Showing total 816 results

101. Blood monocytes, myeloid dendritic cells and the cytokines interleukin (IL)-7 and IL-15 maintain human CD4+ T memory cells with mixed helper/regulatory function.

Author

McKinlay, Adam, Radford, Kristen, Kato, Masato, Field, Ken, Gardiner, Damien, Khalil, Dalia, Burnell, Fiona, Hart, Derek, and Vuckovic, Slavica

Subjects

MONOCYTES, DENDRITIC cells, INTERLEUKINS, T cells, ANTIGENS, CELL proliferation

Abstract

The number and function of human T cells in the periphery are regulated by homeostatic signals received from antigen-presenting cells (APCs) and the common gamma chain (γc) cytokines interleukin (IL)-7 and IL-15. We found that, in the absence of introduced antigen, blood monocytes or myeloid dendritic cells (MDCs) in the presence of IL-7 and IL-15 (IL-7/IL-15) can regulate CD4+ T memory (Tm) cell numbers by polyclonal cell proliferation. The dynamics of CD4+ Tm cell proliferation, in the presence of IL-7/IL-15, was dependent on contact with MDCs and to a lesser extent on contact with monocytes. IL-7/IL-15 either alone or combined with monocytes or MDCs enhanced the proportion of CD4+ Tm cells with activated and effector phenotype and diminished the helper function of CD4+ Tm cells. These CD4+ Tm cells, preconditioned with IL-7/IL-15 alone or with monocytes or MDCs and IL-7/IL-15, reduced T cell-dependent immunoglobulin M (IgM) and IgG responses. This appeared to be a contact-dependent effect involving a reduction in antibody-producing CD27+ B memory cells, but contact-independent suppression by soluble factors also contributed to the antibody-producing capacity of CD27+ B memory cells. These results indicate that blood monocytes, MDCs and the cytokines IL-7/IL-15 contribute to homeostasis of CD4+ Tm cells by regulating their number, activation state and helper/suppressor (regulatory) function. In healthy individuals, this mode of regulating CD4+ Tm cell homeostasis may provide a basis for the control of autoimmune responses. [ABSTRACT FROM AUTHOR]

Published

2007

102. The fate of effector CD8 T cells in vivo is controlled by the duration of antigen stimulation.

Author

Xiaopei Huang and Yiping Yang

Subjects

T cells, ANTIGENS, IMMUNOTHERAPY, T cell receptors, CLINICAL immunology, IMMUNITY

Abstract

What controls the fate of the T-cell response remains incompletely defined. Gain of effector function facilitated by costimulation has been thought to be a crucial factor in determining the outcome of the T-cell response, i.e. long-term memory in the presence of costimulation versus tolerance induction in the absence of costimulation. In this study, we show that while costimulation or cognate CD4 helps to promote the acquisition of effector function during the initial phase of the CD8 T-cell response, the fate of effector CD8 T cells is controlled by the duration of subsequent antigenic stimulation. Effector CD8 T cells differentiate into memory cells only after clearance of antigen, whereas in the presence of persistent antigen, effector CD8 T cells are tolerized. Furthermore, protective immunity against tumour cannot develop in the persisting antigen environment. These results suggest that removal of persisting antigen by other means might be a prerequisite for effective immunotherapy in cancer. [ABSTRACT FROM AUTHOR]

Published

2006

103. Chemokine receptor expression and modulation by Mycobacterium tuberculosis antigens on mononuclear cells from human lymphoid tissues.

Author

Arias, Mauricio A., Pantoja, Adelis E., Jaramillo, Gabriela, Paris, Sara C., Shattock, Robin J., García, Luis F., and Griffin, George E.

Subjects

CHEMOKINES, MYCOBACTERIUM tuberculosis, ANTIGENS, MONONUCLEOSIS, LYMPHOID tissue, MACROPHAGES

Abstract

Chemokine receptor switching on lymphoid cells is an important factor regulating migration and homing, but little is known about the expression of such molecules during Mycobacterium tuberculosis infection in humans. We describe CCR2, CCR5 and CCR7 expression on human cells from blood, spleen and pulmonary hilar lymph nodes (PHLN) stimulated by M. tuberculosis antigens. CCR2 was not expressed by CD3+ cells regardless of the presence of antigen, but was highly expressed on CD14+ CD63+ monocytes/macrophages. CCR2 decreased on splenic monocytes/macrophages by nearly 50% in culture, independent of antigen, but remained high in blood and PHLN. CCR5 was low in CD3+ cells and was down-regulated by M. tuberculosis antigens on blood and splenic cells but not in PHLN. CCR5 was highly expressed on monocytes/macrophages and was down-regulated by M. tuberculosis antigens at 48 hr only in blood. Less than 15% of CD3+ cells from spleen and PHLN were CCR7+, whereas nearly 40% from blood expressed this receptor on primary isolation. However, CCR7 in PHLN increased in culture, independent of antigen. Monocytes/macrophages did not express CCR7. Thus, we characterize, for the first time, chemokine receptor expression and differential modulation by M. tuberculosis antigens on human mononuclear cells from spleen, blood and PHLN. Knowledge of chemokine receptor switching in human lymphoid tissue provides novel insight into mechanisms of the immune response to M. tuberculosis with potential effects on directing cell trafficking. [ABSTRACT FROM AUTHOR]

Published

2006

104. Expression levels of Mycobacterium tuberculosis antigen-encoding genes versus production levels of antigen-specific T cells during stationary level lung infection in mice.

Author

Rogerson, Brian J., Yu-Jin Jung, LaCourse, Ronald, Ryan, Lynn, Enright, Nicholas, and North, Robert J.

Subjects

MYCOBACTERIUM tuberculosis, TUBERCULOSIS, ANTIGENS, LUNG infections, TUBERCULIN, SEPTUM (Brain)

Abstract

Mycobacterium tuberculosis lung infection in mice was controlled at an approximately stationary level after 20 days of log linear growth. Onset of stationary level infection was associated with the generation by the host of T helper type 1 (Th1) immunity, as evidenced by the accumulation of CD4 Th1 cells specific for the early secretory antigen (ESAT-6) of M. tuberculsosis encoded by esat6, and for a mycolyl transferase (Ag85B) encoded by fbpB. CD4 T cells specific for these antigens were maintained at relatively high numbers throughout the course of infection. The number of CD4 T cells generated against ESAT-6 was larger than the number generated against Ag85B, and this was associated with a higher transcription level of esat6. The total number of transcripts of esat6 increased during the first 15 days of infection, after which it decreased and then approximately stabilized at 106·5 per lung. The total number of fbpB transcripts increased for 20 days of infection before decreasing and then approximately stabilizing at 104·8 per lung. The number of transcripts of esat6 per colony-forming unit of M. tuberculosis fell from 8·6 to 0·8 after day 15, and of fbpB from 0·3 to less than 0·02 after day 10, suggesting that at any given time during stationary level infection the latter gene was expressed by a very small percentage of bacilli. Expressed at an even lower level was an M. tuberculosis replication gene involved in septum formation ( ftsZ), indicating that there was no significant turnover of the M. tuberculosis population during stationary level infection. [ABSTRACT FROM AUTHOR]

Published

2006

105. Mechanisms of immune suppression by interleukin-10 and transforming growth factor-β: the role of T regulatory cells.

Author

Taylor, Alison, Verhagen, Johan, Blaser, Kurt, Akdis, Mübeccel, and Akdis, Cezmi A.

Subjects

IMMUNOSUPPRESSION, ALLERGENS, T cells, ANTIGENS, ALLERGIES, IMMUNOTHERAPY, LYMPHOKINES, ANTINEOPLASTIC agents

Abstract

Specific immune suppression and induction of tolerance are essential processes in the regulation and circumvention of immune defence. The balance between allergen-specific type 1 regulatory (Tr1) cells and T helper (Th) 2 cells appears to be decisive in the development of allergy. Tr1 cells consistently represent the dominant subset specific for common environmental allergens in healthy individuals. In contrast, there is a high frequency of allergen-specific interleukin-4 (IL-4)-secreting T cells in allergic individuals. Allergen-specific immunotherapy can induce specific Tr1 cells that abolish allergen-induced proliferation of Th1 and Th2 cells, as well as their cytokine production. Tr1 cells utilize multiple suppressor mechanisms, such as IL-10 and transforming growth factor-β (TGF-β) as secreted cytokines and various surface molecules, such as cytotoxic T-lymphocyte antigen 4 and programmed death-1. IL-10 only inhibits T cells stimulated by low numbers of triggered T-cell receptors, which depend on CD28 costimulation. IL-10 inhibits CD28 tyrosine phosphorylation, preventing the binding of phosphatidylinositol 3-kinase p85 and consequently inhibiting the CD28 signalling pathway. In addition, IL-10 and TGF-β secreted by Tr1 cells skew the antibody production from immunoglobulin E (IgE) towards the non-inflammatory isotypes IgG4 and IgA, respectively. Induction of antigen-specific Tr1 cells can thus re-direct an inappropriate immune response against allergens or auto-antigens using a broad range of suppressor mechanisms. [ABSTRACT FROM AUTHOR]

Published

2006

106. Induction of antigen-specific regulatory T cells in the liver-draining celiac lymph node following oral antigen administration.

Author

Hultkrantz, Susanne, Östman, Sofia, and Telemo, Esbjörn

Subjects

T cells, ANTIGENS, LYMPH nodes, CELL receptors, IMMUNE response, TUMORS

Abstract

Regulatory T cells are induced by oral administration of an antigen, but the physiological requirements and localization of the inductive sites are largely unknown. Using an adoptive transfer system of cells transgenic for ovalbumin T-cell receptor (OVA TCR tg), we found that antigen-specific CD4+ T cells were activated in the liver-draining celiac lymph node (CLN) shortly after ovalbumin feeding, and that a significantly higher proportion of the T cells in the CLN developed into the putative regulatory phenotype [co-expressing CD25 with the glucocortico-induced tumour necrosis factor (TNF) receptor family related gene (GITR), cytotoxic T-lymphocyte antigen (CTLA)-4 and CD103] than in Peyer's patches, the mesenteric and peripheral lymph nodes and the spleen. In addition, a particularly high level of expression of CD103 on the OVA-specific T cells in the CLN may favour homing to the epithelium of the intestine. While equally suppressive, OVA tg T cells isolated from the CLN of OVA-fed DO11·10 mice were less dependent on transforming growth factor (TGF)-β for suppression than cells isolated from the peripheral and mesenteric lymph nodes, which indicates the involvement of an additional suppressive mechanism. The expression of FoxP3 was not up-regulated in any of the lymph node compartments studied. Our phenotypic and functional findings suggest that the induction of regulatory T cells in the CLN may be relevant in the control of the immune response to dietary antigens. [ABSTRACT FROM AUTHOR]

Published

2005

107. The Vγ2/Vδ2 T-cell repertoire inMacaca fascicularis: functional responses to phosphoantigen stimulation by the Vγ2/Jγ1.2 subset.

