In the absence of a CD40 signal, B cells are tolerogenic

Suhlmann, Janet E.; Foy, Teresa M.; Aruffo, Alejandro; Crassi, Karen M.; Ledbetter, Jeffrey A.; Green, William R.; Xu, Jinbao; Shultz, Leonard D.; Roopeslan, Derry; Flavell, Richard A.; Fast, Loren D.; Noelle, Randolph J.; Durie, Fiona H.

doi:10.1016/1074-7613(95)90009-8

Cited by 141 publications

(86 citation statements)

References 29 publications

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“…Longterm cardiac alloengraftment was also achieved in 75% of mice after transient administration of anti-CD154 (versus 0% in the control group) [45], and brief treatment with this antibody after transplantation of allogeneic pancreatic islet cells induced indefinite graft survival in approximately 40% of the treated mice and delayed rejection in the remaining recipients, whereas all of the control mice rejected at day 15 [46]. Furthermore, prior transfusion of the recipients with donor lymphocytes (donor-specific transfusion, DST) along with anti-CD154 lead to long-term islet cell survival in 96% of the mice in this study [46], consistent with the observation that allogeneic B cells are a powerful tolerigen if not activated through CD40 [43,44]. Finally, renal allograft rejection in rhesus monkeys was also prevented out to approximately 100 days by transient administration of anti-CD154, at which time re-treatment with the antibody inhibited the rejection process [47].…”

Section: Tolerance Induction To Alloantigensupporting

confidence: 73%

“…Despite the fact that the injected DCs expressed high levels of MHC Class I, MHC Class II, as well as both B7.1 and B7.2 on their surface, allogeneic helper (cytokine production) and cytotoxic T cell responses were found to be greatly diminished in the CD154-deficient mice [unpublished results]. It is not yet clear whether DCs deprived of CD40 maturation signals are actively tolerigenic toward T cells, as has been described for resting B cells [43,44]. However, these data indicate that CD40/CD154 costimulation that occurs in the context of helper T cell/DC cognate interaction is critical for the acquistion of DC antigen-presenting capabilities.…”

Section: The Role Of Cd40 In DC Maturationmentioning

confidence: 99%

“…For instance, the administration of purified allogeneic CD40-deficient B cells or wild-type allogeneic B cells along with anti-CD154 leads to the induction of allotolerance in the CD4 ϩ and CD8 ϩ T cell compartments of the recipient. However, preactivation of the B cells with LPS, accompanied by the induction of high levels of B7.1 and B7.2, restores normal alloreactive T cell responses in these studies [43,44]. Longterm cardiac alloengraftment was also achieved in 75% of mice after transient administration of anti-CD154 (versus 0% in the control group) [45], and brief treatment with this antibody after transplantation of allogeneic pancreatic islet cells induced indefinite graft survival in approximately 40% of the treated mice and delayed rejection in the remaining recipients, whereas all of the control mice rejected at day 15 [46].…”

Section: Tolerance Induction To Alloantigenmentioning

confidence: 99%

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The role of CD40/CD154 interactions in the priming, differentiation, and effector function of helper and cytotoxic T cells

Mackey

Barth

Noelle

1998

Journal of Leukocyte Biology

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197

137

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This review focuses on the emerging body of literature suggesting a critical role for CD40/CD154 interactions in antigen-presenting cell (APC) activation, CD4 ؉ and CD8 ؉ T cell priming, and effector T cell maturation. In this context effective antigen presentation involves not only T cell expansion and long-term survival but also the ability of the APC to guide the T cell response toward the Th1 (interferon-␥ producing) or the Th2 (interleukin-4 producing) phenotype. We suggest a model to explain why CD40/CD154 interactions are critical for some helper and cytotoxic T cell responses, whereas others occur independently of this receptor/ligand pair. In addition, we will discuss the potential role for CD40/CD154 interactions in effector T cell maturation and cytokine production.

