Uncovering of Functional Alternative CTLA-4 Counter-Receptor in B7-Deficient Mice

Freeman, Gordon J.; Borriello, Frank; Hodes, Richard J.; Reiser, Hans; Hathcock, Karen S.; László, Glória; McKnight, Andrew J.; Kim, Jinny; Du, Lingyao; Lombard, David B.; Gray, Gary S.; Nadler, Lee M.; Sharpe, Arlene H.

doi:10.1126/science.7694362

Cited by 354 publications

(155 citation statements)

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“…Although DC express several other important intercellular adhesion and costimulatory molecules, including CDUa, CD40, CD44, CD48/58, and CD54, B7-2 (CD86) appears to be the major CD28/CTLA-4 ligand and accounts for the costimulation provided by this pathway during in vitro T-cell responses. The early and sustained expression ofB7-2 mRNA (within 8 hr) <before maximal B7-1 expression) in activated murine B cells (30) suggests that it may provide a critical signal involved in the decision between activation or inactivation of T cells within 24 hr of stimula- tion (31,32). Moreover, APC from B7-1 "knockout" mice that express B7-2 are competent APC (30).…”

Section: Discussionmentioning

confidence: 99%

“…The early and sustained expression ofB7-2 mRNA (within 8 hr) <before maximal B7-1 expression) in activated murine B cells (30) suggests that it may provide a critical signal involved in the decision between activation or inactivation of T cells within 24 hr of stimula- tion (31,32). Moreover, APC from B7-1 "knockout" mice that express B7-2 are competent APC (30). MHC class II+ DC progenitors that are B7-2-may (as is the case with inhibition of B7-2 expression 127]) allow T cell receptor-mediated signaling events to occur, but inhibit the distinct costimulatory signaJ(s) that is necessary for optimal cytokine production and cytokine-dependent T-cell proliferation.…”

Section: Discussionmentioning

confidence: 99%

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COSTIMULATORY MOLECULE-DEFICIENT DENDRITIC CELL PROGENITORS (MHC CLASS II+, CD80dim, CD86-) PROLONG CARDIAC ALLOGRAFT SURVIVAL IN NONIMMUNOSUPPRESSED RECIPIENTS12

et al. 1996

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We have shown previously that granulocyte-macrophage colony-stimulating factor-stimulated mouse bone marrow-derived MIIC class II+ dendritic cell (DC) progenitors that are deficient in cell surface expression of the costimulatory molecules B7-1 (CD80) and B7-2 (CD86) can induce alloantigen-specific T-cell anergy in vitro. To test the in vivo relevance of these findings, 2x 10 6 BI0 (H2 b ) mouse bone marrow-derived DC progenitors (NLDC 145+, MIIC class II+, B7-1 ditn , B7_2-/dim ) that induced T-cell hyporesponsiveness in vitro were injected systemically into normal C3H (H2k) recipients. Seven days later, the mice received heterotopic heart transplants from BI0 donors. No immunosuppressive treatment was given. Median graft survival time was prolonged significantly from 9.5 to 22 days. Median graft survival time was also increased, although to a lesser extent (16.5 days), in mice that received third-party (BALB/c; H2 d ) DC progenitors. Ex vivo analysis of host T-cell responses to donor and third-party alloantigens 7 days after the injection of DC progenitors (the time of heart transplant) revealed minimal anti-donor mixed leukocyte reaction and cytotoxic T lymphocyte reactivity. These responses were reduced substantially compared with those of spleen cells from animals pretreated with "mature" granulocyte-macrophage colony-stimulating factor + interleukin-4-stimulated DC (MHC class nbr'ght, B7-1 +, B7_2brlght), many of which rejected their heart grafts in an accelerated fashion. Among the injected donor MHC class 11+ DC progenitors that migrated to recipient secondary lymphoid tissue were cells that appeared to have up-regulated cell surface B7-1 and B7-2 molecule expression. This observation may explain, at least in part, the temporary or unstable nature of the hyporesponsiveness induced by the DC progenitors in nonimmunosuppressed recipients.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

COSTIMULATORY MOLECULE-DEFICIENT DENDRITIC CELL PROGENITORS (MHC CLASS II+, CD80dim, CD86-) PROLONG CARDIAC ALLOGRAFT SURVIVAL IN NONIMMUNOSUPPRESSED RECIPIENTS12

et al. 1996

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“…Indeed, in a recent study, anti-CDBO (B7-1) mAbs failed to inhibit human dendritic Langerhans cell-induced alloactivation of T cells (4Jl. Early and sustained expression of B7-2 mRNA (within 8 hr) (before maximal B7-1 expression) in activated murine B cells (42), suggests that it may provide a critical signal (within the first 24 hr) involved in the decision between activation or inactivation of T cells within 24 hr of stimulation (43,44). Moreover, APCs from mice in which the B7-1 gene has been "knocked out" express B7-2 and are competent APCs (42).…”