Author

Cairo, Cristiana, Propp, Nadia, Hebbeler, Andrew M., Colizzi, Vittorio, and Pauza, C. David

Subjects

T cell receptors, CELL receptors, KRA, MOLECULAR weights, ANTIGENS, MAJOR histocompatibility complex

Abstract

Circulating Vγ2/Vδ2 T cells in human and non-human primates respond to small molecular weight non-peptidic phosphoantigens in a major histocompatibility complex (MHC)-unrestricted manner. These responses are encoded by the Vγ2/Jγ1.2 chain of the T-cell receptor and are positively selected during early development to create a biased repertoire in adults. We characterized the Vγ2 chain in cynomolgus macaques (Macaca fascicularis) to develop a non-human primate model for studying the effects of infection and therapy on the circulating Vγ2/Vδ2 T-cell subset. The cynomolgus macaque Vγ2 chain was highly homologous to the Vγ2 chain from human beings and rhesus macaques (Macaca mulatta), though we noted conserved substitutions in critical residues within the CDR3 for both macaque species. Despite these substitutions, Vγ2/Vδ2+ T cells from cynomolgus monkeys exhibited polyclonal responses to two different phosphoantigens. Proliferative responses were observed with both isopentenylpyrophosphate and alendronate, but stronger interferon-γ secretory responses were observed with isopentenylpyrophosphate.In vitrostimulation and expansion led to selective outgrowth of the Vγ2/Jγ1.2 subset, with a marked shift in the Vγ2 spectratype. As a result of the less biased starting repertoire for Vγ2, the cynomolgus macaque constitutes a sensitive model for examining the effects ofin vitroorin vivotreatments on the Vγ2/Vδ2 T-cell population. Our studies establish the value of cynomolgus macaques as a model for Vγ2/Vδ2 T-cell responses to non-peptidic antigens, and further evidence the remarkable evolutionary conservation of this unusual, phosphoantigen-responsive T-cell subset that is found only in primate species. [ABSTRACT FROM AUTHOR]

Published

2005

108. Epicutaneous immunization inducesαβ T-cell receptor CD4 CD8 double-positive non-specific suppressor T cells that inhibit contact sensitivity via transforming growth factor-β.

Author

Szczepanik, Marian, Bryniarski, Krzysztof, Tutaj, Monika, Ptak, Maria, Skrzeczynska, Joanna, Askenase, Philip W., and Ptak, Wlodzimierz

Subjects

ANTIGENS, GROWTH factors, CYTOKINES, IMMUNIZATION, LYMPHOCYTES, IMMUNOLOGY

Abstract

Since it was previously shown that protein antigens applied epicutaneously in mice induce allergic dermatitis mediated by production of T helper 2 (Th2) cytokines we postulated that this might induce suppression of Th1 immunity. Here we show that epicutaneous immunization of normal mice with a different protein antigen applied on the skin in the form of a patch induces a state of subsequent antigen-non-specific unresponsiveness caused by suppressor T cells (Ts) that inhibit sensitization and elicitation of effector T-cell responses. Suppression is transferablein vivobyαβ-T-cell receptor CD4+ CD8+ double positive lymphocytes harvested from lymphoid organs of skin patched animals and are not major histocompatibility complex-restricted nor antigen specific. Both CD25+ and CD25– CD4+ CD8+ T cells are able to suppress adoptive transfer of Th1 effector cells mediating cutaneous contact sensitivity.In vivotreatment with monoclonal antibodies showed that the cytokines interleukin (IL)-4, IL-10 and transforming growth factor-β (TGF-β) are involved in the induction of the Ts cells. Additionally, using IL-10–/– mice we found that IL-10 is involved in skin induced tolerance. Furtherin vitroexperiments showed that lymph node cells of skin tolerized mice non-specifically suppress[3H]thymidine incorporation by antigen-stimulated immune cells and this effect can be abolished by adding anti-TGF-β, but not anti-IL-4 nor anti-IL-10 antibodies. These studies indicate the crucial role of TGF-β in skin induced tolerance due to non-antigen-specific Ts cells and also show that IL-4, IL-10 and TGF-β play an important role in the induction of epicutaneously induced Ts cell suppression. [ABSTRACT FROM AUTHOR]

Published

2005

109. Cross-linking of neutrophil CD11b results in rapid cell surface expression of molecules required for antigen presentation and T-cell activation.

Author

Sandilands, Gavin P., Ahmed, Zubir, Perry, Nicole, Davison, Martin, Lupton, Alison, and Young, Barbara

Subjects

NEUTROPHILS, CELL membranes, BIOMOLECULES, ANTIGENS, T cells, PROTEIN crosslinking, IMMUNOLOGY

Abstract

Recent studies suggest that neutrophils may play a role in antigen presentation. In support of this hypothesis it has been shown that these cells appear to contain cytoplasmic stores of molecules required for this function, i.e. major histocompatibility complex class II (DR) antigen, CD80 and CD86. In this study we have considered a mechanism for the translocation of these preformed molecules onto the cell surface which does not require active synthesis. Cross-linking of the Mac-1 molecule (CD18 + CD11b) was shown to result in rapid cell surface expression of CD80, CD86 and DR antigen on the surface of normal human peripheral blood neutrophils. A distinct subpopulation (approximately 20%) of neutrophils appeared to be enlarged and were found to express significantly elevated levels of these molecules on the cell surface following cross-linking of CD11b when compared with control cells. The level of expression of CD80, CD86 and DR antigen on these large cells was comparable to, and in some cases greater than, the levels found expressed on the surface of monocytes obtained from the same donors. In addition, these cytoplasmic molecules were shown by confocal laser microscopy and by immunoelectron microscopy to be located within secretory vesicles. Following rapid translocation onto the cell surface, CD80 and CD86 appeared to be colocalized within large clusters reminiscent of the supramolecular antigen clusters previously found on conventional antigen-presenting cells. These findings therefore lend further support for the hypothesis that neutrophils may have a role to play in antigen presentation and/or T-cell activation. [ABSTRACT FROM AUTHOR]

Published

2005

110. Characterization of T-regulatory cells, induced by immature dendritic cells, which inhibit enteroantigen-reactive colitis-inducing T-cell responses in vitro and in vivo.

Author

Gad, Monika, Kristensen, Nanna N., Kury, Evelyn, and Claesson, Mogens H.

Subjects

T cells, COLITIS, DENDRITIC cells, LYMPHOID tissue, ANTIGENS, INTERLEUKIN-10

Abstract

Regulatory T (Treg) cells, derived from co-cultures of unfractionated CD4+ T cells and immature dendritic cells (DC), suppress enteroantigen-induced proliferation of CD4+ CD25− T cells. The DC-induced Treg cells are a mixture of CD25+ (10–20%) and CD25− (80–90%) T cells. However, all the suppressor activityin vitroandin vivoresides in the CD25+ T-cell subset. The CD25+ DC-induced Treg cells can inhibit enteroantigen-induced proliferationin vitrothrough a transwell membrane, and their function does not appear to depend on previous activation. DC-induced CD25+ Treg cells display a naïve phenotype, expressing high levels of CD45RB andl-selectin (CD62L). In addition, the DC-induced Treg cells mediate a stronger suppressive activity than prototype CD25+ regulatory T cells. The DC-induced Treg cells, and hereof purified CD25+ and CD25− T-cell fractions, were co-injected into severe combined immunodeficiency (SCID) mice with colitis-inducing CD4+ CD25− T cells. Both unfractionated CD4+ and purified CD25+ Treg cells fully protected the recipients against the development of colitis. In contrast, co-transfer of fractionated CD25− T cells offered no protection against disease development. Enterobacterial antigen-exposed CD4+ T cells of the protected mice secreted higher levels of interleukin-10 and lower levels of interferon-γ than the unprotected mice. The present data demonstrate DC-induced CD4+ CD25+ Treg cells, which phenotypically and functionally differ from the generally accepted prototype of CD25+ Treg cells. These data may initiate new procedures for the expansion of Treg cells for clinical use. [ABSTRACT FROM AUTHOR]

Published

2004

111. Antigen presentation by MART-1 adenovirus-transduced interleukin-10-polarized human monocyte-derived dendritic cells.

Author

Mehrotra, Shikhar, Chhabra, Arvind, Chakraborty, Abolokita, Chattopadhyay, Subhasis, Slowik, Mark, Stevens, Robert, Zengou, Ryan, Mathias, Clinton, Butterfield, Lisa H., Dorsky, David I., Economou, James S., Mukherji, Bijay, and Chakraborty, Nitya G.

Subjects

DENDRITIC cells, INTERLEUKIN-10, ANTIGENS, T cells, MAJOR histocompatibility complex, IMMUNE response

Abstract

Dendritic cells (DC) play critical roles in generating an immune response and in inducing tolerance. Diverse microenvironmental factors can‘polarize’ DC toward an immunogenic or non-immunogenic phenotype. Among the various microenvironmental factors, interleukin-10 (IL-10) exhibits a potent immunosuppressive effect on antigen-presenting cells (APC). Here, we show that monocyte-derived DC generated in the presence of IL-10 exhibit a profound down-regulation of many genes that are associated with immune activation and show that the IL-10-grown DC are poor stimulators of CD8+ T cells in a strictly autologous and major histocompatibility complex (MHC) class I-restricted melanoma antigen recognized by T cells (MART-1)epitope presentation system. However, these IL-10-grown DC can efficiently activate the epitope-specific CD8+ T cells when they are made to present the epitope following transduction with an adenoviral vector expressing the MART-1 antigen. In addition, we show that the MART-1 protein colocalizes with the MHC class I protein, equally well, in the iDC and in the DC cultured in presence of IL-10 when both DC types are infected with the viral vector. We also show that the vector transduced DC present the MART-127−35 epitope for a sustained period compared to the peptide pulsed DC. These data suggest that although DCs generated in the presence of IL-10 tend to be non-immunogenic, they are capable of processing and presenting an antigen when the antigen is synthesized within the DC. [ABSTRACT FROM AUTHOR]

Published

2004

112. Understanding thymus-independent antigen-induced reduction of thymus-dependent immune responses.

Author

Lindroth, Karin, Mastache, Elena Fernández, Roos, Izaura, Fernández, África González, and Fernández, Carmen

Subjects

IMMUNOGLOBULINS, IMMUNE response, POLYSACCHARIDES, DEXTRAN, ANTIGENS, MOLECULAR weights

Abstract

Deficiencies in immune responses against polysaccharides can have direct consequences for patients, and therefore, a better undestanding of these immune reactions is crucial We have studied the immune response against the polysaccharide dextran B512 (Dx). Administration of immunogenic doses of thymus-independent (TI) Dx reduces the immunoglobulin G1 response to later challenges with a thymus-dependent (TD) form of Dx. We investigated if this suppression is a general phenomenon caused not only by Dx but also by other TI antigens, and examined possible mechanisms contributing to this unresponsiveness. We show that clonal exhaustion is not involved in modulating subsequent responses, nor is signalling via FcγRIIB or other antibody mediated pathways. The reduced TD response is not an exclusive Dx phenomenon; it is also induced by TI antigen oxazolone (Ox). However, responses against the hapten dinitrophenyl (DNP) are not affected, indicating that the TI priming negative effect is not a general process. This may be explained by the restricted immune response to both Dx and Ox, in contrast to the unrestricted DNP response. Our conclusion from these experiments is that the underlying mechanism for the TI-induced reduction of latter TD responses is a property of the TI activation itself. [ABSTRACT FROM AUTHOR]

Published

2004

113. Normal human pregnancy is associated with an elevation in the immune suppressive CD25+ CD4+ regulatory T-cell subset.

