges NF-κB and the chromatin remodeling SWI/ SNF complex by interacting with BRG1-Associated Factor 60 ( BAF60) proteins as well as IκB-ζ, which forms a complex with the NF-κB p50 subunit. These interactions are essential for Toll-like receptor-, RIG-I-, and Listeria-mediated expression of proinflammatory genes including Il6 and Il12b in macrophages. Consistently, effective clearance of Listeria infection required Akirin2. Furthermore, Akirin2 and IκB-ζ recruitment to the Il6 promoter depend upon the presence of IκB-ζ and Akirin2, respectively, for regulation of chromatin remodeling. BAF60 proteins were also essential for the induction of Il6 in response to LPS stimulation. Collectively, the IκB-ζ-Akirin2- BAF60 complex physically links the NF-κB and SWI/ SNF complexes in innate immune cell activation. By recruiting SWI/ SNF chromatin remodellers to IκB-ζ, transcriptional coactivator for NF-κB, the conserved nuclear protein Akirin2 stimulates pro-inflammatory gene promoters in mouse macrophages during innate immune responses to viral or bacterial infection. [ABSTRACT FROM AUTHOR]

Published

2014

11. Regnase-1 and Roquin Regulate a Common Element in Inflammatory mRNAs by Spatiotemporally Distinct Mechanisms.

Author

Mino, Takashi, Murakawa, Yasuhiro, Fukao, Akira, Vandenbon, Alexis, Wessels, Hans-Hermann, Ori, Daisuke, Uehata, Takuya, Tartey, Sarang, Akira, Shizuo, Suzuki, Yutaka, Vinuesa, Carola G., Ohler, Uwe, Standley, Daron M., Landthaler, Markus, Fujiwara, Toshinobu, and Takeuchi, Osamu

Subjects

*MESSENGER RNA, *SPATIOTEMPORAL processes, *CARRIER proteins, *IMMUNOLOGY of inflammation, *HOMEOSTASIS, *RIBOSOMES

Abstract

Summary Regnase-1 and Roquin are RNA binding proteins essential for degradation of inflammation-related mRNAs and maintenance of immune homeostasis. However, their mechanistic relationship has yet to be clarified. Here, we show that, although Regnase-1 and Roquin regulate an overlapping set of mRNAs via a common stem-loop structure, they function in distinct subcellular locations: ribosome/endoplasmic reticulum and processing-body/stress granules, respectively. Moreover, Regnase-1 specifically cleaves and degrades translationally active mRNAs and requires the helicase activity of UPF1, similar to the decay mechanisms of nonsense mRNAs. In contrast, Roquin controls translationally inactive mRNAs, independent of UPF1. Defects in both Regnase-1 and Roquin lead to large increases in their target mRNAs, although Regnase-1 tends to control the early phase of inflammation when mRNAs are more actively translated. Our findings reveal that differential regulation of mRNAs by Regnase-1 and Roquin depends on their translation status and enables elaborate control of inflammation. [ABSTRACT FROM AUTHOR]

Published

2015

12. A MyD88/IL1R Axis Regulates PD-1 Expression on Tumor-Associated Macrophages and Sustains Their Immunosuppressive Function in Melanoma.

Author

Tartey S, Neale G, Vogel P, Malireddi RKS, and Kanneganti TD

Subjects

Animals, Cell Line, Tumor, Disease Models, Animal, Disease Progression, Female, Gene Expression Regulation, Neoplastic, Humans, Male, Melanoma pathology, Mice, Mice, Knockout, Myeloid Differentiation Factor 88 genetics, Receptors, Interleukin-1 genetics, Skin Neoplasms pathology, Immune Tolerance genetics, Melanoma immunology, Myeloid Differentiation Factor 88 deficiency, Myeloid Differentiation Factor 88 metabolism, Programmed Cell Death 1 Receptor metabolism, Receptors, Interleukin-1 metabolism, Signal Transduction genetics, Skin Neoplasms immunology, Tumor-Associated Macrophages immunology

