Your search keyword '"Antibody Formation genetics"' showing total 20 results

1. Comprehensive viromewide antibody responses by systematic epitope scanning after hematopoietic cell transplantation.

Author

Bender Ignacio RA, Dasgupta S, Stevens-Ayers T, Kula T, Hill JA, Lee SJ, Mielcarek M, Duerr A, Elledge SJ, and Boeckh M

Subjects

Adult, Antibodies, Viral blood, Antibody Formation genetics, Cytomegalovirus immunology, Female, Follow-Up Studies, Graft vs Host Disease etiology, HLA Antigens genetics, HLA Antigens immunology, Humans, Male, Middle Aged, Postoperative Period, Tissue Donors, Transplant Recipients, Transplantation, Homologous, Antibodies, Viral immunology, Antibody Formation immunology, Epitopes immunology, Hematopoietic Stem Cell Transplantation adverse effects, Immunity, Humoral

Abstract

Further insight into humoral viral immunity after hematopoietic cell transplantation (HCT) could have potential impact on donor selection or monitoring of patients. Currently, estimation of humoral immune recovery is inferred from lymphocyte counts or immunoglobulin levels and does not address vulnerability to specific viral infections. We interrogated the viral antibody repertoire before and after HCT using a novel serosurvey (VirScan) that detects immunoglobulin G responses to 206 viruses. We performed VirScan on cryopreserved serum from pre-HCT and 30, 100, and 365 days after myeloablative HCT from 37 donor-recipient pairs. We applied ecologic metrics (α- and β-diversity) and evaluated predictors of metrics and changes over time. Donor age and donor/recipient cytomegalovirus (CMV) serostatus and receipt systemic glucocorticoids were most strongly associated with VirScan metrics at day 100. Other clinical characteristics, including pre-HCT treatment and conditioning, did not affect antiviral repertoire metrics. The recipient repertoire was most similar (pairwise β-diversity) to that of donor at day 100, but more similar to pre-HCT self by day 365. Gain or loss of epitopes to common viruses over the year post-HCT differed by donor and recipient pre-HCT serostatus, with highest gains in naive donors to seropositive recipients for several human herpesviruses and adenoviruses. We used VirScan to highlight contributions of donor and recipient to antiviral humoral immunity and evaluate longitudinal changes. This work builds a foundation to test whether such systematic profiling could serve as a biomarker of immune reconstitution, predict clinical events after HCT, or help refine selection of optimal donors., (© 2019 by The American Society of Hematology.)

Published

2019

2. MicroRNA-17-92 is required for T-cell and B-cell pathogenicity in chronic graft-versus-host disease in mice.

Author

Wu Y, Schutt S, Paz K, Zhang M, Flynn RP, Bastian D, Sofi MH, Nguyen H, Dai M, Liu C, Chang YJ, Blazar BR, and Yu XZ

Subjects

Animals, Antibody Formation genetics, Autoantibodies genetics, Autoantibodies immunology, Bronchiolitis Obliterans genetics, Bronchiolitis Obliterans pathology, Disease Models, Animal, Germinal Center immunology, Germinal Center pathology, Graft vs Host Disease genetics, Graft vs Host Disease pathology, Lymphocyte Activation genetics, Mice, Mice, Knockout, MicroRNAs genetics, Plasma Cells pathology, Scleroderma, Diffuse genetics, Scleroderma, Diffuse pathology, Th1 Cells pathology, Th17 Cells pathology, Bronchiolitis Obliterans immunology, Graft vs Host Disease immunology, MicroRNAs immunology, Plasma Cells immunology, Scleroderma, Diffuse immunology, Th1 Cells immunology, Th17 Cells immunology

Abstract

Chronic graft-versus-host disease (cGVHD) is characterized as autoimmune-like fibrosis and antibody production mediated by pathogenic T cells and B cells. MicroRNA-17-92 (miR-17-92) influences the survival, differentiation, and function of lymphocytes in cancer, infections, and autoimmunity. To determine whether miR-17-92 regulates T- and B-cell responses in cGVHD, we generated mice conditionally deficient for miR-17-92 in T cells, B cells, or both. Using murine models of allogeneic bone marrow transplantation, we demonstrate that expression of miR-17-92 in donor T and B cells is essential for the induction of both scleroderma and bronchiolitis obliterans in cGVHD. Mechanistically, miR-17-92 expressed in T cells not only enhances the differentiation of pathogenic T helper 1 (Th1) and Th17 cells, but also promotes the generation of follicular Th cells, germinal center (GC) B cells, and plasma cells. In B cells, miR-17-92 expression is required for autoantibody production and immunoglobulin G deposition in the skin. Furthermore, we evaluated a translational approach using antagomirs specific for either miR-17 or miR-19, key members in miR-17-92 cluster. In a lupus-like cGVHD model, systemic administration of anti-miR-17, but not anti-miR-19, alleviates clinical manifestations and proteinuria incidence in recipients through inhibiting donor lymphocyte expansion, B-cell activation, and GC responses. Blockade of miR-17 also ameliorates skin damage by reducing Th17 differentiation in a scleroderma-cGVHD model. Taken together, our work reveals that miR-17-92 is required for T-cell and B-cell differentiation and function, and thus for the development of cGVHD. Furthermore, pharmacological inhibition of miR-17 represents a potential therapeutic strategy for the prevention of cGVHD., (© 2018 by The American Society of Hematology.)

Published

2018

3. Endemic Burkitt lymphoma is associated with strength and diversity of Plasmodium falciparum malaria stage-specific antigen antibody response.