Author

Foey, Andrew D. and Brennan, Fionula M.

Subjects

T cells, ANTIGENS, IMMUNE response, HOMOGRAFTS, WOMEN, MESSENGER RNA, DENDRITIC cells

Abstract

CD4+ CD25+ T regulatory cells (TReg), suppress antigen-specific immune responses and are important for allograft tolerance. During pregnancy the mother tolerates an allograft expres- sing paternal antigens (the fetus) requiring substantial changes in immune regulation over a programmed period of time. We analysed whether immune-suppressive TReg cells were altered during pregnancy and therefore might play a part in this tolerant state. The presence of TReg cells was assessed in the blood of 25 non-pregnant, 63 pregnant and seven postnatal healthy women by flow cytometry. We observed an increase in circulating TReg cells during early pregnancy, peaking during the second trimester and then a decline postpartum. Isolated CD25+ CD4+ cells expressed FoxP3 messenger RNA, a marker of TReg cells, and suppressed proliferative responses of autologous CD4+ CD25­T cells to allogeneic dendritic cells. These data support the concept that normal pregnancy is associated with an elevation in the number of TReg cells which may be important in maintaining materno-fetal tolerance. [ABSTRACT FROM AUTHOR]

Published

2004

114. A monoclonal antibody to the rat Crry/p65 antigen, a complement regulatory membrane protein, stimulates adhesion and proliferation of thymocytes.

Author

Arsenović-Ranin, N., Vučević, D., Okada, N., Dimitrijević, M., and Čolić, M.

Subjects

MONOCLONAL antibodies, ANTIGENS, MEMBRANE proteins, EPITHELIAL cells, INTERFERONS

Abstract

Summary A murine monoclonal antibody (mAb), 3F10, was produced by fusion of spleen cells obtained from mice immunized with a rat cortical thymic epithelial cell line (R-TNC.1) stimulated with interferon-γ and P3X myeloma cells. 3F10 recognized an antigen expressed both on thymocytes and non-lymphoid cells in the thymus. Flow cytometry showed that 3F10 stained more than 98% thymocytes and 90% R-TNC.1 cells. Immunoprecipitation and Western blot studies demonstrated that 3F10 reacted with molecules of 55000 and 65000 MW from both thymocyte and R-TNC.1 cell lysates. 3F10 recognized the same antigen on Chinese hamster ovary cells transfected with rat Crry as did 5I2 mAb, confirming the specificity of 3F10 mAb for the rat homologue of mouse Crry/p65, a membrane-bound complement regulatory protein. 3F10 mAb induced homotypic aggregation of thymocytes and exhibited an additive effect on the aggregation evoked by phorbol myristate acetate. The aggregation was dependent on active cell metabolism, intact cytoskeleton, divalent cations and activation of protein phosphatases 1 and 2A (as assessed by use of okadaic acid). In contrast, H-7, HA1004 and genistein partially inhibited, whereas staurosporine potentiated the aggregation of thymocytes triggered by 3F10. 3F10 mAb also stimulated binding of thymocytes to the R-TNC.1 line. Both homotypic and heterotypic adhesive interactions are mediated by leucocyte function-associated antigen-1 (LFA-1). In addition, 3F10 stimulated proliferation of thymocytes induced by suboptimal concentrations of concanavalin A. These data suggest that rat Crry/p65 might be involved in the regulation of both cell adhesion and activation of thymocytes. This is a novel, non-complement-dependent function of Crry/p65. [ABSTRACT FROM AUTHOR]

Published

2000

115. Anti-anti-idiotypic (Ab3) antibodies that bind progesterone-11α–bovine serum albumin differ in their combining sites from antibodies raised directly against the antigen.

Author

Kirsch, R. D., Beale, D., He, M., Corper, A. L., Krawinkel-Brenig, U., and Taussig, M. J.

Subjects

IMMUNOGLOBULINS, ALBUMINS, ANTIGENS

Abstract

Polyclonal rabbit anti-idiotypic (Ab2) antibodies raised against the antiprogesterone mAb DB3 (Ab1) were used to induce an Ab3 antiprogesterone response in BALB/c mice. While the affinity of Ab3 sera for progesterone was 10—50-times lower than that of DB3, their steroid-binding specificity showed considerable similarity to DB3. Two immunoglobulin M (IgM) Ab3 monoclonal antibodies (mAbs), 1A4 and 3B11, were obtained, both of which bound progesterone conjugated to bovine serum albumin (progesterone—BSA). 1A4 also bound free progesterone, although with low affinity and very broad cross-reactivity. Like DB3, 1A4 is encoded by a heavy-chain variable region (V[sub H]) gene segment from the small VGAM3.8 family, a restriction that is characteristic of antibodies raised against progesterone-11α—BSA. In contrast, 3B11 binds progesterone-11α—BSA but not free progesterone and is encoded by an unrelated V[sub H] gene from the J558 family. The light chain variable region (V[sub L]) of 1A4 lacks the intradomain disulphide bridge owing to replacement of CysL23 by Tyr. Both the 1A4 and 3B11 heavy chains have extremely short complementarity determining region (CDR) H3 loops, comprising three and four amino acids, respectively. Modelling of the combining site of 1A4 from the X-ray crystallographic structure of DB3 indicates that the short H3 loop is a major factor in the loss of affinity and specificity for steroid. [ABSTRACT FROM AUTHOR]

Published

2000

116. Common antigenicity between Japanese cedar (Cryptomeria japonica) pollen and Japanese cypress (Chamaecyparis obtusa) pollen, I. H‐2 complex affects cross responsiveness to Cry j 1 and Cha o 1 at the T‐ and B‐cell level in mice.

Author

Kingetsu, I., Ohno, N., Hayashi, N., Sakaguchi, M., Inouye, S., and Saito, S.

Subjects

ALLERGENS, ANTIGENS

Abstract

Summary Common antigenicity among two purified Japanese cedar pollen allergens (Cry j 1 and Cry j 2) and one Japanese cypress pollen allergen (Cha o 1) was explored at the T‐cell and B‐cell level in mice of different H‐2 haplotypes. Cry j 2 did not show any common antigenicity with Cry j 1 or Cha o 1. B10.S (H‐2S) mice immunized with Cry j 1 or Cha o 1 generated T cells and antibodies reactive to both antigens, indicating the common antigenicity of these antigens. C57BL/6 (H‐2b) mice were non‐responders to Cry j 1. BALB/c (H‐2d) mice immunized with Cry j 1 or Cha o 1 and C57BL/6 mice immunized with Cha o 1 generated T cells that were only reactive with the respective immunogen, but produced antibody reactive to both Cry j 1 and Cha o 1, indicating that Cry j 1 and Cha o 1 share their B‐cell epitope but not their T‐cell epitope. This finding may provide a clue for the clarification of the T‐cell and B‐cell epitopes of Cry j 1 and Cha o 1, even though the data are influenced by H‐2 complex restriction in mice. Considering that H‐2 complex restriction affects cross responsiveness to Cry j 1 and Cha o 1 at the T‐ and B‐cell level in mice, we assessed the possible situation in humans exposed sequentially to Japanese cedar pollen and Japanese cypress pollen. [ABSTRACT FROM AUTHOR]

Published

2000

117. The effects of monoclonal antibodies against iC3b receptors in mice with experimentally induced disseminated candidiasis.

Author

Lee, K.H., Yoon, M.S., and Chun, W.H.

Subjects

MONOCLONAL antibodies, CANDIDIASIS, IMMUNOGLOBULINS, ANTIGENS, CANDIDA albicans, INTEGRINS

Abstract

CR3 (iC3b receptor), composed of CD11b/CD18, is a β2 integrin. A protein that shares antigenic and structural homology with the α-chain of CD11b/CD18 has been isolated from the surface of Candida albicans. This molecule is thought to be essential in the pathogenesis of disseminated candidiasis. To evaluate the effects of anti-iC3b receptor antibodies on adhesion between human dermal microvascular endothelial cells (HDMEC) and C. albicans, and in treatment of candidal infection, a binding assay of C. albicans to cultured HDMEC was performed in vitro. An antiiC3b receptor-specific monoclonal antibody was administered to mice infected with C. albicans. The mice were monitored for mortality and renal involvement by culture and histopathological findings. Flow cytometric analysis demonstrated surface expression of iC3b receptor on C. albicans. The adherence of C. albicans to HDMEC was significantly decreased by treatment with anti-iC3b receptor antibodies. Anti-iC3b receptor antibodies significantly increased the survival time and rate while lowering the renal fungal burden. The iC3b receptors are involved in the adherence of C. albicans to vascular endothelial cells and are likely to be involved in the pathogenesis of disseminated candidiasis. The increased survival in mice infected with C. albicans after treatment with anti-iC3b receptor antibodies indicates that this modality may be beneficial for future development of a new therapy for candidiasis. [ABSTRACT FROM AUTHOR]

Published

1997

118. Antigen dose-dependent predominance of either direct or sequential switch in IgE antibody responses.

Author

Sudowe, S., Rademaekers, A., and Kölsch, E.

Subjects

ANTIGENS, IMMUNOGLOBULIN E, IMMUNE serums, SPLEEN, LABORATORY mice, POLYMERASE chain reaction, IMMUNIZATION

Abstract

Priming of CBA/J mice with minute doses of protein antigens (Ag) leads to high IgE antibody (Ab) titres in the immune sera of these animals. In contrast priming with large doses elicits only a marginal production of IgE Ab. In vitro restimulation of spleen cells from animals primed with large doses and lacking of vivo IgE Ab leads to a burst of IgE Ab-forming cells. This in vitro ammnestic response is lacking in mice primed with minute doses of Ag. In order to trace the cellular basis of the of vitro IgE memory response we have extended the analysis of the distribution of Ab isotypes to Ag-primed IgG1-deficient Δ5′Sγl mice. The data presented here must be interpreted as followed. Priming of mice with minute doses of Ag leads to a direct switch from IgM to IgE Ab expression in both strains. These animals have high IgE Ab titres without establishing an IgE memory. The direct switch was verified by polymerase chain reaction and Southern blot analysis of switch circle DNA isolated from Ag-specific B cells of CBA/J mice primed with minute doses of Ag. In contrast to immunization with minute doses, priming with large doses of Ag fails to induce in rive IgE Ab production in CBA/J and Δ5′Sγ1 mice but establishes a Bε memory in CBA/J mice which involves IgG1-bearing intermediate B cells. In rive these Bε memory cells do not enter the status of IgE Ab-producing cells. In vitro they can be released from this anergy and presumed suppression and develop in an ammnestic response into a large population of IgE Ab-forming B cells. This increase in the number of IgE Ab-producing cells after restimulation in vitro is lacking in Δ5′Sγ1 mice, apparently because of their inability to generate IgG1-expressing precursor cells. The notion of a sequential switch and an IgG1 intermediate Bε memory status is also supported by depletion and inhibition experiments. Elimination of IgG1-expressing B cells in CBA/J mice primed with high doses of Ag prevents the IgE Ab burst after in vitro challenge with Ag. The data further suggest that the two switch pathways are not mutually exclusive and that the Ag dose can decide which pathway is preferentially used. [ABSTRACT FROM AUTHOR]

Published

1997

119. Cord blood CD4+ CD45RA+ T cells achieve a lower magnitude of activation when compared with their adult counterparts.