Abstract

Macrophages are critical mediators of tissue homeostasis, cell proliferation, and tumor metastasis. Tumor-associated macrophages (TAM) are generally associated with tumor-promoting immunosuppressive functions in solid tumors. Here, we examined the transcriptional landscape of adaptor molecules downstream of Toll-like receptors in human cancers and found that higher expression of MYD88 correlated with tumor progression. In murine melanoma, MyD88, but not Trif, was essential for tumor progression, angiogenesis, and maintaining the immunosuppressive phenotype of TAMs. In addition, MyD88 expression in myeloid cells drove melanoma progression. The MyD88/IL1 receptor (IL1R) axis regulated programmed cell death (PD)-1 expression on TAMs by promoting recruitment of NF-κBp65 to the Pdcd1 promoter. Furthermore, a combinatorial immunotherapy approach combining the MyD88 inhibitor with anti-PD-1 blockade elicited strong antitumor effects. Thus, the MyD88/IL1R axis maintains the immunosuppressive function of TAMs and promotes tumor growth by regulating PD-1 expression. SIGNIFICANCE: These findings indicate that MyD88 regulates TAM-immunosuppressive activity, suggesting that macrophage-mediated immunotherapy combining MYD88 inhibitors with PD-1 blockade could result in better treatment outcomes in a wide variety of cancers. GRAPHICAL ABSTRACT: http://cancerres.aacrjournals.org/content/canres/81/9/2358/F1.large.jpg., (©2021 American Association for Cancer Research.)

Published

2021

13. Akirin2-Mediated Transcriptional Control by Recruiting SWI/SNF Complex in B Cells.

Author

Tartey S and Takeuchi O

Subjects

Animals, DNA-Binding Proteins genetics, Epigenesis, Genetic, Gene Expression Regulation, Humans, NF-kappa B metabolism, Protein Serine-Threonine Kinases genetics, Signal Transduction, Transcription Factors genetics, B-Lymphocytes immunology, Chromatin metabolism, DNA-Binding Proteins metabolism, Inflammation immunology, Protein Serine-Threonine Kinases metabolism, Transcription Factors metabolism

Abstract

Extensive studies in last decade have demonstrated that dynamic control of gene transcription is key in the regulation of inflammatory responses. Although signaling pathways and transcription factors have a central role, growing evidence for the involvement of chromatin in the regulation of gene expression in immune cells has uncovered an evolutionarily conserved role of pathogen recognition and epigenetic regulation. The substantial potential of these responses to drive pathological inflammation and tissue damage highlights the need for rigorous control of these responses. Recently, an evolutionarily conserved nuclear factor, Akirin2, has been identified as an essential link between nuclear factor-κB and chromatin remodelers for transcriptional regulation in macrophages and B cells. In this review, we discuss current understanding of the molecular mechanisms that have instrumental roles in governing the inflammatory response with special emphasis on Akirin2 in B cells.

Published

2016

14. Essential Function for the Nuclear Protein Akirin2 in B Cell Activation and Humoral Immune Responses.

Author

Tartey S, Matsushita K, Imamura T, Wakabayashi A, Ori D, Mino T, and Takeuchi O

Subjects

Animals, Antigens, CD19 genetics, Antigens, CD19 immunology, Apoptosis, B-Lymphocytes cytology, CD40 Antigens genetics, CD40 Antigens immunology, Cell Proliferation, Cyclin D genetics, Cyclin D immunology, Cyclin D2 genetics, Cyclin D2 immunology, DNA Helicases genetics, DNA Helicases immunology, Gene Expression Regulation, Mice, Mice, Knockout, NF-kappa B genetics, NF-kappa B immunology, Nuclear Proteins genetics, Nuclear Proteins immunology, Promoter Regions, Genetic, Protein Transport, Proto-Oncogene Proteins c-myc genetics, Proto-Oncogene Proteins c-myc immunology, Repressor Proteins deficiency, Repressor Proteins genetics, Signal Transduction, Toll-Like Receptors genetics, Toll-Like Receptors immunology, Transcription Factors genetics, Transcription Factors immunology, B-Lymphocytes immunology, Cell Lineage immunology, Immunity, Humoral, Lymphocyte Activation, Repressor Proteins immunology

Abstract

Akirin2, an evolutionarily conserved nuclear protein, is an important factor regulating inflammatory gene transcription in mammalian innate immune cells by bridging the NF-κB and SWI/SNF complexes. Although Akirin is critical for Drosophila immune responses, which totally rely on innate immunity, the mammalian NF-κB system is critical not only for the innate but also for the acquired immune system. Therefore, we investigated the role of mouse Akirin2 in acquired immune cells by ablating Akirin2 function in B lymphocytes. B cell-specific Akirin2-deficient (Cd19(Cre/+)Akirin2(fl/fl)) mice showed profound decrease in the splenic follicular (FO) and peritoneal B-1, but not splenic marginal zone (MZ), B cell numbers. However, both Akirin2-deficient FO and MZ B cells showed severe proliferation defect and are prone to undergo apoptosis in response to TLR ligands, CD40, and BCR stimulation. Furthermore, B cell cycling was defective in the absence of Akirin2 owing to impaired expression of genes encoding cyclin D and c-Myc. Additionally, Brg1 recruitment to the Myc and Ccnd2 promoter was severely impaired in Akirin2-deficient B cells. Cd19(Cre/+)Akirin2(fl/fl) mice showed impaired in vivo immune responses to T-dependent and -independent Ags. Collectively, these results demonstrate that Akirin2 is critical for the mitogen-induced B cell cycle progression and humoral immune responses by controlling the SWI/SNF complex, further emphasizing the significant function of Akirin2 not only in the innate, but also in adaptive immune cells., (Copyright © 2015 by The American Association of Immunologists, Inc.)