Author

Aka P, Vila MC, Jariwala A, Nkrumah F, Emmanuel B, Yagi M, Palacpac NM, Periago MV, Neequaye J, Kiruthu C, Tougan T, Levine PH, Biggar RJ, Pfeiffer RM, Bhatia K, Horii T, Bethony JM, and Mbulaiteye SM

Subjects

Adolescent, Animals, Antibody Specificity immunology, Antigens, Protozoan immunology, Burkitt Lymphoma complications, Case-Control Studies, Child, Child, Preschool, Endemic Diseases, Female, Genetic Variation immunology, Genetic Variation physiology, Humans, Infant, Infant, Newborn, Life Cycle Stages genetics, Life Cycle Stages immunology, Malaria, Falciparum immunology, Male, Plasmodium falciparum genetics, Plasmodium falciparum growth & development, Antibody Formation genetics, Burkitt Lymphoma epidemiology, Burkitt Lymphoma immunology, Malaria, Falciparum epidemiology, Malaria, Falciparum parasitology, Plasmodium falciparum immunology

Abstract

Endemic Burkitt lymphoma (eBL) is linked to Plasmodium falciparum (Pf) infection geographically, but evidence from individual-level studies is limited. We investigated this issue among 354 childhood eBL cases and 384 age-, sex-, and location-matched controls enrolled in Ghana from 1965 to 1994. Immunoglobulin G1 (IgG1) and immunoglobulin G3 (IgG3) antibodies to antigens diagnostic of recent infection Pf histidine-rich protein-II (HRP-II) and 6NANP, Pf-vaccine candidates SE36 and 42-kDa region of the 3D7 Pf merozoite surface protein-1 (MSP-1), and tetanus toxoid were measured by indirect enzyme-linked immunoassay. Odds ratios (ORs) and 95% confidence intervals (CIs) for association with eBL were estimated using unconditional logistic regression. After adjustments, eBL was positively associated with HRP-IIIgG3 seropositivity (adjusted OR: 1.60; 95% CI 1.08-2.36) and inversely associated with SE36IgG1 seropositivity (adjusted OR: 0.37; 95% CI 0.21-0.64) and with tetanus toxoidIgG3 levels equal or higher than the mean (adjusted OR: 0.46; 95% CI 0.32-0.66). Anti-MSP-1IgG3 and anti-6NANPIgG3 were indeterminate. eBL risk was potentially 21 times higher (95% CI 5.8-74) in HRP-IIIgG3-seropositive and SE36IgG1-seronegative responders compared with HRP-IIIgG3-seronegative and SE36IgG1-seropositive responders. Our results suggest that recent malaria may be associated with risk of eBL but long-term infection may be protective.

Published

2013

4. KAP1 regulates gene networks controlling mouse B-lymphoid cell differentiation and function.

Author

Santoni de Sio FR, Massacand J, Barde I, Offner S, Corsinotti A, Kapopoulou A, Bojkowska K, Dagklis A, Fernandez M, Ghia P, Thomas JH, Pinschewer D, Harris N, and Trono D

Subjects

Animals, Antibody Formation genetics, Antibody Formation immunology, B-Lymphocytes immunology, B-Lymphocytes metabolism, Bacterial Proteins genetics, Cell Differentiation immunology, Cell Differentiation physiology, Chromatin metabolism, Epigenesis, Genetic genetics, Epigenesis, Genetic immunology, Epigenesis, Genetic physiology, Gene Expression Profiling, Gene Expression Regulation, Gene Regulatory Networks genetics, Gene Regulatory Networks physiology, Luminescent Proteins genetics, Lymphocyte Count, Lymphocytes immunology, Lymphocytes metabolism, Mice, Mice, Inbred C57BL, Mice, Transgenic, Microarray Analysis, Nuclear Proteins genetics, Nuclear Proteins metabolism, Repressor Proteins genetics, Repressor Proteins metabolism, Tripartite Motif-Containing Protein 28, B-Lymphocytes physiology, Cell Differentiation genetics, Lymphocytes physiology, Nuclear Proteins physiology, Repressor Proteins physiology

Abstract

Chromatin remodeling is fundamental for B-cell differentiation. In the present study, we explored the role of KAP1, the cofactor of KRAB-ZFP transcriptional repressors, in this process. B-lymphoid-specific Kap1-KO mice displayed reduced numbers of mature B cells, lower steady-state levels of Abs, and accelerated rates of decay of neutralizing Abs after viral immunization. Transcriptome analyses of Kap1-deleted B splenocytes revealed an up-regulation of PTEN, the enzymatic counteractor of PIK3 signaling, and of genes encoding DNA-damage response factors, cell-cycle regulators, and chemokine receptors. ChIP/seq studies established that KAP1 bound at or close to several of these genes and controlled chromatin status at their promoters. Genome wide, KAP1 binding sites lacked active B cell-specific enhancers and were enriched in repressive histone marks, further supporting a role for this molecule in gene silencing in vivo. Likely responsible for tethering KAP1 to at least some of these targets, a discrete subset of KRAB-ZFPs is enriched in B lymphocytes. Our results therefore reveal the role of KRAB/KAP1-mediated epigenetic regulation in B-cell development and homeostasis.

Published

2012

5. TACI deficiency impairs sustained Blimp-1 expression in B cells decreasing long-lived plasma cells in the bone marrow.