Author

Hassan, J. and Reen, D. J.

Subjects

CORD blood, T cells, ANTIGENS, MONOCLONAL antibodies, INTERLEUKIN-2, GRAFT versus host disease, IMMUNOLOGY

Abstract

Highly purified CD4+ CD45RA+ cells from cord blood and peripheral blood from healthy adults were studied. The levels of expression of the CD2, CD3, CD4 and CD28 antigens were similar; however, CD45 and CD45RA antigen expression were slightly lower in cord cells. The reduced expression of the CD45RA antigen on cord CD4+ T cells was confirmed in whole blood. Functional assessment revealed deficiencies in cord CD4+ CD45RA+ T cells. Interleukin-2 (IL-2) production in response to specific triggering via CD2 monoclonal antibody (mAb) alone, or CD2 mAb in combination with CD28 mAb showed marked underproduction (about 10% of adult production). When CD25 expression was examined, it was observed that the proportion of activated CD4+ CD45RA+ T cells in cord blood was lower than in adult (about 20% of adult expression). Proliferation to CD2 mAbs or CD2+28 mAbs of cord blood naive cells was similarly depressed. Investigation of IL-2 mRNA expression under these stimulatory conditions paralleled the results observed for CD25 expression, IL-2 production and proliferation. When phorbol 12-myristate 13-acetate (PMA) was added to the cells triggered with CD2+28mAbs, the responses examined were enhanced in both cord and adult blood with no significant differences between the groups. These findings suggest that under identical conditions of stimulation, purified cord blood CD4+ CD45RA+ T cells do not acquire similar activation status as their adult counterparts. These finding may help in understanding the reduced graft-versus-host disease (GVHD) observed in cord blood stem cell transplantation. [ABSTRACT FROM AUTHOR]

Published

1997

120. Apoptosis in a Fas-resistant, T-cell receptor-sensitive human leukaemic T-cell clone.

Author

Delehanty, L. L., Payne, J. A., Farrow, S. N., Brown, R., and Champion, B. R.

Subjects

T cell receptors, CELL receptors, APOPTOSIS, ANTIGENS, GENETIC mutation, IMMUNOREGULATION, IMMUNOLOGY

Abstract

The Fas (CD95) antigen plays a key role in regulating T-cell activation and survival. We have generated a Fas-resistant subclone of the human T-cell leukaemia line, H9, which is still able to undergo apoptosis in response to T-cell receptor ligation. Molecular analyses revealed that resistance to Fas-mediated apoptosis was due to a heterozygous mutation in the death domain of the Fas gene which generates a stop codon, and thus encodes a truncated Fas molecule. Fas ligation was able to induce apoptosis in the presence of cycloheximide, indicating that the mutant Fas molecule retained some signalling capability, which is death-domain independent. These cells will provide a useful tool for dissecting the complexities of Fas signalling pathways. [ABSTRACT FROM AUTHOR]

Published

1997

121. Expression of HIS50 Ag: a rat homologue of mouse heat-stable antigen and human CD24 on B lymphoid cells in the rat.

Author

Hermans, M. H. A., Deenen, G. J., de Boer, N., Wang Bo, Kroese, F. G. M., and Opstelten, D.

Subjects

ANTIGENS, B cells, MONOCLONAL antibodies, DNA, T cells, CELL membranes

Abstract

Recently, a cDNA encoding a newly identified rat antigen (HIS50 Ag) that binds to monoclonal antibody (mAb) HIS50 was cloned and shown to be homologous to cDNA encoding murine heat-stable antigen (HSA) and human CD24. Here we show that, like CD24 and HSA, at least part of HIS50 Ag is inserted into the plasma membrane by a glycosyiphosphatidylinositol (GPI)-lipid linkage and we describe its expression in rat haemolymphopoietic tissues. HIS50 Ag expression was almost exclusively confined to B lymphoid cells, the vast majority of T lymphoid cells, erythroid and myeloid cells were HIS50 -. Cell suspension analysis indicated that in bone marrow (SM) almost all Thy-1 + cells, H1S24 + cells [H1S24 recognizes the B-cell form of leucocyte common antigen (LCA)], terminal deoxynucleotidyl transferase-positive (TdT +) cells and (c + s)κ + cells expressed HIS50 Ag, and all (c+s)μ+ cells. A presumably early population of B lymphoid cells, expressing HIS24 Ag without HIS50 Ag, TdT or immunoglobulin (HIS24+HIS50- TdT- Ig-), constituted 1 .6% of BM nucleated cells. In blood, one-fifth of mononuclear cells were HIS50+, and about 85% of these expressed μ and/or κ chains. In spleen, flow cytometry analysis and immunohistology demonstrated heterogeneous expression of HIS5O Ag: immunoglobulin M (IgM)bright cells (as found largely in red pulp and marginal zone) were HIS50bright, while IgMdull cells expressed low or undetectable levels of HIS 50 Ag. Germinal centre B cells expressed high levels of HIS50 Ag. Germinal centres of lymph nodes and tonsil of man also bound HIS50. We conclude that HIS50 Ag expression in the haemolymphopoietic system of rat is virtually restricted to the B lineage. [ABSTRACT FROM AUTHOR]

Published

1997

122. Induction of murine CD5 expression by v-H-<em>ras</em>.

Author

Weichert, T. R. and Schwartz, R. C.

Subjects

ANTIGENS, BONE marrow, RETROVIRUSES, B cells, ONCOGENES, BIOMARKERS

Abstract

The murine CD5 surface antigen is a frequent marker on B-lineage cell lines produced from bone marrow infected with retroviruses expressing v-H-ras. Since CD5 + B cells cannot be detected in adult murine bone marrow, either the viral targets of transformation are a minor contaminating population of CD5 + B-lineage cells or the v-H-ras oncogene is inducing the expression of CD5 on Blineage cells not previously expressing this marker. We have found that v-H-ras can induce the expression of CD5 on two CD5 - preB-cell lines established from murine bone marrow. This induction correlates with increased steady-state levels of CD5 mRNA. These results present the possibility that CD5 expression may be modulated by specific signalling as well as early lineage commitment. [ABSTRACT FROM AUTHOR]

Published

1997

123. Differential expression of function-related antigens on newborn and adult monocyte subpopulations.

Author

Murphy, F. J. and Reen, D. J.

Subjects

ANTIGENS, MONOCYTES, LEUCOCYTES, CORD blood, IMMUNOGLOBULINS, IMMUNOGENETICS, MAJOR histocompatibility complex, EMBRYOLOGY, HLA histocompatibility antigens

Abstract

Umbilical cord blood and adult peripheral blood monocytes were separated into two subpopulations. based on the intensity of CD14 expression, and the coexpression of various antigens associated with monocyte function was examined. The majority of cord and adult monocytes expressed CD14 at a high density (CD14bright) while approximately 15% of monocytes expressed this antigen at a lower level (CD14dim). Three times as many CD14dim monocytes expressed CD16 (FcγRIII) as did CD14bright monocytes in both cord and adult preparations, while its level of expression (mean fluorescence intensity) was significantly reduced on cord CD14dim monocytes relative to adult CD14dim monocytes. The percentage of cord blood CD14dim monocytes expressing human leucocyte antigen-DR (major histocompatibility complex class II antigen) was significantly reduced relative to adult CD14dim cells; however, the level of expression of this antigen was greater on both cord and adult CD14dim monocytes compared with CD14bright cells. Cord CD14bright cells expressed CD36 (OKM5) to a greater extent than did their adult counterparts. The level of expression of CD62L was reduced on cord CD14dim cells compared with adult CD14dim cells. CD11b (CR3) was expressed both on a higher percentage of cells and also with a greater intensity on both cord and adult CD14bright monocytes compared with their CD14dim counterpart. These results show that significant differences exist between cord and adult monocyte subpopulations with regard to expression of various antigens associated with specific effector function. [ABSTRACT FROM AUTHOR]

Published

1996

124. Mucosal immunoadjuvant activity of liposomes: role of alveolar macrophages.

Author

De Haan, A., Groen, G., Prop, J., Van Rooijen, N., and Wilschut, J.

Subjects

IMMUNOLOGICAL adjuvants, INFLUENZA viruses, PARAMYXOVIRUSES, RESPIRATORY infections, VIRUS diseases, LIPOSOMES, PHOSPHOLIPIDS, BILAYER lipid membranes, ANTIGENS

Abstract

Previously, we have reported on a liposomal adjuvant system for stimulation of both systemic IgG and mucosal s-IgA responses against viral antigens (influenza virus subunit antigen or whole inactivated measles virus) administered intranasaily to mice. Immune stimulation is observed with negatively charged, but not with zwitterionic, liposomes and is independent of a physical association of the antigen with the liposomes. Furthermore, liposome-mediated immune stimulation requires deposition of the liposomes and the antigen in the lower respiratory tract. In the present study, it is shown that alveolar macrophages (AM) are the main target cells for negatively charged liposomes administered to the lungs of mice. AM isolated from animals, to which negatively charged liposomes were administered beforehand, showed large intracellular vacuoles, suggestive of massive liposome uptake. Under ex vivo conditions, both AM and RAW 264 cells exhibited a high capacity to take up negatively charged liposomes. The deposition of negatively charged liposomes, but not zwitterionic, liposomes in the lung reduced the phagocytic and migratory behaviour of AM, as assessed on the basis of transport of carbon particles to the draining lymph nodes of the lungs. Depletion of AM in vivo with dichloromethylene diphosphonate, facilitated an enhanced systemic and local antibody response against influenza subunit antigen deposited subsequently to the lower respiratory tract. In conclusion, these data provide support for the hypothesis that uptake of negatively charged liposomes blocks the immunosuppressive activity of AM, thereby facifitating local and systemic antibody responses. [ABSTRACT FROM AUTHOR]

Published

1996

125. Covalent binding of C3b to tetanus toxin: influence on uptake/internalization of antigen by antigen-specific and non-specific B cells.

Author

Villiers, M.-B., Villiers, C.L., Jacquier-Sarlin, M.R., Gabert, F.M., Journet, A.M., and Colomb, M.G.