Published

2015

15. Critical role of AZI2 in GM-CSF-induced dendritic cell differentiation.

Author

Fukasaka M, Ori D, Kawagoe T, Uematsu S, Maruyama K, Okazaki T, Kozaki T, Imamura T, Tartey S, Mino T, Satoh T, Akira S, and Takeuchi O

Subjects

Animals, Antigens immunology, Cell Differentiation drug effects, Cell Proliferation, Cytokines biosynthesis, Dendritic Cells drug effects, Gene Expression, Gene Order, Gene Targeting, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Lymphocyte Activation genetics, Lymphocyte Activation immunology, Macrophages immunology, Macrophages metabolism, Membrane Proteins pharmacology, Mice, Mice, Knockout, Protein Serine-Threonine Kinases metabolism, T-Lymphocytes immunology, Toll-Like Receptors metabolism, Adaptor Proteins, Signal Transducing genetics, Cell Differentiation genetics, Dendritic Cells cytology, Dendritic Cells metabolism

Abstract

TNFR-associated factor family member-associated NF-κB activator (TANK)-binding kinase 1 (TBK1) is critical for the activation of IFN regulatory factor 3 and type I IFN production upon virus infection. A set of TBK1-binding proteins, 5-azacytidine-induced gene 2 (AZI2; also known as NAP1), TANK, and TBK1-binding protein 1 (TBKBP1), have also been implicated in the production of type I IFNs. Among them, TANK was found to be dispensable for the responses against virus infection. However, physiological roles of AZI2 and TBKBP1 have yet to be clarified. In this study, we found that none of these TBK1-binding proteins is critical for type I IFN production in mice. In contrast, AZI2, but not TBKBP1, is critical for the differentiation of conventional dendritic cells (cDCs) from bone marrow cells in response to GM-CSF. AZI2 controls GM-CSF-induced cell cycling of bone marrow cells via TBK1. GM-CSF-derived DCs from AZI2-deficient mice show severe defects in cytokine production and T cell activation both in vitro and in vivo. Reciprocally, overexpression of AZI2 results in efficient generation of cDCs, and the cells show enhanced T cell activation in response to Ag stimulation. Taken together, AZI2 expression is critical for the generation of cDCs by GM-CSF and can potentially be used to increase the efficiency of immunization by cDCs.

Published

2013

16. Essential roles of K63-linked polyubiquitin-binding proteins TAB2 and TAB3 in B cell activation via MAPKs.

Author

Ori D, Kato H, Sanjo H, Tartey S, Mino T, Akira S, and Takeuchi O

Subjects

Adaptor Proteins, Signal Transducing chemistry, Animals, Cell Differentiation immunology, Cells, Cultured, Epitopes, B-Lymphocyte immunology, Female, Mice, Mice, Inbred C57BL, Mice, Transgenic, Polyubiquitin chemistry, Adaptor Proteins, Signal Transducing metabolism, B-Lymphocytes immunology, Lymphocyte Activation immunology, MAP Kinase Kinase Kinases physiology, Polyubiquitin metabolism

Abstract

Polyubiquitination of proteins plays a critical role in the activation of immune cells. K63-linked polyubiquitin-binding proteins TGF-β-activated kinase 1 (TAK1)-binding protein (TAB)2 and TAB3 are implicated in NF-κB signaling via TAK1 activation. However, TAB2 alone is dispensable for NF-κB activation in embryonic fibroblasts, and the functional roles of TAB2 and TAB3 in immune cells has yet to be clarified. In this study, we demonstrate that TAB2 and TAB3 are essential for B cell activation leading to Ag-specific Ab responses, as well as B-1 and marginal zone B cell development. TAB2 and TAB3 are critical for the activation of MAPKs, especially ERK, but not NF-κB, in response to TLR and CD40 stimulation in B cells. Surprisingly, TAB2 and TAB3 are dispensable for TAK1 activation in B cells, indicating that TAB2 and TAB3 activate MAPKs via a pathway independent of TAK1. In contrast to B cells, macrophages lacking TAB2 and TAB3 did not show any defects in the cytokine production and the signaling pathway in response to TLR stimulation. Furthermore, TAB2 and TAB3 were dispensable for TNF-induced cytokine production in embryonic fibroblasts. Thus, TAB2- and TAB3-mediated K63-linked polyubiquitin recognition controls B cell activation via MAPKs, but not the TAK1/NF-κB axis.

Published

2013