Author

Tsuji S, Cortesão C, Bram RJ, Platt JL, and Cascalho M

Subjects

Animals, Antibody Formation genetics, B-Lymphocytes immunology, B-Lymphocytes physiology, Bone Marrow metabolism, Bone Marrow physiology, Bone Marrow Cells metabolism, Bone Marrow Cells physiology, Cell Count, Cell Proliferation, Cells, Cultured, Cellular Senescence genetics, Cellular Senescence physiology, Down-Regulation genetics, Gene Expression, Mice, Mice, Inbred C57BL, Mice, Knockout, Plasma Cells metabolism, Positive Regulatory Domain I-Binding Factor 1, Transcription Factors metabolism, Transmembrane Activator and CAML Interactor Protein physiology, B-Lymphocytes metabolism, Bone Marrow Cells cytology, Plasma Cells cytology, Transcription Factors genetics, Transmembrane Activator and CAML Interactor Protein genetics

Abstract

Deficiencies in transmembrane activator and CAML interactor (TACI) result in common variable immune deficiency, a syndrome marked by recurrent infections with encapsulated microorganisms, impaired production of antibodies, and lymphoproliferation. How TACI promotes antibody production and inhibits lymphoproliferation is not understood. To answer this question, we studied the generation of immunity to protein antigens in both TACI-deficient and TACI-proficient mice. We show that TACI promotes sustained Blimp-1 expression by B cells responding to antigen, which in turn limits B-cell clonal expansion and facilitates differentiation of long-lived antibody-secreting cells. Short-term IgG secretion occurs independently of TACI as DNA double-strand breaks associated with isotype class switching induce Blimp-1 transiently, independently of TACI. Our results showing that TACI induces and maintains Blimp-1 provide, for the first time, a unified molecular and cellular mechanism explaining the primary features of common variable immune deficiency, exquisite vulnerability to infection with encapsulated organisms, lymphoproliferation, and hypogammaglobulinemia.

Published

2011

6. Maintenance and break of immune tolerance against human factor VIII in a new transgenic hemophilic mouse model.

Author

van Helden PM, Unterthurner S, Hermann C, Schuster M, Ahmad RU, Schiviz AN, Weiller M, Antoine G, Turecek PL, Muchitsch EM, Schwarz HP, and Reipert BM

Subjects

Animals, Antibody Formation genetics, Antibody Formation physiology, Disease Models, Animal, Factor VIII antagonists & inhibitors, Female, Hemophilia A immunology, Hemophilia A pathology, Humans, Immune Tolerance physiology, Immunologic Memory physiology, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Models, Biological, Species Specificity, Factor VIII genetics, Factor VIII immunology, Hemophilia A genetics, Immune Tolerance genetics, Immunologic Memory genetics

Abstract

Replacement of the missing factor VIII (FVIII) is the current standard of care for patients with hemophilia A. However, the short half-life of FVIII makes frequent treatment necessary. Current efforts focus on the development of longer-acting FVIII concentrates by introducing chemical and genetic modifications to the protein. Any modification of the FVIII protein, however, risks increasing its immunogenic potential to induce neutralizing antibodies (FVIII inhibitors), and this is one of the major complications in current therapy. It would be highly desirable to identify candidates with a high risk for increased immunogenicity before entering clinical development to minimize the risk of exposing patients to such altered FVIII proteins. In the present study, we describe a transgenic mouse line that expresses a human F8 cDNA. This mouse is immunologically tolerant to therapeutic doses of native human FVIII but is able to mount an antibody response when challenged with a modified FVIII protein that possesses altered immunogenic properties. In this situation, immunologic tolerance breaks down and antibodies develop that recognize both the modified and the native human FVIII. The applicability of this new model for preclinical immunogenicity assessment of new FVIII molecules and its potential use for basic research are discussed.

Published

2011

7. Constitutive reductions in mTOR alter cell size, immune cell development, and antibody production.

Author

Zhang S, Readinger JA, DuBois W, Janka-Junttila M, Robinson R, Pruitt M, Bliskovsky V, Wu JZ, Sakakibara K, Patel J, Parent CA, Tessarollo L, Schwartzberg PL, and Mock BA

Subjects

Animals, B-Lymphocytes metabolism, Body Size genetics, Cell Differentiation genetics, Cell Differentiation immunology, Cell Lineage genetics, Cell Lineage immunology, Cell Size, Down-Regulation immunology, Down-Regulation physiology, Gene Knockdown Techniques, Mice, Mice, Inbred BALB C, Mice, Transgenic, Organ Size genetics, Spleen anatomy & histology, Spleen metabolism, Antibody Formation genetics, B-Lymphocytes cytology, B-Lymphocytes physiology, TOR Serine-Threonine Kinases genetics

Abstract

Mammalian TOR (mTOR) regulates cell growth, proliferation, and migration. Because mTOR knock-outs are embryonic lethal, we generated a viable hypomorphic mouse by neo-insertion that partially disrupts mTOR transcription and creates a potential physiologic model of mTORC1/TORC2 inhibition. Homozygous knock-in mice exhibited reductions in body, organ, and cell size. Although reductions in most organ sizes were proportional to decreased body weight, spleens were disproportionately smaller. Decreases in the total number of T cells, particularly memory cells, and reduced responses to chemokines suggested alterations in T-cell homing/homeostasis. T-cell receptor-stimulated T cells proliferated less, produced lower cytokine levels, and expressed FoxP3. Decreased neutrophil numbers were also observed in the spleen, despite normal development and migration in the bone marrow. However, B-cell effects were most pronounced, with a partial block in B-cell development in the bone marrow, altered splenic populations, and decreases in proliferation, antibody production, and migration to chemokines. Moreover, increased AKT(Ser473) phosphorylation was observed in activated B cells, reminiscent of cancers treated with rapamycin, and was reduced by a DNA-pk inhibitor. Thus, mTOR is required for the maturation and differentiation of multiple immune cell lineages. These mice provide a novel platform for studying the consequences of constitutively reduced mTORC1/TORC2 activity.

Published

2011

8. IL-6 increases B-cell IgG production in a feed-forward proinflammatory mechanism to skew hematopoiesis and elevate myeloid production.