Subjects

TETANUS toxin, BACTERIAL toxins, CLOSTRIDIUM tetani, NEUROTOXIC agents, ANTIGENS, IMMUNITY

Abstract

Antigen opsonization by the C3b fragment of complement is a significant event in the modulation of cell-mediated immune response, but its mechanism is still largely unknown. The structural characteristics of C3b allow it to act as a bifunctional ligand between antigen and cells via their membrane C3b receptors. It was thus of interest to study the influence of the covalent link between C3b and antigen on the fixation and internalization of this antigen by antigen-presenting cells. Tetanus toxin (TT) was used as antigen, either free or covalently linked to C3b (TT-C3b). The antigen-presenting cells were TT-specific (4.2) or non-specific (BL15) Epstein-Barr virus (EBV)transformed B cells. C3b was found to play an important role in antigen fixation and internalization by both antigen-specific and antigen non-specific cells. Covalent binding of C3b on TT (1) permitted fixation and internalization of this antigen by non-specific cells via their complement receptors; (2) enhanced antigen fixation and resulted in cross-linking between membrane immunoglobulins and complement receptors on antigen-specific cells. The consequences of covalent C3b binding to TT were analysed using antigen-specific and antigen-nonspecific cells. In both cases, a net increase in antigen fixation was observed. At the intracellular level, covalent C3b binding to TT resulted in a large TT incorporation in endosomes of nonspecific cells, similar to that observed in antigen-specific cells. Thus, C3b covalently linked to antigen enlarges the array of B-cell types capable of presenting antigen, including non-specific cells. [ABSTRACT FROM AUTHOR]

Published

1996

126. Regulation by non-major histocompatibility complex genes of the allo-4-hydroxy-phenylpyruvate dioxygenase (F liver protein) response.

Author

Brunner, M.C. and Mitchison, N.A.

Subjects

MAJOR histocompatibility complex, PROTEINS, LIVER, ANTIGENS, CYTOKINES, GENETIC transcription

Abstract

Although rapid progress is being made in the quantitative genetics of multifactorial disease, no response to a simple antigen has yet been subjected to full genomic analysis. The well-characterized antigen allo-HPPD (4-hydroxy-phenylpyruvate dioxygenase, previously known as F liver antigen) is a good candidate for such treatment. Old and new data bearing on this possibility are here assembled. In respect of antibody production and an early burst of interleukin-4 (IL-4) transcription, introduction of the non-major histocompatibility complex (MHC) background from A/J strain mice into FI hybrids with C57BL10 strains up-regulates the response. These findings can be aligned with previous quantitative genetics carried out on airway hyperresponsiveness in related strains, and to a lesser extent with the genetics of autoimmune diabetes in the mouse. Taken together, the findings suggest that regulation of the pro-inflammatory cytokines are largely responsible for the variation. Additional data indicate that these non-MHC genes are are to a variable extent (depending on the response parameter) epistatic to the down-regulatory MHC allele H-2Ab. [ABSTRACT FROM AUTHOR]

Published

1996

127. Chimaeric monoclonal antibodies encoded by the human VH26 gene from naïve transgenic mice display a wide range of antigen-binding specificities.

Author

Harmer, I. J., Mageed, R. A., Kaminski, A., Charles, P., Brüggemann, M., and Mackworth-Young, C. G.

Subjects

IMMUNOGLOBULINS, GENES, ANTIGENS, HYBRIDOMAS, TRANSGENIC mice, ENZYME-linked immunosorbent assay

Abstract

To elucidate the molecular basis for the ability of antibodies encoded by the human VH26 heavy-chain variable region gene to react with diverse antigens, we have generated 34 hybridomas secreting chimaeric monoclonal antibodies (human μ heavy chain/mouse light chains) from transgenic mice. The transgenic mice carry an immunoglobulin minilocus containing the human VH26 gene, human DH and JH gene segments, and genes encoding the human Cμ region. The minilocus in these animals undergoes functional rearrangement resulting in the production of chimaeric antibodies in which human μ heavy chains utilizing the VH26 gene are paired with mouse κ or λ light chains. The hybridomas described in this study were generated from naive animals and were selected solely on the basis of human μ-chain expression. The antibodies described have covalently attached mouse light chains and are multimeric in structure. The binding properties of the antibodies were examined using a panel of both self- and foreign antigens using enzyme-linked immunosorbent assays, agglutination or radio-immunoprecipitation assays and immunofluorescence. Chimaeric immunoglobulins from 21 of the 34 hybridoma clones (61·7%) reacted with one or more antigens, of which 13 (38·2%) reacted with more than two antigens. These studies demonstrate that the VH26 gene, in combination with human DH and JH gene segments, and mouse light-chain genes, is able to encode antibodies with a wide range of ligand-binding specificities. These findings have important implications in the context of the possible origins of autoantibodies encoded by VH26 which may play a role in the pathogenesis of a number of autoimmune conditions. [ABSTRACT FROM AUTHOR]

Published

1996

128. Expression of major histocompatibility complex class II antigens on normal porcine intestinal endothelium.

Author

Wilson, A.D., Haverson, K., Southgate, K., Bland, P.W., Stokes, C.R., and Bailey, M.

Subjects

MAJOR histocompatibility complex, IR genes, MONOCLONAL antibodies, ANTIGENS, HLA histocompatibility antigens, IMMUNOGLOBULINS

Abstract

A novel monoclonal antibody (MIL 11) specific for an antigen expressed on porcine endothelial cells is described. The antigen recognized by MIL 11 is most strongly expressed in the intestine but is also expressed on the capillary endothelium of a wide range of tissues. Using two- and three-colour immunofluorescence microscopy we demonstrated the extensive coexpression of MIL 11 and major histocompatibility complex (MHC) class II antigens on normal porcine capillary endothelium in the intestine, trachea, thymus and small veins, while endothelium of large vessels and the heart were negative for MHC class II. In contrast to humans and rodents, available reagents do not detect MHC class II on the intestinal epithlium of pigs. However, porcine intestinal endothelium expressed both DR and DQ antigens. A population of strongly class II-positive cells was also detected immediately adjacent to the endothelium in the lamina propria. Three-colour immunofluorescence microscopy highlighted the close association between endothelium and intestinal CD4+ T cells. Lamina propria T cells were mainly MHC class II positive, whereas those in the epithelial compartment were MHC class II negative. [ABSTRACT FROM AUTHOR]

Published

1996

129. Interferon-γ differentially regulates antigen-processing functions in distinct endocytic compartments of macrophages with constitutive expression of class II major histocompatibility complex molecules.

Author

Hockett, R.D., Cook, J.R., Findlay, K., and Harding, C.V.

Subjects

MAJOR histocompatibility complex, INTERFERONS, MACROPHAGES, HYBRIDOMAS, ANTIGENS, RIBONUCLEASES

Abstract

RAW264.7 cells were transfected to express constitutively the murine class II major histocompatibility complex (MHC-II) molecule, I-Ak. The resulting RAW.Ak cells presented HEL(46-61) peptide to 3A9 T hybridoma cells, but they were unable to process and present HEL protein in their resting state. However, IFN-γ stimulation induced the ability of RAW.Ak to process and present HEL protein, with little effect on their ability to present HEL(46-61) peptide. Antigen catabolism showed little change with IFN-γ, stimulation, suggesting that the production of peptides was not the regulated step in the processing pathway. Furthermore, HEL(46-61) peptide delivered directly into lysosomes by acid-resistant liposomes was also presented only upon IFN-γ stimulation, while the presentation of peptides delivered into endosomes by acid-sensitive liposomes showed a lesser dependence on IFN-γ stimulation. Thus, IFN-γ regulated the ability of peptides delivered into certain lysosomal compartments to meet with MHC-II molecules and form peptide-MHC complexes, or to transport subsequently to the plasma membrane. Two other antigens, ribonuclease A and haemoglobin, were processed by RAW.Ak cells without IFN-γ stimulation, suggesting that these antigens could be processed by different mechanisms, perhaps in earlier endocytic compartments. Thus, different antigens may be processed in distinct endocytic compartments, and an IFN-γ-regulated mechanism controls the rescue of peptides from lysosomal compartments for presentation at the plasma membrane. [ABSTRACT FROM AUTHOR]

Published

1996

130. Expression of both B7-1 and CD28 contributes to the IL-2 responsiveness of CTLL-2 cells.

Author

Belani, R. and Weiner, G. J.

Subjects

INTERLEUKIN-2, T cells, IMMUNOGLOBULINS, ANTIGENS, LYMPHOCYTES, BIOLOGICAL assay

Abstract

The CTLL-2 bioassay is used frequently to determine interleukin-2 (IL-2) concentrations in experimental samples, including samples that contain reagents which affect the CD28-B7 interaction. We therefore evaluated whether the CD28-B7 pathway plays a role in the growth of CTLL-2 cells. Flow cytometry demonstrated that CTLL-2 cells express both CD28 and B7-1. CTLA4-immunoglobulin (CTLA4-Ig) inhibited the growth of CTLL-2 cells over a range of IL-2 concentrations, suggesting that the CD28-B7 interaction plays an important role in the growth of CTLL-2 cells. Anti-B7-1 antibody also inhibited CTLL-2 proliferation at all concentrations of IL-2. These results indicate that the CTLL-2 bioassay may not be a reliable means of determining IL-2 levels in experimental samples containing reagents that affect the CD28-B7 interaction. They also suggest that co-expression of CD28 and B7 may contribute to the growth of malignant T cells. [ABSTRACT FROM AUTHOR]

Published

1996

131. Human γ/δ T-cell response to <em>Listeria monocytogenes</em> protein components <em>in vitro</em>.

Author

Munk, M. E., Elser, C., and Kaufmann, S. H. E.

Subjects

CELLULAR immunity, T cells, LISTERIA monocytogenes, MACROPHAGES, ANTIGENS, IMMUNITY, LISTERIOSIS

Abstract

Listeria monocytogenes is a facultative intracellular pathogen that replicates inside mononuclear phagocytes and induces specific cellular immunity. Listeriosis encompasses many clinical syndromes and meningitis is the most frequent clinical manifestation. Human α/β and γ/δ T cells have been shown to respond to L. monocytogenes antigens and to play an important role in resistance against listerial infection. We investigated the nature of listerial ligands and the influence of the major virulence factor, listeriolysin (hly), on the stimulation of human γ/δ T cells from healthy individuals. We found that a listerial somatic protein ligand, which is sensitive to proteinase treatment, stimulated γ/δ T cells in vitro; the majority of Listeria-responsive γ/δ T cells expressed Vγ9Vδ2 T-cell receptor chains and human leucocyte antigen-DR molecules; γ/δ T-cell responses to hly+ and hly- Listeria strains were comparable; L. monocytogenes strains of different virulence stimulated γ/δ T cells equally. Thus, protein components of L. monocytogenes unrelated to virulence activate human γ/δ T cells in vitro. [ABSTRACT FROM AUTHOR]

Published

1996

132. Derivation of T-cell receptor α-chain double expresser lines from normal murine mature T cells.

Author

Eshima, K., Suzuki, H., Yamazaki, S., and Shinohara, N.