Section: Discussionmentioning

confidence: 99%

BONE MARROW-DERIVED DENDRITIC CELL PROGENITORS (NLDC 145+, MHC CLASS II+, B7-1dim, B7-2−) INDUCE ALLOANTIGEN-SPECIFIC HYPORESPONSIVENESS IN MURINE T LYMPHOCYTES1,2

et al. 1995

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The functional maturation of dendritic cells (DC) and other antigen-presenting cells is believed to reflect the upregulation of cell surface major histocompatibility complex (MHC) class II and other T cell costimulatory molecules, especially the CD28 ligands B7-1 (CD80) and B7-2 (CD86). In this study, we propagated cells exhibiting characteristics of DC precursors from the bone marrow (BM) of BIO mice (H_2 b ; I-A +) in response to granulocyte-macrophage colony stimulating factor (GM-CSF). The methods used were similar to those employed previously to propagate DC progenitors from normal mouse liver. Cells expressing DC lineage markers (NLDC 145+, 33Dl +, N418+) harvested from 8-tO-day GM-CSF stimulated BM cell cultures were CD45+, heat-stable antigen+, CD54+, CD44+, MHC class 11+, B7_1 dbn but B7-2-(costimulatory molecule-deficient). Supplementation of cultures with interleukin-4 (IL-4) in addition to GM-CSF however, resulted in marked upregulation of MHC class II and B7-2 expression. These latter cells exhibited potent allostimulatory activity in primary mixed leukocyte cultures. In contrast, the cells stimulated with GM-CSF alone were relatively weak stimulators and induced alloantigen-specific hyporesponsiveness in allogeneic T cells (C3H; H_2k; I-E+) detected upon restimulation in secondary MLR. This was associated with blockade of IL-2 production. Reactivity to thirdparty stimulators was intact. The hyporesponsiveness induced by the GM-CSF stimulated, costimulatory molecule-deficient cells was prevented by incorporation of anti-CD28 monoclonal antibody in the primary MLR and was reversed by addition of IL-2 to restimulated T cells. The findings show that MHC class 11+ B7-2-cells with a DC precursor phenotype can induce alloantigen-specific hyporesponsiveness in vitro. Under the appropriate conditions, such costimulatory molecule-deficient cells could contribute to the induction of donor-specific unresponsiveness in vivo.

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“…Briefly, 5 g of total RNA was reverse transcribed into cDNA using Moloney murine leukemia virus reverse transcriptase (Life Technologies, Gaithersburg, MD). The cDNA was then amplified using specific primers for B7 Ig V-like exon, as described (41). Amplifications were performed in 2 mM MgCl 2 , 50 mM KCl, 10 mM Tris-HCl (pH 8.3), 0.2 mM of each deoxynucleotide triphosphate, 1 M of each primer, and 2.5 U AmpliTaq polymerase (PerkinElmer/Cetus, Norwalk, CT).…”

Section: Rna Preparation and Rt-pcrmentioning

confidence: 99%

CD80+Gr-1+ Myeloid Cells Inhibit Development of Antifungal Th1 Immunity in Mice with Candidiasis

Mencacci

Montagnoli

Bacci

et al. 2002

The Journal of Immunology

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124

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To find out whether polymorphonuclear neutrophils (PMN), abundantly recruited in disseminated Candida albicans infection, could directly affect the activation of Th cells we addressed the issues as to whether murine PMN, like their human counterparts, express costimulatory molecules and the functional consequence of this expression in terms of antifungal immune resistance. To this purpose, we assessed 1) the expression of CD80 (B7-1) and CD86 (B7-2) molecules on peripheral, splenic, and inflammatory murine Gr-1+ PMN; 2) its modulation upon interaction with C. albicans in vitro, in vivo, and in human PMN; 3) the effect of Candida exposure on the ability of murine PMN to affect CD4+ Th1 cell proliferation and cytokine production; and 4) the mechanism responsible for this effect. Murine PMN constitutively expressed CD80 molecules on both the surface and intracellularly; however, in both murine and human PMN, CD80 expression was differentially modulated upon interaction with Candida yeasts or hyphae in vitro as well as in infected mice. The expression of the CD86 molecule was neither constitutive nor inducible upon exposure to the fungus. In vitro, Gr-1+ PMN were found to inhibit the activation of IFN-γ-producing CD4+ T cells and to induce apoptosis through a CD80/CD28-dependent mechanism. A population of CD80+Gr-1+ myeloid cells was found to be expanded in conventional as well as in bone marrow-transplanted mice with disseminated candidiasis, but its depletion increased the IFN-γ-mediated antifungal resistance. These data indicate that alternatively activated PMN expressing CD80 may adversely affect Th1-dependent resistance in fungal infections.

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Uncovering of Functional Alternative CTLA-4 Counter-Receptor in B7-Deficient Mice

Cited by 354 publications

References 18 publications

COSTIMULATORY MOLECULE-DEFICIENT DENDRITIC CELL PROGENITORS (MHC CLASS II+, CD80dim, CD86-) PROLONG CARDIAC ALLOGRAFT SURVIVAL IN NONIMMUNOSUPPRESSED RECIPIENTS12

COSTIMULATORY MOLECULE-DEFICIENT DENDRITIC CELL PROGENITORS (MHC CLASS II+, CD80dim, CD86-) PROLONG CARDIAC ALLOGRAFT SURVIVAL IN NONIMMUNOSUPPRESSED RECIPIENTS12

BONE MARROW-DERIVED DENDRITIC CELL PROGENITORS (NLDC 145+, MHC CLASS II+, B7-1dim, B7-2−) INDUCE ALLOANTIGEN-SPECIFIC HYPORESPONSIVENESS IN MURINE T LYMPHOCYTES1,2

CD80+Gr-1+ Myeloid Cells Inhibit Development of Antifungal Th1 Immunity in Mice with Candidiasis

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