Author

Maeda K, Mehta H, Drevets DA, and Coggeshall KM

Subjects

Aging genetics, Aging immunology, Animals, Antibody Formation genetics, Antigen-Antibody Complex genetics, Antigen-Antibody Complex immunology, Antigen-Antibody Complex metabolism, B-Lymphocytes metabolism, Cells, Cultured, Immunoglobulin G biosynthesis, Inflammation genetics, Inflammation immunology, Inflammation metabolism, Inositol Polyphosphate 5-Phosphatases, Interleukin-6 genetics, Interleukin-6 metabolism, Leukocyte Common Antigens genetics, Leukocyte Common Antigens immunology, Leukocyte Common Antigens metabolism, Macrophages, Peritoneal immunology, Macrophages, Peritoneal metabolism, Mice, Mice, Knockout, Myelopoiesis genetics, Phosphoric Monoester Hydrolases genetics, Phosphoric Monoester Hydrolases metabolism, Receptors, IgG genetics, Receptors, IgG immunology, Receptors, IgG metabolism, Antibody Formation immunology, B-Lymphocytes immunology, Immunoglobulin G immunology, Interleukin-6 immunology, Myelopoiesis immunology, Phosphoric Monoester Hydrolases immunology

Abstract

Src homology 2 domain-containing inositol 5-phosphatase (SHIP(-/-)) animals display an age-related increase in interleukin-6 (IL-6), a decrease in B lymphopoiesis, and an elevation in myelopoiesis. We investigated the origin of the IL-6 production and show that it is largely produced by peritoneal and splenic macrophages. IL-6 production by these macrophages is not a direct result of the loss of SHIP: IL-6 production is not spontaneous, is absent from bone marrow-derived macrophages, declines with prolonged culture of macrophages, and requires a stimulus present in vivo. The IL-6-rich peritoneal cavity of SHIP(-/-) mice shows more than 700-fold more immunoglobulin G (IgG) than wild-type, approximately 20% of which is aggregated or in an immune complex and contains B220(+) cells that secrete IgG. The SHIP-deficient peritoneal macrophages show evidence of IgG receptor stimulation. Animals lacking both the signal-transducing gamma-chain of IgG receptors and SHIP or Ig and SHIP produce less IL-6. The data indicate a feed-forward process in which peripheral macrophages, responding through IgG receptors to secreted IgG, produce IL-6, to support further B-cell production of IgG. Because of the proinflammatory phenotype of SHIP(-/-) animals, these findings emphasize the importance of IL-6-neutralizing strategies in autoimmune and proinflammatory diseases.

Published

2010

9. Interleukin-6/STAT3 signaling regulates the ability of naive T cells to acquire B-cell help capacities.

Author

Eddahri F, Denanglaire S, Bureau F, Spolski R, Leonard WJ, Leo O, and Andris F

Subjects

Animals, Antibody Formation drug effects, Antibody Formation genetics, B-Lymphocytes drug effects, Interleukin-6 genetics, Interleukin-6 pharmacology, Interleukins metabolism, Interleukins physiology, Lymphocyte Activation genetics, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Knockout, Receptors, CXCR5 metabolism, STAT3 Transcription Factor genetics, Signal Transduction genetics, Signal Transduction physiology, T-Lymphocytes drug effects, T-Lymphocytes immunology, T-Lymphocytes, Helper-Inducer immunology, B-Lymphocytes immunology, Cell Differentiation immunology, Interleukin-6 physiology, STAT3 Transcription Factor physiology, T-Lymphocytes physiology, T-Lymphocytes, Helper-Inducer physiology

Abstract

The conditions leading to the activation/differentiation of T-helper (Th) cells dedicated for B-cell antibody production are still poorly characterized. We now demonstrate that interleukin-6 (IL-6) promotes the differentiation of naive T lymphocytes into helper cells able to promote B-cell activation and antibody secretion. IL-6-driven acquisition of B-cell help capacity requires expression of the signal transducer and activator of transcription 3 (STAT3), but not STAT4 or STAT6 transcription factors, suggesting that the ability to provide help to B cells is not restricted to a well-defined Th1 or Th2 effector population. T cell-specific STAT3-deficient mice displayed reduced humoral responses in vivo that could not be related to an altered expansion of CXCR5-expressing helper T cells. IL-6 was shown to promote IL-21 secretion, a cytokine that was similarly found to promote the differentiation of naive T cells into potent B-cell helper cells. Collectively, these data indicate that the ability to provide B-cell help is regulated by IL-6/IL-21 through STAT3 activation, independently of Th1, Th2, Th17, or follicular helper T cell (T(FH)) differentiation.

Published

2009

10. PARP-14, a member of the B aggressive lymphoma family, transduces survival signals in primary B cells.

Author

Cho SH, Goenka S, Henttinen T, Gudapati P, Reinikainen A, Eischen CM, Lahesmaa R, and Boothby M

Subjects

Animals, Antibody Formation drug effects, Antibody Formation genetics, Apoptosis genetics, Apoptosis immunology, B-Lymphocytes drug effects, B-Lymphocytes metabolism, Cell Differentiation drug effects, Cell Differentiation genetics, Cell Survival genetics, Female, Immunoglobulin A immunology, Interleukin-4 pharmacology, Mice, Mice, Inbred C57BL, Mice, Knockout, Multigene Family, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Neoplasm Proteins physiology, Poly(ADP-ribose) Polymerases chemistry, Poly(ADP-ribose) Polymerases genetics, Poly(ADP-ribose) Polymerases metabolism, Sequence Homology, B-Lymphocytes physiology, Poly(ADP-ribose) Polymerases physiology

Abstract

Poly(ADP-ribos)ylation is one of the longest-known but most enigmatic posttranslational modifications transducing specific signals. The enzyme responsible for the majority of poly(ADP-ribose) polymerization in cells, PARP-1, promotes DNA repair but also mediates a caspase-independent form of apoptosis in response to stressors such as irradiation. However, the biologic function of most other PARPs is not known. Macro-PARPs constitute one branch of the large family of PARP-like proteins also designated as B aggressive lymphoma proteins (BAL1, 2a/2b, 3, or PARP-9, PARP-14, and PARP-15). To elucidate biologic role(s) of a BAL-family macro-PARP, we analyzed mice deficient in PARP-14, a binding partner of the IL-4-induced transcription factor Stat6. We show here that PARP-14 plays a fundamental role mediating protection against apoptosis in IL-4-treated B cells, including that after DNA damage, and mediates IL-4 effects on the levels of gene products that regulate cell survival, proliferation, and lymphomagenesis. Collectively, the results establish that PARP-14 mediates regulation of gene expression and lymphocyte physiology by IL-4 and has a function distinct from PARP-1. Furthermore, the findings suggest mechanisms by which BAL-family proteins might influence pathologic processes involving B lymphocytes.