Subjects

T cell receptors, T cells, LYMPHOCYTES, GENES, IMMUNOGLOBULINS, ANTIGENS

Abstract

Because the T-cell receptor (TCR) α-chain locus is known to lack allelic exclusion of rearrangements, and as a recent report revealed the existence of α-chain double expressers among normal human peripheral blood lymphocytes (PBL), the possible existence of TCR α-chain double expressers among mature routine T cells was examined. Although two-colour staining analysis of normal T-cell populations did not immediately reveal recognizable clusters of Vet double expressers, alternative/n vitro stimulations of normal murine T cells with antibodies to two different TCR Vα chains reproducibly induced TCR α-chain double-expresser lines. TCR complexes with different α-chains on such T cells were both shown to be functional. The cell lines were heterogeneous with respect to Vβ usage and the ratio of the expressed amounts of the two α-chains on the surface. The ratio of the two expressed α-chains was found to be very stable over a long period of time. These results are consistent with the earlier report on α-chain double expressers among human T cells and also show normal occurrence of TCR α-chain double expressers in routine T-cell populations. [ABSTRACT FROM AUTHOR]

Published

1996

133. Modulation of superantigen-induced T-cell deletion by antibody anti-Pgp-1 (CD44).

Author

Ayroldi, E., Cannarile, L., and Riccardi, C.

Subjects

IMMUNOGLOBULINS, ANTIGENS, T cells, STAPHYLOCOCCUS, ENTEROTOXINS, BACTERIAL toxins

Abstract

We examined the effects of anti-Pgp- I (CD44) antibody on the in vitro deletion of murine CD4 and CD8 single positive T cells induced by Staphylococcal enterotoxin B (SEB). Soluble anti-Pgp-1 antibody enhanced the apoptosis and decreased the proliferation of SEB-responding T cells. In contrast, cross-linked anti-Pgp-1 antibody provided costimulatory signals for the T-cell activation induced by anti-CD3 antibody. Hyaluronic acid (HA), a ligand of Pgp-1, did not affect proliferation and deletion induced by SEB, whereas it mimicked the effects of the cross-linked antibody in anti-CD3-driven proliferation. T-cell Pgp-1 surface expression after 48 hr incubation with SEB was unchanged as compared to unstimulated cells. However, when the memory T cells were established, some Vβ8+ (SEB-specific) T cells Pgp-1low became Pgp-1high, displaying a bimodal character. Moreover, the Pgp-1 increased expression correlated with an increase of Pgp-1 soluble form in the supernatant. These findings suggested that signals following the triggering of the Pgp-1 molecule are important in controlling T-cell survival. [ABSTRACT FROM AUTHOR]

Published

1996

134. Limiting dilution analysis of CD4 T-cell cytokine production in mice administered native versus polymerized ovalbumin: directed induction of T-helper type-1-like activation.

Author

Gieni, R. S., Yang, X., Kelso, A., and Hayglass, K. T.

Subjects

T cells, CYTOKINES, TH1 cells, ANTIGENS, IMMUNITY, INTERFERONS, INTERLEUKIN-4, OOGENESIS

Abstract

Polarized expression of T-helper type-1 (Th1)- or Th2-like patterns of cytokine production frequently correlates with disease outcome. Previously, we have described the long-lived reciprocal regulation of ovalbumin (OVA)-specific IgE (> 95% inhibition) and IgG2a (300–800-fold increased) production following administration of high MW OVA polymers (OVA-POL), in both de novo and ongoing OVA (alum)-induced responses. Here, limiting dilution analysis (LDA) was used to compare precursor frequencies of CD4 T cells producing interferon-γ (IFN-γ), interleukin-4 (IL-4) or IL-10 following OVA versus OVA-POL exposure in vivo. Adjuvants were not used, so as to circumvent their impact on measurement of precursor frequencies. We found that the two forms of antigen elicited T-cell activation of comparable intensity, as indicated by equivalent precursor frequencies of clonogenic antigen-specific CD4 T cells. However, they elicited qualitatively different cytokine responses. OVA-POL treatment led to 10-fold higher (mean of six independent LDA experiments) frequencies of IFN-γ-producing cells, and a mean fivefold lower frequency of IL-10-producing cells, than was observed following in vivo administration of unmodified OVA. Thus, the high MW polymerized form of antigen acted to steer commitment of naive (for this antigen) CD4 T-cell activation from a situation in which IL-10 producers outnumbered IFN-γ-producing cells by a factor of 4:1 (found in mice administered OVA), to one where IFN-γ producers dominated by a factor of 11:1 (in mice given OVA-POL), i.e. a qualitative shift in the nature of the OVA-specific response induced from Th2-1ike to Th1-like. In vivo co-administration of anti-IFN-γ monoclonal antibody (mAb) abolished the capacity of OVA-POL to preferentially elicit Th1-like dominance. Interestingly. although the ratios of IFN-γ:IL-4 and IFN-γ:IL-10 OVA-specific precursor frequencies were strongly increased following OVA-POL exposure (mean 18- and 47-fold higher), the frequency of IL-4-producing CD4 T cells did not differ significantly. The data suggest that this modified antigen promotes in vivo commitment of naive T cells towards a Th1-like response, with consequent inhibition of IgE and enhancement of IgG2a responses, not through direct effects on IL-4 production, but via decreased frequencies of IL-10 and increased frequencies of IFN-γ-producing OVA-specific CD4 cells. Collectively, the data (1) demonstrate the ability to manipulate commitment of antigen-driven CD4 T-cell populations in naive mice to specific patterns of cytokine gene expression, and (2) provide in vivo evidence of the regulatory role played by IFN-γ in limiting induction and/or expansion of IL-4- and IL-10-producing CD4 cells to protein allergens. [ABSTRACT FROM AUTHOR]

Published

1996

135. Bone marrow-derived chimerism in non-irradiated, cyclosporin-treated rats receiving microvascularized limb transplants: evidence for donor-derived dendritic cells in recipient lymphoid tissues.

Author

Talmor, M., Steinman, R M., Codner, M. A., Chen, M., Harper, A. D., Witmer-Pack, M. D., and Hoffman, L. A.

Subjects

BONE marrow transplantation, ANTIGENS, IMMUNOLOGICAL tolerance, MOSAICISM, HEMATOPOIETIC system, IMMUNOSUPPRESSION, CYCLOSPORINE, MAJOR histocompatibility complex, TRANSPLANTATION immunology

Abstract

Tolerance to donor transplantation antigens develops when recipients are made chimeric with donor bone marrow. To establish chimerism, the haemopoietic system of recipients typically is severely compromised. We report on a system in which chimerism develops without ablative therapies. Immunosuppression with cyclosporin A allowed the lower limb of a rat to be replaced by a microvascularized transplant from a fully allogeneic donor. Many donor-derived cells populated recipient lymph nodes and spleen, and most had the large size, irregular shape and strong major histocompatibility complex (MHC) class II expression that typify dendritic cells. Donor ceils were not found in the macrophage-rich regions of lymphoid tissues, but instead occupied splenic white pulp and lymph node cortex. The donor cells were derived from radiosensitive marrow precursors, as chimerism was abolished if the grafted limb was irradiated, or if muscle and skin flaps devoid of bone were grafted. Donor cells were rare or not detectable in blood, thymus and liver. Whereas lymphoid chimerism was prominent following limb transfer, donor cells were not detected 1–2 weeks after an injection of two femur equivalents of a marrow suspension. We suggest that dendritic cells that undergo rapid turnover in lymphoid organs are replaced from allogeneic precursors in bone grafts. The combination of cyclosporin and vascularized bone provides a means for inducing chimerism in lymphoid tissues of non-irradiated recipients. [ABSTRACT FROM AUTHOR]

Published

1995

136. Development and antigen specificity of the lymphoproliferation response of pigs to pseudorabies virus: dichotomy between secondary B- and T-cell responses.

Author

Kimman, T. G., De Bruin, T. M. G., Voermans, J. J. M., Peeters, B. P. H., and Blanchi, A. T. J.

Subjects

IMMUNE response, ANTIGENS, IMMUNOSPECIFICITY, CELL proliferation, AUJESZKY'S disease virus, B cells, T cells

Abstract

To better understand the contribution of T cells to the immunity of pigs to pseudorabies virus (PRV), we examined the lymphoproliferation response to this virus. Depletion studies demonstrated that both CD2+ CD8+ and CD2+ CD4+ cells contributed to lymphoproliferation, but to varying degrees upon stimulation with live and ultraviolet (UV) light-inactivated PRV. Flow cytometric analysis revealed the emergence of both CD2+CD8+ and CD2+CD4+ lymphoblastoid cells. To examine the contribution of specific viral proteins, we prepared immortalized porcine B cells of haplotype d/d that stably expressed a single PRV protein, and used these cells for in vitro stimulation of lymphocytes from PRV-immune miniature pigs of the same haplotype. Cells expressing PRV gB or gC induced proliferation. An immunization/challenge experiment showed that the lymphoproliferation response was stronger upon immunization with the virulent NIA-3 strain than with the attenuated Bartha strain. Upon challenge inoculation, the NIA-3-immunized pigs were almost completely immune, in contrast to the Bartha-immunized pigs. Such poorly protected pigs showed secondary B- and T-cell immune responses upon challenge. In contrast, the better protected NIA-3-immunized pigs did not show a secondary B-cell response. However, they developed a secondary lymphoproliferation response, which was quicker and stronger than in the Bartha-immunized pigs. This dichotomy between secondary B- and T-cell responses indicates that an effective T-cell memory response is able to quickly eliminate challenge virus in immune pigs, so preventing a secondary B-cell response. [ABSTRACT FROM AUTHOR]

Published

1995

137. Induction of T-cell hyporesponsiveness by intrahepatic modulation of donor antigen-presenting cells.

Author

Chung, S. W., Gorczynski, R. M., Dziadkowiec, I., and Levy, G. A.

Subjects

T cells, LYMPHOCYTES, ANTIGENS, IMMUNITY, IMMUNOGLOBULINS, CELL proliferation

Abstract

In this study, we examined the ability of varying populations of donor cells from B6 mice to induce hyporesponsiveness in T lymphocytes from C3H mice in vitro and in vivo. Small, resting B lymphocytes were inefficient stimulators of T-lymphocyte proliferation compared to splenic mononuclear cells (SMNC) and lipopolysaccharide (LPS)-induced B-cell blasts in vitro (P < 0.05). Pretreatment of SMNC with anti-B7-1 or anti-intracellular adhesion molecule-1 (ICAM-1) monoclonal antibodies (mAb) similarly resulted in inefficient stimulation of T-cell proliferation in vitro (P < 0.05). However, in vivo, only intrahepatic, but not intravenous, injection of donor cells into C3H mice resulted in decreased T-lymphocyte proliferation in response to restimulation by alloantigen. This effect was most pronounced following intrahepatic injection of resting B lymphocytes or SMNC pretreated with anti-ICAM-1 mAb compared to uninjected or intravenously injected mice (P < 0.05). The hyporesponsiveness was associated with an increased production of interleukin-4 (IL-4) by the responder T lymphocytes and correlated with enhanced skin allograft survival. These data demonstrate that intrahepatic injection of donor-derived cells induces T-lymphocyte hyporesponsiveness. The mechanism appears to be modulated by an ICAM-1-mediated signal resulting in expansion of an IL-4-producing T-lymphocyte population. [ABSTRACT FROM AUTHOR]

Published

1995

138. Different migration patterns of antigen-presenting cells correlate with Th1/Th2-type responses in mice.

Author

Morikawa, Y., Tohya, K., Ishida, H., Matsuura, N., and Kakudo, K.

