Mechanisms of Gene Therapy for Tolerance: B7 Signaling Is Required for Peptide-IgG Gene-Transferred Tolerance Induction

Litzinger, Mary; Su, Yan; Lei, Tiechi; Soukhareva, Nadejda; Scott, David W.

doi:10.4049/jimmunol.175.2.780

Cited by 36 publications

(38 citation statements)

References 30 publications

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“…In addition, MZ B cells also express higher levels of B7.1 and B7.2 than FO B cells do, thus facilitating effective antigen presentation to CTLA-4 ϩ regulatory T cells. 23,24 Through fluorescence-activated cell sorter analysis, we found that the B7 costimulatory molecules were further up-regulated on IgG1 anti-CD20 treatment plus high-dose FVIII exposure. In contrast, control IgG plus FVIII treatment had no significant effect on this phenotype of MZ B cells, compared with nontreated naive mice (Figure 3).…”

Section: Resultsmentioning

confidence: 99%

Effect of B-cell depletion using anti-CD20 therapy on inhibitory antibody formation to human FVIII in hemophilia A mice

Zhang

Skupsky

Scott

2011

Blood

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We herein tested the effect of B-cell depletion on tolerance induction to factor VIII (FVIII) in a mouse model of hemophilia A. Two subclasses of anti–mouse CD20 monoclonal antibodies with differential depletion effects were used. Thus, IgG1 anti-CD20 selectively depleted follicular B cells and spared marginal zone B cells, whereas IgG2a anti-CD20 efficiently depleted both. In FVIII primed mice, a single dose of either IgG1 or IgG2a anti-CD20 pretreatment prevented the increase in inhibitor formation in the majority of treated mice by subsequent daily, high-dose FVIII intravenous injection as a model for immune tolerance induction. However, the IgG1, but not the IgG2a, anti-CD20 pretreatment led to a significant increase of regulatory T cells in the spleen. Importantly, 3 months after the partial B-cell depletion with IgG1 anti-CD20, the FVIII-specific hyporesponsive state remained. We suggest a tolerogenic role of the remaining marginal zone B cells as a potential mechanism for anti-CD20 therapy.

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Section: Resultsmentioning

confidence: 99%

Effect of B-cell depletion using anti-CD20 therapy on inhibitory antibody formation to human FVIII in hemophilia A mice

Zhang

Skupsky

Scott

2011

Blood

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“…On the other hand, we have performed experiments in which the B cells of B MOG mice were activated in vivo using LPS or anti-CD40, but naive T cells transferred to these mice were not sufficiently stimulated to proliferate. It has previously been shown that activated transferred B cells need to express B7 molecules to induce tolerance (10). It is possible that, in our system, tolerance can also be achieved by costimulatory molecules other than B7.…”

Section: Discussionmentioning

confidence: 99%

“…On the other hand, memory T cells may not need costimulation and could therefore be activated by B cells. A problem of this hypothesis is that also activated B cells, which normally do express B7 molecules, can induce tolerance of T cells (10). It is therefore not clear whether it is indeed the absence of costimulation what causes B cells to induce tolerance.…”

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confidence: 98%

Tolerance without Clonal Expansion: Self-Antigen-Expressing B Cells Program Self-Reactive T Cells for Future Deletion

Frommer

Heinen

Wunderlich

et al. 2008

The Journal of Immunology

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2), it was presumed that anti-IgD Abs targeted resting B cells, and due to a lack of costimulatory molecules, these B cells tolerized MBP-specific T cells. Similarly, it was shown that passive transfer of B cells expressing a myelin peptide prevented the induction of EAE (6 -8) or even EAE relapses (9). One explanation why B cells induce tolerance of naive but not memory T cells might be the need for expression of costimulatory molecules by the APC to activate naive T cells, specifically B7-1 and/or B7-2, but resting B cells do not express these molecules. On the other hand, memory T cells may not need costimulation and could therefore be activated by B cells. A problem of this hypothesis is that also activated B cells, which normally do express B7 molecules, can induce tolerance of T cells (10). It is therefore not clear whether it is indeed the absence of costimulation what causes B cells to induce tolerance.To study the role of B cells in tolerance induction we have generated mice that express an MHC class II-restricted immunodominant T cell epitope of myelin oligodendrocyte glycoprotein (MOG) specifically on B cells. These mice were found to be resistant to EAE induction. We could show that, following interaction of naive T cells with B cells presenting their specific Ag, T cells are partially activated, resulting in very marginal proliferation and up-regulation of coinhibitory molecules such as CTLA-4, B and T lymphocyte attenuator (BTLA), PD-1, and CD5. Subsequent in vivo activation of tolerized T cells leads to their deletion. Thus, we assessed that naive B cells induce peripheral tolerance by inducing expression of negative costimulatory molecules by Ag-specific T cells, followed by Ag-induced cell death (AICD) upon the next Ag encounter. Materials and Methods Generation of invariant chain (Ii) MOG miceThe targeting vector ROSA26STOP*IiMOG was constructed by introduction into the XbaI site of the vector ROSA26 -1 (11); a gift from P. Soriano (Fred Hutchinson Cancer Research Center, Seattle, WA) of a fragment comprising (5Ј to 3Ј): adenoviral splice acceptor, loxP, 2ϫ SV40 polyadenylation signal, FRT-flanked pGK-neo, a STOP cassette (12), loxP, mutant invariant chain (termed IiMOG), and bovine poly(A). The mutant invariant chain (IiMOG) was generated by assembly PCR on Ii template cDNA (derived from plasmid pcEX V3 mIi31, carrying the cDNA of the

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“…Though the number of B cells used to induce tolerance was relatively high, it is unlikely that this contributed to an specific effect, because control mice injected with an equal number of nontransduced or GFP-transduced B cells showed no induction of an immune response. Moreover, in earlier studies performed by others (27,28), a comparable number of B cells (15-20 ϫ 10 6 ) were transferred to confer Ag-specific immune response.…”

Section: Discussionmentioning

confidence: 99%

In Vivo Induction of Type 1-Like Regulatory T Cells Using Genetically Modified B Cells Confers Long-Term IL-10-Dependent Antigen-Specific Unresponsiveness

Ahangarani

Janssens

VanderElst

et al. 2009

The Journal of Immunology

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Mechanisms of Gene Therapy for Tolerance: B7 Signaling Is Required for Peptide-IgG Gene-Transferred Tolerance Induction

Cited by 36 publications

References 30 publications

Effect of B-cell depletion using anti-CD20 therapy on inhibitory antibody formation to human FVIII in hemophilia A mice

Effect of B-cell depletion using anti-CD20 therapy on inhibitory antibody formation to human FVIII in hemophilia A mice

Tolerance without Clonal Expansion: Self-Antigen-Expressing B Cells Program Self-Reactive T Cells for Future Deletion

In Vivo Induction of Type 1-Like Regulatory T Cells Using Genetically Modified B Cells Confers Long-Term IL-10-Dependent Antigen-Specific Unresponsiveness

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