Published

2009

11. Triggering TLR7 in mice induces immune activation and lymphoid system disruption, resembling HIV-mediated pathology.

Author

Baenziger S, Heikenwalder M, Johansen P, Schlaepfer E, Hofer U, Miller RC, Diemand S, Honda K, Kundig TM, Aguzzi A, and Speck RF

Subjects

Acquired Immunodeficiency Syndrome genetics, Acquired Immunodeficiency Syndrome pathology, Animals, Antibody Formation drug effects, Antibody Formation genetics, Antibody Formation immunology, B-Lymphocytes pathology, Female, Humans, Imidazoles immunology, Immunoglobulin G immunology, Male, Membrane Glycoproteins genetics, Mice, Mice, Knockout, RNA, Viral genetics, Signal Transduction drug effects, Signal Transduction genetics, Signal Transduction immunology, Toll-Like Receptor 7 genetics, Toll-Like Receptor 8 agonists, Toll-Like Receptor 8 genetics, Toll-Like Receptor 8 immunology, Acquired Immunodeficiency Syndrome immunology, B-Lymphocytes immunology, HIV-1, Imidazoles pharmacology, Membrane Glycoproteins agonists, Membrane Glycoproteins immunology, RNA, Viral immunology, Toll-Like Receptor 7 agonists, Toll-Like Receptor 7 immunology

Abstract

Chronic immune activation is a major cause for progressive immunodeficiency in human immunodeficiency virus type-1 (HIV) infection. The underlying trigger, however, remains largely unknown. HIV single-stranded RNA is a potent immune activator by triggering Toll-like receptor (TLR) 7/8. Thus, we hypothesized that sustained TLR7 triggering induces chronic immune activation and thereby contributes to progressive immunodeficiency. We used the synthetic compound R848 or a mixture of uridine-rich HIV single-stranded (ss) RNA oligonucleotides--both are potent TLR7/8 agonists--to explore the effects of sustained TLR7 triggering on the murine lymphoid system. Sustained TLR7 triggering induced an immunopathology reminiscent of progressive lymphoid destruction in HIV disease; we observed lymphopenia, elevated proinflammatory cytokines, splenomegaly, contracted lymphoid subsets, and lymphoid microarchitecture alteration with reduced marginal zone B-lymphocytes. Upon exposure to inactivated vesiculo-stomatitis virus, antibody production was abolished, although splenic lymphocytes were activated and total IgG was elevated. Our data imply that HIV itself may directly contribute to immune activation and dysfunction by stimulating TLR7. Thus, manipulation of TLR7 signaling may be a potential strategy to reduce chronic hyper-immune activation and, thereby, disease progression in HIV infection.

Published

2009

12. Clinical and immunologic consequences of a somatic reversion in a patient with X-linked severe combined immunodeficiency.

Author

Speckmann C, Pannicke U, Wiech E, Schwarz K, Fisch P, Friedrich W, Niehues T, Gilmour K, Buiting K, Schlesier M, Eibel H, Rohr J, Superti-Furga A, Gross-Wieltsch U, and Ehl S

Subjects

B-Lymphocytes immunology, B-Lymphocytes pathology, Child, Preschool, Epithelial Cells immunology, Epithelial Cells pathology, Hematopoietic Stem Cell Transplantation, Humans, Interleukin Receptor Common gamma Subunit immunology, Killer Cells, Natural immunology, Killer Cells, Natural pathology, Lymphoid Progenitor Cells immunology, Lymphoid Progenitor Cells pathology, Lymphopenia immunology, Lymphopenia pathology, Lymphopenia therapy, Male, Receptors, Antigen, T-Cell, gamma-delta genetics, Receptors, Antigen, T-Cell, gamma-delta immunology, T-Lymphocytes immunology, T-Lymphocytes pathology, X-Linked Combined Immunodeficiency Diseases immunology, X-Linked Combined Immunodeficiency Diseases pathology, X-Linked Combined Immunodeficiency Diseases therapy, Antibody Formation genetics, Interleukin Receptor Common gamma Subunit genetics, Lymphopenia genetics, Point Mutation, X-Linked Combined Immunodeficiency Diseases genetics

Abstract

X-linked severe combined immunodeficiency is a life-threatening disorder caused by mutations in the gene encoding the interleukin-2 receptor gamma chain (IL2RG). Hypomorphic mutations and reversion of mutations in subpopulations of cells can result in variant clinical phenotypes, making diagnosis and treatment difficult. We describe a 5-year-old boy with mild susceptibility to infection who was investigated for a mutation in IL2RG due to persistent natural killer (NK)- and T-cell lymphopenia. A functionally relevant novel T466C point mutation was found in B, NK, and epithelial cells, whereas alpha/beta and gamma/delta T cells showed the normal gene sequence, suggesting reversion of the mutation in a common T-cell precursor. This genetic correction in T cells resulted in a diverse T-cell repertoire and significant immunity despite failure to produce specific antibodies linked to an intrinsic defect of mutant B cells. These observations confirm the potential of revertant T-cell precursors to reconstitute immune function, but questions remain on the longevity of revertant cells implicating the need for careful follow up and early consideration of hematopoietic stem cell transplantation (HSCT).