Subjects

EMIGRATION & immigration, ANTIGENS, IMMUNITY, ALLERGIES, IMMUNOLOGIC diseases, ANTIVIRAL agents

Abstract

Antibodies are produced when antigen-presenting cells (APC) pulsed with an antigen are injected intravenously (i.v.) into BALB/c mice, but subcutaneous (s.c.) injection of such APC causes delayed-type hypersensitivity (DTH). To identify the anatomic sites where T and B cells are activated, we labelled splenic dendritic cells (DC) with a fluorochrome, PKH 26, injected them i.v. or s.c., and used the label to locate them. When the DC were injected i.v., germinal centres in the spleen were hyperplastic on day 1. Most DC moved to T-dependent areas of the white and red pulp on day I and remained there at least until day 5, but no DC migrated into the lymph nodes. When the DC were injected s.c., they were in the sinus on day 1 and had entered T-dependent area of draining lymph nodes only by day 3; hyperplasia of germinal centres in the spleen and migration of DC into the spleen were not found. We used the polymerase chain reaction (PCR) to study which mice had spleen cells and lymph node cells that produced the cytokines interleukin (IL)-2, IL-4, IL10, and interferon-γ (IFN-γ). In the sensitization phase, day I after DC injection i.v., almost all IL10 transcript was found in spleen cells, but after DC injection s.c., IL-2 message was most abundant in lymph node cells. The expression of mRNA for IL-4 and IFN-γ in mice that received DC i.v. was not different from that in mice that received DC s.c. in this phase. Immunohistochemical staining showed that cells stained for IL-10 were in the T-dependent area of the spleen from mice that received DC i.v. 1 day after the injection. Three days after the injection of DC i.v., cells stained for IL-10 were in the germinal centres as well. The number of such cells in the spleen of mice that received DC i.v. was significantly more than that in mice that received DC s.c. IL-10 may be important in development of TH2 response. [ABSTRACT FROM AUTHOR]

Published

1995

139. Antigen processing and presentation.

Subjects

ANTIGENS, ENDOPLASMIC reticulum, ORGANELLES, PROTEINASES, PROTEOLYTIC enzymes, MHC antibodies, MAJOR histocompatibility complex, IMMUNOGENETICS

Abstract

Presents several abstracts related to antigens. "Generation of Class 1 Restricted Epitopes in the Cytosol and in the Endoplasmic Reticulum of Processing Mutant Cells," V. Cerundolo, T. Elliott, A. Kelly, A. Townsend; "How Special are the Proteinases for Antigen Processing?," by B M Chain; "Intracellular Transportation Pathways of Major Histocompatibility Complex Class II Molecules," by Jean Pieters, Desirée Verwoerd, and Berhard Dobberstein.

Published

1994

140. Human IgG subclass responses and subclass restriction to <em>Schistosoma mansoni</em> egg antigens.

Author

Langley, J. G., Kariuki, H.C., Hammersley, A. P., Ouma, J. H., Butterwort, A. E., and Dunne, D. W.

Subjects

IMMUNE response, IMMUNOLOGY, ANTIGENS, IMMUNITY, IMMUNOGLOBULINS, SCHISTOSOMA mansoni

Abstract

In areas endemic for schistosomiasis, there is great heterogeneity in antibody isotype responses to parasite antigens amongst infected individuals. At the population level, the isotype composition of antibody responses undergoes dynamic changes which are associated with the age of infected individuals. Here we examine the IgG subclass responses to Schistosoma mansoni eggs (soluble egg antigens; SEA) of infected individuals by immunoblot and ELISA. By controlled treatment of SEA-coated ELISA plates and immunoblot nitrocellular strips with sodium periodate, in order to oxidize terminal carbohydrate residues selectively, we were able to relate individuals subjects' isotype responses to the different antigens that they responded to, and to the presence of putative carbohydrate and peptide epitopes on those antigens. IgG2 responses were restricted strictly to sodium periodate-sensitive carbohydrate epitopes and antigens of relatively high molecular weight. These antigens were not usually recognized by other isotypes and, therefore, they were only recognized by individuals who had high levels of IgG2. IgG1 and IgG3 responses were directed against both carbohydrate and peptide epitopes, whereas IgG4 responses were restricted to periodate-resistant epitopes. This suggests that the fall in IgG2 responses, and reciprocal rise in IgG4 antibodies, seen in young children as their intensities of schistosome infection increase, is not the result of isotype switching, and that, if these two subclasses are involved in blocking immunity to schistosomiasis, they are operating independently. [ABSTRACT FROM AUTHOR]

Published

1994

141. Recognition of a CD4+ mouse medullary thymocyte subpopulation by <em>Amaranthus leucocarpus</em> lectin.

Author

Lascurain, R., Chávez, R., Gorocica, P., Pérez, A., Montaño, L. F., and Zenteno, E.

Subjects

LECTINS, AMARANTHS, PEANUTS, ANTIGENS, IMMUNITY, PLANT immunology, IMMUNOLOGY

Abstract

We have used the Galβ(l→3)GalNAc-specific Amaranthus leucocarpus lectin to isolate a thymus cell subpopulation which is different from that sorted with Arachis hypogaea lectin. The cells recognized by A. leucocarpus lectin were predominantly CD4+, whereas a minor proportion of CD8+ cells (approximately 11%) were also identified. The A. leucocarpus-positive cells were located in the thymus medulla and the cortico-medullary junction. The cortex was negative for A. leucocarpus cells. [ABSTRACT FROM AUTHOR]

Published

1994

142. Antigen-specific human immunoglobulin production in SCID mice transplanted with human peripheral lymphocytes is dependent on CD4+ CD45RO+ T cells.

Author

Mártensson, C., Kristensson, K., Kalliomäki, S., Borrebaeck, C. A. K., and Carlsson, R.

Subjects

MICE, T cells, SERUM, IMMUNOGLOBULINS, LYMPHOCYTES, BLOOD, IMMUNIZATION, ANTIGENS

Abstract

Severe combined immunodeficient (SCID) mice, lacking mature T and B cells and virtually devoid of endogenous serum immunoglobulins, spontaneously produce large amounts of human immunoglobulin after transplantation with human peripheral blood lymphocytes (PBL). Moreover, after immunization with antigen an active immune response resulting in a production of specific antibodies can be induced. Here we report that human T cells must be co-transplanted with B cells into the SCID mice for immunoglobulin production to occur. Resting human B cells could be activated to immunoglobulin production in the absence of human monocytes and a specific antibody response to tetanus toxoid (TT) could be induced, suggesting that the human B cells could present antigen to T cells in the SCID environment. Production of human immunoglobulins, as well as specific antibodies, was obtained only if CD4+ T cells of the memory phenotype, i.e. expressing CD45RO, were present. No human immunoglobulin, either of IgM or of IgG isotype, was found in SCID sera if mice were co-transplanted with human B cells and CD45RA expressing CD4+ T cells. However, FACS analysis revealed that the transplanted CD45RA+ cells became activated and differentiated towards CD45RO+ cells within 1-2 weeks. These cells also gained the lymphokine gene expression pattern associated with CD45RO+ cells, as demonstrated by polymerase chain reaction (PCR) analysis, and could support immunoglobulin production in SCID mice transplanted with fresh B cells. In fact, after differentiation of CD4+ CD45RA+ T cells towards expression of CD45RO, either in vivo in the SCID mouse or in vitro, these cells could interact with and activate human B cells to immunoglobulin production. [ABSTRACT FROM AUTHOR]

Published

1994

143. Differential function of dendritic cells isolated from blood and lymph nodes.

Author

Hill, S., Coates, J. P., Kimber, I., and Knight, S. C.

Subjects

DENDRITIC cells, LYMPH nodes, SPLEEN, MICE, PROTEINS, ANTIGENS, IMMUNE response, CHEMICALS

Abstract

Dendritic cells (DC) isolated from the lymph nodes or spleens of mice and pulsed with contact sensitizers or protein antigens stimulate primary proliferative responses by syngeneic T cells and responses to alloantigens in the mixed leucocyte reaction (MLR). Using enriched human peripheral blood DC, we attempted to stimulate primary immune responses to contact sensitizers by autologous lymphocytes/n vitro. No significant proliferation above background levels or CD69 expression (an early activation antigen on lymphocytes) was detected despite using a wide range of donors, chemicals, antigens and cell concentrations. Culture of DC for up to 5 days in vitro in the presence of phytohaemagglutinin (PHA)-conditioned culture supernatants, or recombinant granulocyte-macrophage colony-stimulating factor (GM-CSF) also failed to induce primary proliferative responses to contact sensitizers. Comparisons were made between blood and lymph node DC from mice to explore whether the lack of stimulation was the result of differences between mouse and human DC or between DC isolated from different tissues. DC from lymph nodes stimulated primary responses to contact sensitizers in both blood and lymph node lymphocytes whereas blood DC did not stimulate responses. Both lymph node and blood DC stimulated an allogeneic MLR, although blood DC were less efficient than those from lymph node. The data show that DC from different tissues exhibit variable functional activity. DC from blood and lymph nodes were examined to determine whether surface antigen expression is related to functional activity. Murine blood DC expressed similar levels of LFA-1, LECAM-1 and CD44 compared with lymph node DC but lower levels of MHC class if, B7 and ICAM-1. These results may therefore have important implications for antigen processing and presentation in cells from different tissue compartments. [ABSTRACT FROM AUTHOR]

Published

1994

144. Antibodies to human and non-human primate cellular and culture medium components in macaques vaccinated with the simian immunodeficiency virus.

Author

Bergmeier, L. A., Walker, J., Tao, L., Cranage, M., and Lehner, T.

Subjects

SIMIAN viruses, T cells, INFECTION, IMMUNIZATION, ANTIGENS, IMMUNOGLOBULINS, MITOGENS, ANIMALS

Abstract

Inactivated simian immunodeficiency virus (SIV) grown in a human T-cell fine induces protection from infection by the virus in macaques. However, observations that immunization with uninfected human T cells or with SIV-1 prepared in human T cells can also induce protection, has raised the possibility that protective antigens could be of human cellular origin. Sera from animals immunized with fixed infected and uninfected human T cells, as well as from animals immunized with partially purified cell-free SIV have been examined for their ability to bind to human and macaque peripheral blood mononuclear cells (PBMC) and to components present in fetal calf serum (FCS) in which the cells were grown. Analysis by flow cytometry suggests that antibodies to human cell surface antigens can be elicited with both inactivated SIV grown in human T cells and by uninfected T cells. There was a significant association between the presence of anti-cell antibodies and protection from infection. However, anti-cell surface antibodies were not detected with macaque mononuclear cells by flow cytometry or by immunoprecipitation, unless these cells were first treated with FCS or activated by a mitogen. Immunoprecipitation of resting human PBMC with sera from immunized animals suggests the presence of antibodies to class I heavy and fight chains [β2-microglobulin (β2m)] and to bovine β2m, which may originate in FCS used to grow the cell fine. Antibodies to CIM were also found in sera from animals immunized with SIV grown in human T cells. We suggest that human cellular components augmented by FCS elicit anti-class I heavy chain, β2m, CD4 and FCS antibodies which may be responsible for protection against SIV infection in macaques. [ABSTRACT FROM AUTHOR]

Published

1994

145. Monoclonal antibodies to leucosialin (CD43) induce homotypic aggregation of the human mast cell line HMC-1: characterization of leucosialin on HMC-1 cells.