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Section: Tolerance Induction To Alloantigensupporting

confidence: 73%

Section: The Role Of Cd40 In DC Maturationmentioning

confidence: 99%

Section: Tolerance Induction To Alloantigenmentioning

confidence: 99%

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The role of CD40/CD154 interactions in the priming, differentiation, and effector function of helper and cytotoxic T cells

Mackey

Barth

Noelle

1998

Journal of Leukocyte Biology

Self Cite

197

137

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“…In other models of tolerance, B cells induce CD8 ϩ suppressor T cells when peptides are presented in the context of the nonclassical class I molecule Qa-1 (10). Coupled with other studies showing that B cells can serve as tolerogenic APC (11)(12)(13)(14)(15)(16), these results suggested that the B cell might present Ag in the ACAID spleen.…”

mentioning

confidence: 72%

Ocular Immune Privilege Promoted by the Presentation of Peptide on Tolerogenic B Cells in the Spleen. II. Evidence for Presentation by Qa-1

D’Orazio¹,

Mayhew

Niederkorn

2001

The Journal of Immunology

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Ocular immune privilege is the result of several unique features of the eye, including the systemic down-regulation of Th1 immune responses to Ags encountered in the anterior chamber of the eye—a phenomenon termed anterior chamber-associated immune deviation (ACAID). The induction of ACAID requires the participation of three cell populations: the ocular ACAID APC, the splenic B cell, and the splenic T cell. Because B cells have been implicated in tolerogenic Ag presentation in other systems, we hypothesized that B cells were responsible for the induction of regulatory T cells in ACAID. The central hypothesis for this study is that APC from the eye migrate to the spleen where they release antigenic peptides (OVA) that are captured and presented to T cells by splenic B cells. A combination of in vitro and in vivo studies demonstrated that splenic B cells, incubated with ACAID APC in vitro, were capable of inducing ACAID when transferred to naive mice. The induction of ACAID required the normal expression of β2-microglobulin on both the B cell and ACAID APC, but not on the T suppressor cells. Moreover, the induction of ACAID regulatory cells required histocompatibility between the B cells and regulatory T cells at the TL/Qa region. The results indicate that: 1) B cells are necessary for the induction of ACAID; 2) ACAID B cells do not directly suppress the expression of delayed-type hypersensitivity; and 3) the induction of Ag-specific regulatory T cells by ACAID B cells requires histocompatibility at the TL/Qa region.

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“…Indeed, treatment with anti-CD154 mAb diminished the response to alloantigen on B cells in vitro (18), whereas immunization with resting B cells from CD154 Ϫ/Ϫ mice induced tolerance to alloantigen (19). Treatment with anti-CD154 mAb blocks both primary and secondary immune responses to T cell-dependent Ags, as well as the development of germinal centers and the generation of memory cells (20).…”

Section: Discussionmentioning

confidence: 99%

The CD154-CD40 T Cell Costimulation Pathway Is Required for Host Sensitization of CD8+ T Cells by Skin Grafts Via Direct Antigen Presentation

Zhai

Shen

Gao

et al. 2002

The Journal of Immunology

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Although the CD154-CD40 T cell costimulation pathway has been shown to mediate alloimmune responses in normal recipients, little is known about its role in sensitized hosts. In this work, by using novel models of cardiac allograft rejection in skin-sensitized CD154- and CD40-deficient mice, we reaffirm the key role of CD154-CD40 signaling in host sensitization to alloantigen in vivo. First, we identified CD8+ T cells as principal effectors in executing accelerated rejection in our model. Disruption of CD154-CD40 signaling in recipients at the T cell side (CD154-deficient) but not at the APC side (CD40-deficient) abrogated accelerated (<2 days) rejection and resulted in long-term (>100 days) graft survival. This suggests that the CD154-dependent mechanism in host CD8+ T cell sensitization operates via the direct Ag presentation. Then, in comparative studies of alloimmune responses in CD154-deficient and wild-type recipients, we showed that, although alloreactive B cell responses were inhibited, alloreactive T cell responses were down-regulated selectively in the CD8+ T cell compartment, leaving CD4+ T cells largely unaffected. This unique alteration in host alloreactivity, seen not only in peripheral lymphocytes but also in allograft infiltrate, may represent the key mechanism by which disruption of CD154-CD40 signaling prevents sensitization to alloantigen in vivo and leads to long-term allograft survival.

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In the absence of a CD40 signal, B cells are tolerogenic

Cited by 141 publications

References 29 publications

The role of CD40/CD154 interactions in the priming, differentiation, and effector function of helper and cytotoxic T cells

The role of CD40/CD154 interactions in the priming, differentiation, and effector function of helper and cytotoxic T cells

Ocular Immune Privilege Promoted by the Presentation of Peptide on Tolerogenic B Cells in the Spleen. II. Evidence for Presentation by Qa-1

The CD154-CD40 T Cell Costimulation Pathway Is Required for Host Sensitization of CD8+ T Cells by Skin Grafts Via Direct Antigen Presentation

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