Published

2008

13. Rapidly induced, T-cell independent xenoantibody production is mediated by marginal zone B cells and requires help from NK cells.

Author

Li S, Yan Y, Lin Y, Bullens DM, Rutgeerts O, Goebels J, Segers C, Boon L, Kasran A, De Vos R, Dewolf-Peeters C, Waer M, and Billiau AD

Subjects

Animals, B-Lymphocytes cytology, CD40 Ligand antagonists & inhibitors, CD40 Ligand immunology, Immunoglobulin M immunology, Killer Cells, Natural cytology, Mice, Mice, Knockout, Mice, Nude, T-Lymphocytes immunology, Transplantation, Heterologous immunology, Antibodies, Heterophile immunology, Antibody Formation genetics, B-Lymphocytes immunology, Cell Communication immunology, Killer Cells, Natural immunology, Models, Immunological

Abstract

Xenoantibody production directed at a wide variety of T lymphocyte-dependent and T lymphocyte-independent xenoantigens remains the major immunologic obstacle for successful xenotransplantation. The B lymphocyte subpopulations and their helper factors, involved in T-cell-independent xenoantibody production are only partially understood, and their identification will contribute to the clinical applicability of xenotransplantation. Here we show, using models involving T-cell-deficient athymic recipient mice, that rapidly induced, T-cell-independent xenoantibody production is mediated by marginal zone B lymphocytes and requires help from natural killer (NK) cells. This collaboration neither required NK-cell-mediated IFN-gamma production, nor NK-cell-mediated cytolytic killing of xenogeneic target cells. The T-cell-independent IgM xenoantibody response could be partially suppressed by CD40L blockade.

Published

2007

14. M17, a gene specific for germinal center (GC) B cells and a prognostic marker for GC B-cell lymphomas, is dispensable for the GC reaction in mice.

Author

Schenten D, Egert A, Pasparakis M, and Rajewsky K

Subjects

Animals, Antibody Formation genetics, Biomarkers, Tumor deficiency, Germinal Center pathology, Humans, Immunoglobulin Variable Region genetics, Immunoglobulin Variable Region immunology, Intracellular Signaling Peptides and Proteins, Lymphoma, B-Cell genetics, Lymphoma, B-Cell pathology, Lymphoma, Large B-Cell, Diffuse genetics, Lymphoma, Large B-Cell, Diffuse pathology, Mice, Mice, Mutant Strains, Microfilament Proteins, Neoplasm Proteins deficiency, Prognosis, Somatic Hypermutation, Immunoglobulin genetics, T-Lymphocytes immunology, T-Lymphocytes pathology, Antibody Formation immunology, Biomarkers, Tumor immunology, Germinal Center immunology, Lymphoma, B-Cell immunology, Lymphoma, Large B-Cell, Diffuse immunology, Neoplasm Proteins immunology, Somatic Hypermutation, Immunoglobulin immunology

Abstract

In T-cell-dependent antibody responses, antigen-specific B cells undergo a phase of secondary antibody diversification in germinal centers (GCs). Somatic hypermutation (SHM) introduces mutations into the rearranged immunoglobulin (Ig) variable (V) region genes, and class-switch recombination (CSR) alters the Ig heavy (H) chain constant region. Aberrant SHM or CSR is thought to contribute to the development of GC-derived B-cell malignancies. Diffuse large B-cell lymphomas (DLBCLs) are a heterogeneous group of such GC-derived tumors. Based on their gene expression profile, DLBCLs can be divided into activated B-cell-like and GC-like subgroups. The human gene HGAL is predominantly expressed in GCs. It is also part of the gene expression signature of GC-like DLBCL, and its high expression in DLBCL has been associated with a better clinical prognosis. We have generated mice deficient of the HGAL homologue M17 in order to investigate its functional significance. The mutant animals form normal GCs, undergo efficient CSR and SHM, and mount T-cell-dependent antibody responses similar to wild-type controls. Thus, M17 is dispensable for the GC reaction, and its potential function in the pathogenesis of DLBCL remains elusive.

Published

2006

15. Correction of canine X-linked severe combined immunodeficiency by in vivo retroviral gene therapy.

Author

Ting-De Ravin SS, Kennedy DR, Naumann N, Kennedy JS, Choi U, Hartnett BJ, Linton GF, Whiting-Theobald NL, Moore PF, Vernau W, Malech HL, and Felsburg PJ

Subjects

Animals, Antibody Formation genetics, Antibody Formation immunology, B-Lymphocytes immunology, Dogs, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells immunology, Immunization, Receptors, Interleukin-2 immunology, Recovery of Function immunology, Retroviridae, Severe Combined Immunodeficiency genetics, Severe Combined Immunodeficiency immunology, T-Lymphocytes immunology, Transplantation, Autologous, Genetic Therapy methods, Genetic Vectors administration & dosage, Receptors, Interleukin-2 genetics, Recovery of Function genetics, Severe Combined Immunodeficiency therapy, Transduction, Genetic methods

Abstract

X-linked severe combined immunodeficiency (XSCID) is characterized by profound immunodeficiency and early mortality, the only potential cure being hematopoietic stem cell (HSC) transplantation or gene therapy. Current clinical gene therapy protocols targeting HSCs are based upon ex vivo gene transfer, potentially limited by the adequacy of HSC harvest, transduction efficiencies of repopulating HSCs, and the potential loss of their engraftment potential during ex vivo culture. We demonstrate an important proof of principle by showing achievement of durable immune reconstitution in XSCID dogs following intravenous injection of concentrated RD114-pseudotyped retrovirus vector encoding the corrective gene, the interleukin-2 receptor gamma chain (gamma c). In 3 of 4 dogs treated, normalization of numbers and function of T cells were observed. Two long-term-surviving animals (16 and 18 months) showed significant marking of B lymphocytes and myeloid cells, normalization of IgG levels, and protective humoral immune response to immunization. There were no adverse effects from in vivo gene therapy, and in one dog that reached sexual maturity, sparing of gonadal tissue from gene transfer was demonstrated. This is the first demonstration that in vivo gene therapy targeting HSCs can restore both cellular and humoral immunity in a large-animal model of a fatal immunodeficiency.