Author

Weber, S., Ruh, B., Dippel, E., and Czarnetzki, B.M.

Subjects

MONOCLONAL antibodies, MAST cells, CELL lines, LEUCOCYTES, MOLECULAR weights, ANTIGENS

Abstract

CD43 (leucosialin, sialophorin) is the major sialoprotein of nearly ail circulating leucocytes and has important biological activities in cellular differentiation and activation. Recently, the expression of CD43 has also been demonstrated on mast cells and basophils by flow cytometry. In order to further characterize mast cell/basophil leucosialin we have investigated CD43 on the human mast cell line HMC-1, the human basophilic precursor cell line KU-812, and the human promonocytic cell line U-937. The apparent molecular weights (MW) were 123,000 (HMC-1 and KU-812) and 144,000 (U-937) by Western blot analysis. Expression of CD43 on HMC-1 was down-regulated after stimulation with phorbol myristate acetate (PMA). Three monoclonal antibodies (mAb) specific for human CD43 induced homotypic mast cell line (HMC-1) aggregation in a semi-quantitative assay, a phenomenon that has not been described before with mast cells. Monoclonal antibodies specific for seven other surface antigens and an irrelevant mAb of the same isotype had no effect. The level of aggregation was dependent on anti-CD43 mAb concentration, time and temperature. Anti-leucosialin-induced aggregation of HMC-1 cells was completely inhibited by mAb against CD11a (LFA-1) and CD18 (β2-chain). Monoclonal antibody to CD54 (ICAM-1) partially inhibited anti-CD43-induced homotypic aggregation, while antiCD11b (CR3), anti-CD11c (p 150, 95) and a control mAb had no inhibitory effect. We conclude that mast cell line CD43 antigen expression is differentially regulated during cell activation, and speculate that anti-CD43-induced homotypic aggregation of HMC-1 cells is closely associated with modulation of β2-integrins. [ABSTRACT FROM AUTHOR]

Published

1994

146. Differences in non-MHC alloantigens promote tissue rejection but fail to mediate allogeneic co-operation and autoimmunity in mice neonatally injected with semi-allgeneic F1 B cells.

Author

Ramos, A., Merino, R., and Merino, J.

Subjects

ANTIGENS, B cells, LYMPHOCYTES, IMMUNOGLOBULINS, IMMUNITY, CUTANEOUS tuberculosis

Abstract

Mice injected at birth with semi-allogeneic lymphoid cells develop a lupus-like autoimmune syndrome in which donor B cells are polyclonally activated by host alloreactive CD4+ T cells, producing autoantibodies and immune complex-mediated glomerulonephritis. It has been demonstrated that the recognition of major bistocompatibility complex (MHC) class II alloantigens triggers the development of a complete disease. But differences in either MHC class I molecules or Mls-l antigens are not sufficient to induce production of autoantibodies. Here we have investigated whether differences in other non-MHC alloantigens could induce a similar autoimmune disease and whether the maternal environment could modulate the T-B allogeneic co-operation in this model. For this purpose (BALB/c × BC20)F1 hybrid females were backcrossed with BC20 males. R2 mice obtained in this backcross were neonatally injected with 108 (C57BL/6 × BALB.Igb')F1 spleen cells and the tolerance against maternal derived BALB/c alloantigens as well as the development of autoimmune manifestations were subsequently evaluated. In contrast to R2 mice injected at birth with (C578L16 &times BALB.Igb')F1 cells, control R2 mice rejected skin grafts from BALB/c mice and B cells from (C57BL/6 × BALB.Igb')F1 mice, independently of their H-2 haplotype (H-2b/d or H-2b/b). Nevertheless, after neonatal injection of (C57BL/6 × BALB.Igb)F1 cells, none of 19 H-2b/d R2 injected mice presented autoimmune manifestations, in contrast with the typical autoimmune disease observed in all neonatally injected H-2b/b R2 mice (26 mice). These results support that the development of autoimmunity in this model depends exclusively upon differences in MHC class II alloantigens and that the relationship between mother and fetus, through the pregnancy or the breast suckling, is not sufficient to inhibit cytolytic and allo-helper responses against non-inherited maternal-derived alloantigens. [ABSTRACT FROM AUTHOR]

Published

1994

147. Antigen recognition and activation of ovine γδ T cells.

Author

Evans, C. W., Lund, B. T., McConnell, I., and Bujdoso, R.

Subjects

ANTIGENS, T cells, BABESIOSIS, CELL proliferation, TUBERCULOSIS, MYCOBACTERIAL diseases, SHEEP

Abstract

We have investigated several aspects of γδ T cells in sheep. γδT cells of sheep express a unique transmembrane protein termed T19 but lack the expression of particular cell-surface molecules such as CD2, CD4 and CD8 which are typically associated with αβ T cells. The majority of γδ T cells isolated from animals of all ages examined lacked the expression of CD45RA. A faster rate of activation by γδ T cells compared to either CD4 or CDS T cells was seen in the time-course of IL-2 receptor a chain (CD25) cell-surface expression. All γδ T cells expressed the CD25 protein within 8 hr of activation whereas the majority of CD4 or CD8 T cells did not express CD25 until 24 hr post-concanavalin A (Con A) stimulation. This difference in the rate of expression of activation molecules was not restricted to CD25, as a similar trend was seen with cell-surface expression of major histacompatibility complex (MHC) class II molecules. We have used the distinct phenotypic profile of ovine γδ T cells to purify these cells by positive selection via the T cells molecule to assess their in vitro proliferative response to various antigens. Routinely, cell populations comprising more than 93% γδ T cells with yields of approximately 55% were obtained. Purified γδ T cells were capable of responding to Mycobacterium tuberculosis antigen in a primary and secondary in vitro proliferation assay and to ovalbumin in a secondary response. Ovine γδ T cells showed little, if any, proliferative response to allogeneic stimulator cells. [ABSTRACT FROM AUTHOR]

Published

1994

148. A novel internal antigen which distinguishes germinal centre cells from other B-cell types.

Author

Pulford, K., Micklem, K. J., Jones, M., Pezzella, F., Mayne, K. M., Morrison, H., Thomas, J., Falini, B., Norton, A., and Mason, D. Y.

Subjects

ANTIGENS, GERMINAL centers, MONOCLONAL antibodies, B cells, IMMUNOGLOBULINS, LYMPHOCYTIC leukemia, LYMPHOPROLIFERATIVE disorders

Abstract

A new monoclonal antibody, 4KB51, is described which labels the majority of B ceils in blood and in mantle and marginal zones but not germinal centre lymphocytes or plasma cells. Antibody 4KB51 also stains monocytes, neutrophils and the majority of T cells. It recognizes an intracellular antigen of 160,000 MW (unreduced) and 68,000 MW (reduced). Antibody 4KB51 labels the turnout cells in all cases of hairy cell leukaemia and in four of the 16 cases of centrocytic B-cell lymphoma studied. No labelling of the other lymphomas (114 cases) or lymphoid leukaemias (13 cases) tested was seen. Antibody 4KB51 may be of value in defining B-cell subsets and in the differential diagnosis of hairy cell leukaemia and centrocytic lymphomas. The pattern of reactivity of 4KB51 suggests that its target antigen may play a functional role, possibly involved in lymphocyte homing. [ABSTRACT FROM AUTHOR]

Published

1994

149. Expression on procine γδ lymphocytes of a phylogenetically conserved surface antigen previously restricted in expression to ruminant γδ T lymphocytes.

Author

Carr, M.M., Howard, C.J., Sopp, P., Manser, J.M., and Parsons, K.R.

Subjects

LYMPHOCYTES, T cells, IMMUNE system, SWINE, ANTIGENS, IMMUNOLOGY, LEUCOCYTES

Abstract

A 180,000 MW molecule has been identified on porcine leucocytes that is the homologue of the 215,000/300,000 MW WC1 (T19) leucocyte antigen previously considered to be restricted to ruminants. In ruminants the WC1 molecule is expressed by a T-cell subpopulation that is CD2-CD4-CD8-CD5+ and that is γδ T-cell receptor positive (TcR+). In pigs, the 180,000 MW molecule, identified by a new monoclonal antibody CC101, is expressed by a γδ TcR+ T-cell subpopulation that is also CD2-CD4 CD8. The p180+ cells are a major T-cell subpopulation comprising approximately 40% of the peripheral blood mononuclear cells from 6-9-month-old pigs. Expression of p180 identifies the majority of the CD2-CD4-CD8- T cells in porcine blood. The p180+ T cells have a distribution in lymphoid tissues that is distinct from that oft cells that express the CD2, CD4 or CD8 molecules. They are evident particularly in the thymic medulla, the epithelium, lamina propria and interfollicular areas of the small intestine, and the superficial dermis of the skin, but largely absent from conventional T-dependent areas of secondary lymphoid tissue. [ABSTRACT FROM AUTHOR]

Published

1994

150. Biochemical and functional alterations induced by CD23 ligation in the human promonocytic cell line U937.

Author

Paul-Eugene, N., Amirand, C., Ouaaz, F., Ballini, J.-P., Mossalayi, D.M., Dugas, B., and Kolb, J.-P.

Subjects

INTERLEUKIN-4, MONOCLONAL antibodies, MONOCYTES, PHOSPHOINOSITIDES, ANTIGENS, LEUCOCYTES

Abstract

The early events triggered in interleukin-4 (IL-4)-stimulated U937 cells by ligation of CD23/FcεRII with specific monoclonal antibodies (mAb) were analysed, as a model of the action of this molecule on the differentiation of promonocytic cells. As well as IL-4-activated human monocytes, addition of anti-CD23 mAb to IL-4-treated U937 cells triggered cAMP accumulation but did not evoke significant polyphosphoinositide hydrolysis. However, by a microspectrofluorometric technique allowing single cell analysis, anti-CD23 mAb was found to elicit calcium mobilization in these cells. In addition, the treatment induced phenotypic alterations in these cells, as evidenced by the acquisition of the monocyte marker CD14 and the increase of the α-chain (CD11a) and of the common β-chain (CD18) of the leucocyte function-associated antigen 1 (LFA-1) family antigens. Although weaker than in monocytes, CD23 ligation evoked a small secretion of the pro-inflammatory mediators IL-6 and thromboxane B2. These data suggest that a significant maturation of promonocytic cells towards a more mature monocytic phenotype can be achieved through successive exposure to IL-4 and CD23 ligation. [ABSTRACT FROM AUTHOR]

Published

1993