Published

2006

16. Polymorphisms in the IL10 but not in the IL1beta and IL4 genes are associated with inhibitor development in patients with hemophilia A.

Author

Astermark J, Oldenburg J, Pavlova A, Berntorp E, and Lefvert AK

Subjects

Antibody Formation immunology, Autoantibodies immunology, Autoimmune Diseases etiology, Autoimmune Diseases immunology, Blood Coagulation Factor Inhibitors genetics, Blood Coagulation Factor Inhibitors immunology, Dinucleotide Repeats immunology, Factor VIII immunology, Female, Hemophilia A complications, Hemophilia A immunology, Humans, Interleukin-1 genetics, Interleukin-1 immunology, Interleukin-10 immunology, Interleukin-4 genetics, Interleukin-4 immunology, Male, Polymorphism, Restriction Fragment Length, Promoter Regions, Genetic immunology, Severity of Illness Index, Antibody Formation genetics, Autoimmune Diseases genetics, Chromosome Inversion, Dinucleotide Repeats genetics, Hemophilia A genetics, Interleukin-10 genetics, Promoter Regions, Genetic genetics

Abstract

The aim of the Malmö International Brother Study (MIBS) is to evaluate host genetic factors associated with the development of inhibitory antibodies in patients with hemophilia. Factor VIII gene mutations and genetic polymorphisms of the IL1beta, IL4, and IL10 genes, known to influence antibody production in autoimmune diseases, were analyzed in 164 patients (124 with severe, 26 with moderate, and 14 with mild disease) in 78 unrelated families with hemophilia A. Seventy-seven (47%) patients in 54 families had a history of inhibitors (57 high responding, 20 low responding). Inversions were found in 36 families (75 patients). There was no association between the development of inhibitor and the IL1beta Taq I RFLP alleles in exon 5 or the -590 C/T single nucleotide polymorphism (SNP) in the promoter region of IL4. There was, however, a strong association between an allele with 134 bp in one of the CA repeat microsatellites, IL10G, located in the promoter region of the IL10 gene, and the development of inhibitor (odds ratio [OR], 4.4; 95% confidence interval [95% CI], 2.1-9.5; P < .001). The association was consistent in the subgroup of families with severe hemophilia and inversions. IL10 is the first gene located outside the causative factor VIII gene mutation to be associated with inhibitor development.

Published

2006

17. Identification of 2 major loci linked to autoimmune hemolytic anemia in NZB mice.

Author

Kikuchi S, Amano H, Amano E, Fossati-Jimack L, Santiago-Raber ML, Moll T, Ida A, Kotzin BL, and Izui S

Subjects

Anemia, Hemolytic, Autoimmune etiology, Animals, Antibody Formation genetics, Autoantibodies genetics, Chromosomes, Mammalian, Coombs Test, Genetic Linkage, Male, Mice, Anemia, Hemolytic, Autoimmune genetics, Chromosome Mapping, Genetic Predisposition to Disease, Mice, Inbred NZB genetics

Abstract

Using a cohort of C57BL/6 (B6) x (NZB x B6)F1 backcross male mice bearing the Yaa (Y-linked autoimmune acceleration) mutation, we mapped and characterized the NZB-derived susceptibility loci predisposing to the development of autoimmune hemolytic anemia (AHA). Our analysis identified 2 major loci on NZB chromosome 7 and chromosome 1 linked with Coombs antierythrocyte autoantibody production, and their contributions were confirmed by the analysis of B6.Yaa mice (B6 mice bearing the Yaa mutation) congenic for each NZB-derived susceptibility interval. A newly identified Aia3 (autoimmune anemia 3) locus present on NZB chromosome 7 selectively regulated Coombs antibody responses, while the second locus, directly overlapping with Nba2 (NZB autoimmunity 2) on chromosome 1, promoted the development of AHA, likely as part of its effect on overall production of lupus autoantibodies. A higher incidence of Coombs antibody production in B6.Aia3 congenic mice (B6 mice bearing the NZB-Aia3 locus) than B6.Nba2 mice (B6 mice bearing the NZB-Nba2 locus) indicated a major role for Aia3 in AHA. Notably, lack of expansion of B1 cells in B6.Aia3 congenic mice argued against the involvement of this subset in AHA. Finally, our analysis of BC mice also demonstrated the presence of a B6-derived H2-linked locus on chromosome 17 that apparently regulated the production of Coombs antibodies as a result of its overall autoimmune promoting effect.

Published

2005

18. Mapping of genes that control the antibody response to human factor IX in mice.

Author

Lozier JN, Tayebi N, and Zhang P

Subjects

Adenoviridae, Adjuvants, Immunologic pharmacology, Animals, Chromosome Mapping, Enzyme-Linked Immunosorbent Assay, Factor IX genetics, Female, Gene Transfer Techniques, Genetic Vectors, Humans, Major Histocompatibility Complex, Male, Mice, Mice, Inbred A, Mice, Inbred C57BL, Polymorphism, Genetic, Antibody Formation genetics, Factor IX immunology, H-2 Antigens genetics

Abstract

We tested the hypothesis that the antibody response to human factor IX in mice is controlled by genetic factors, especially histocompatibility antigens. Seven inbred mouse strains were immunized against human factor IX by adenoviral gene transfer or serial injections of human factor IX protein. A/J mice had the highest antibody response and 2 C57 mouse strains had the lowest response. We used the adenovirus vector to immunize 26 recombinant inbred mouse strains (AXB and BXA) derived from A/J and C57BL/6J mice and observed highly significant linkage (logarithmic odds [LOD] scores approximately 4.8) for the polymorphic D17Mit62 marker that is 1 centimorgan ( approximately 300 000 base pair [bp]) from the mouse major histocompatibility complex (MHC) locus (H-2). Experiments in mice with chimeric MHC genes indicated that class IaK or class II H-2 (or both) genes were critical, but other genes contributed to the antibody response. Polymorphic markers from chromosomes 1 and 10 that are near important immunoregulatory genes such as interleukin 10 and the interferon-gamma gene show suggestive linkage (LOD scores of approximately 2.3-2.6) to the factor IX antibody response. This study confirms the hypothesis that H-2 (and other) genes control factor IX antibody development in mice and suggests their potential importance for factor IX antibody development in humans with hemophilia B.

Published

2005

19. Reduction of the inhibitory antibody response to human factor VIII in hemophilia A mice by mutagenesis of the A2 domain B-cell epitope.

Author

Parker ET, Healey JF, Barrow RT, Craddock HN, and Lollar P

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Antibody Formation genetics, Blood Coagulation, Epitopes genetics, Epitopes immunology, Hemophilia A blood, Humans, Mice, Mice, Transgenic, Molecular Sequence Data, Recombinant Proteins immunology, Sequence Alignment, Sequence Homology, Amino Acid, Swine, B-Lymphocytes immunology, Factor VIII genetics, Factor VIII immunology, Hemophilia A genetics, Hemophilia A immunology

Abstract

Approximately 25% of patients with hemophilia A develop inhibitory antibodies after treatment with factor VIII. Most of the inhibitory activity is directed against epitopes in the A2 and C2 domains. Anti-A2 inhibitory antibodies recognize a 25-residue segment bounded by R484-I508. Several antigenic residues in this segment have been identified, including R484, R489, and P492. The immunogenicity of purified recombinant B domain-deleted (BDD) human factor VIII molecules containing mutations at R484A/R489A or R484A/R489A/P492A was studied in hemophilia A mice. Inhibitory antibody titers in mice receiving the R484A/R489A/P492A mutant, but not the R484A/R489A mutant, were significantly lower than in mice receiving control human BDD factor VIII. The specific coagulant activity and the in vivo clearance and hemostatic efficacy in hemophilia A mice of the R484A/R489A/P492A mutant were indistinguishable from human BDD factor VIII. Thus, the inhibitory antibody response to human factor VIII can be reduced by mutagenesis of a B-cell epitope without apparent loss of function, suggesting that this approach may be useful for developing a safer form of factor VIII in patients with hemophilia A.

Published

2004

20. Transgenic overexpression of human IL-17E results in eosinophilia, B-lymphocyte hyperplasia, and altered antibody production.

Author

Kim MR, Manoukian R, Yeh R, Silbiger SM, Danilenko DM, Scully S, Sun J, DeRose ML, Stolina M, Chang D, Van GY, Clarkin K, Nguyen HQ, Yu YB, Jing S, Senaldi G, Elliott G, and Medlock ES

Subjects

Amino Acid Sequence, Animals, Antigens, CD19 analysis, B-Lymphocytes pathology, Base Sequence, Cloning, Molecular, Cytokines immunology, Eosinophilia genetics, Humans, Hyperplasia, Immunophenotyping, Interleukin-17 immunology, Lymph Nodes immunology, Mice, Mice, Transgenic, Molecular Sequence Data, Organ Size, RNA, Messenger genetics, Recombinant Proteins immunology, Sequence Alignment, Sequence Homology, Amino Acid, Spleen anatomy & histology, Spleen immunology, Transcription, Genetic, Antibody Formation genetics, B-Lymphocytes immunology, Cytokines genetics, Eosinophilia immunology, Interleukin-17 genetics

Abstract

We have identified and cloned a novel human cytokine with homology to cytokines of the interleukin-17 (IL-17) family, which we have termed human IL-17E (hIL-17E). With the identification of several IL-17 family members, it is critical to understand the in vivo function of these molecules. We have generated transgenic mice overexpressing hIL-17E using an apolipoprotein E (ApoE) hepatic promoter. These mice displayed changes in the peripheral blood, particularly, a 3-fold increase in total leukocytes consisting of increases in eosinophils, lymphocytes, and neutrophils. Splenomegaly and lymphoadenopathy were predominant and included marked eosinophil infiltrates and lymphoid hyperplasia. CCR3(+) eosinophils increased in the blood and lymph nodes of the transgenic mice by 50- and 300-fold, respectively. Eosinophils also increased 8- to 18-fold in the bone marrow and spleen, respectively. In the bone marrow, most of the eosinophils had an immature appearance. CD19(+) B cells increased 2- to 5-fold in the peripheral blood, 2-fold in the spleen, and 10-fold in the lymph nodes of transgenic mice, whereas CD4(+) T lymphocytes increased 2-fold in both blood and spleen. High serum levels of the cytokines IL-2, IL-4, IL-5, granulocyte colony-stimulating factor, eotaxin, and interferon gamma were observed. Consistent with B-lymphocyte increases, serum immunoglobulin (Ig) M, IgG, and IgE were significantly elevated. Antigenic challenge of the transgenic mice with keyhole limpet hemocyanin (KLH) resulted in a decrease in anti-KLH IgG accompanied by increases of anti-KLH IgA and IgE. In situ hybridization of transgenic tissues revealed that IL-17Rh1 (IL-17BR/Evi27), a receptor that binds IL-17E, is up-regulated. Taken together, these data indicate that IL-17E regulates hematopoietic and immune functions, stimulating the development of eosinophils and B lymphocytes. The fact that hIL-17E overexpression results in high levels of circulating eosinophils, IL-4, IL-5, eotaxin, and IgE suggests that IL-17E may be a proinflammatory cytokine favoring Th2-type immune responses.

Published

2002