Intact Active Bone Transplantation Synergizes with Anti-CD40 Ligand Therapy to Induce B Cell Tolerance

Yin, Dengping; Ma, Lianli; Varghese, Anncy; Shen, Jikun; Chong, Anita S.

doi:10.4049/jimmunol.168.10.5352

Cited by 18 publications

(17 citation statements)

References 43 publications

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“…The free bone grafts were prepared by a method modified from the previous description by Yin et al (36). Briefly, the knee joints containing the heads of tibiae and femora from the hind legs of C3H donor mice or third party C56BL/6 mice were harvested, cleaned of connective tissue, and cut into small fragments.…”

Section: Free Bone Cotransplantation and Csa Treatmentmentioning

confidence: 99%

“…To apply this concept to a noncomposite allograft system, previous studies have used "intact active bone" fragments to provide HSCs/MSCs population in its naturally residing environment. It was demonstrated that implantation of such bone grafts under the kidney capsule of recipient mice could synergize with the anti-CD154 Ab to prolong donor organ survival (35,36). To enable a higher number of active cells to be implanted, as well as to develop a clinically relevant procedure, we adopted a technique to implant free bone into the s.c. fat of the recipient animal, the procedure referred to as "free bone cotransplantation".…”

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confidence: 99%

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Free Bone Graft Attenuates Acute Rejection and in Combination with Cyclosporin A Leads to Indefinite Cardiac Allograft Survival

Wang

Ge²,

Arp³

et al. 2009

The Journal of Immunology

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We report on a novel approach aimed at preventing acute vascular rejection (AVR), one of the major unresolved hurdles of clinical transplantation. In a C3H-to-BALB/c heterotopic heart transplant model, we demonstrate that free bone transplantation combined with cyclosporin A suppresses antidonor Ab responses, induces indefinite cardiac allograft survival (>100 days), and preserves graft architecture. In contrast, untreated- or cyclosporin A alone-treated recipients rejected their cardiac grafts on days 7.7 ± 0.6 and 15.5 ± 1.1, respectively, with graft histology indicative of AVR. Splenic dendritic cells from nonrejecting recipients expressed low levels of MHC II, CD40, and CD86, reduced ability to stimulate donor cell proliferation, and augmented IL-10 production of responding T cells in vitro. Adoptive transfer of dendritic cells from long-term surviving recipients 1 day before cardiac grafting was able to confer hyporesponsiveness to naive BALB/c recipients of cardiac allografts. To determine whether graft survival was associated with hematopoietic or stromal elements of the transplanted free bone, we administered isolated bone marrow mononuclear cells or free bone that was irradiated to deplete hematopoietic elements. Although bone marrow mononuclear cells had no effect on cardiac graft survival, irradiated free bone transplantation was capable of prolonging graft survival. Most interestingly, the prolongation effect was Ag nonspecific, because third party irradiated bone graft was also effective. Due to the fact that current immunosuppressive approaches are clinically ineffective at preventing AVR, this study provides promise for further investigations of BM components as a means of addressing a currently unmet medical need.

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Section: Free Bone Cotransplantation and Csa Treatmentmentioning

confidence: 99%

mentioning

confidence: 99%

Free Bone Graft Attenuates Acute Rejection and in Combination with Cyclosporin A Leads to Indefinite Cardiac Allograft Survival

Wang

Ge²,

Arp³

et al. 2009

The Journal of Immunology

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“…Blocking CD154-CD40 interaction also prevents the T-dependent humoral responses (18). As a result, alloantibody production is inhibited (19), which can also be important for the long-term survival of allografts. However, the detailed mechanism of how alloreactive B cells are regulated by such costimulation-targeted therapies is not clear.…”

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confidence: 99%

Peripheral deletion of mature alloreactive B cells induced by costimulation blockade

Shen

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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(4). In animal models, the major evidence comes from studies using the MT mice. These mice have a targeted mutation at the transmembrane domain of B cell receptor -chain and have defects in B cells and antibody secretion (5), as well as a reduction in T cell and dendritic cell numbers (6). In a mouse cardiac transplant model in which B10.A (H-2 a ) hearts are transplanted into H-2 b MT mouse, acute rejection is prevented. Passive transfer of complement-activating alloantibodies restores acute rejection, suggesting that antibodies can facilitate the development of acute allograft rejection (7).Anti-CD154 (CD40 ligand) treatment has been shown to be an effective way of preventing transplant rejection in animal models (8-11). It has been proposed that such treatment impairs the maturation of host antigen-presenting cells, generates tolerogenic dendritic cells, promotes T cell anergy (12) and deletion (13), and induces regulatory T cells (14, 15). Graft survival can be further enhanced by donor-specific transfusion (DST) (16), and in the presence of anti-CD154, the infused DST is presented by host antigen-presenting cells in a tolerogenic manner, resulting in T cell anergy and regulation (17). Blocking CD154-CD40 interaction also prevents the T-dependent humoral responses (18). As a result, alloantibody production is inhibited (19), which can also be important for the long-term survival of allografts. However, the detailed mechanism of how alloreactive B cells are regulated by such costimulation-targeted therapies is not clear.To characterize the fate of alloreactive B cells after tolerance induction by anti-CD154-based therapy, we took advantage of a B cell receptor transgenic mouse, . This mouse inherits the transgenes that encode the heavy and light chain of a B cell receptor that recognizes the mouse class I MHC molecule H-2K b . B cells expressing the transgene can develop normally on the BALB/c background but are efficiently regulated by receptor editing on the C57BL/6 background (21). When the K b antigen is only expressed by the liver hepatocytes, the 3-83 B cells are deleted in the periphery (22). We used 3-83Igi mice on the BALB/c background as recipients of transplanted C57BL/6 hearts. We then induced tolerance with anti-CD154 and DST. The alloreactive 3-83 B cells are easily detected by an anti-idiotype (Id) antibody (23), allowing us to visualize changes in these B cells after tolerance induction. The results of our study showed that alloreactive B cells were specifically deleted in the periphery at the mature stage.

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“…Early studies indicated that anti-CD154 treatment could suppress B cell responses, but not induce B cell tolerance (36). In contrast, we have reported that anti-CD154 therapy, in the context of allograft tolerance models, can induce the long-term suppression of alloantibody and anti-Galactose-␣(1-3) Galactose carbohydrate moiety Ab production (37). To address the different effects of anti-CD154 on B cell responses, we have examined the basis for how alloreactive B cell responses are controlled in a mouse heart allograft transplant model.…”

Section: Discussionmentioning

confidence: 89%

Long-Term Control of Alloreactive B Cell Responses by the Suppression of T Cell Help

Yin

et al. 2008

The Journal of Immunology

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Alloantibodies can play a key role in acute and chronic allograft rejection. However, relatively little is known of factors that control B cell responses following allograft tolerance induction. Using 3-83 Igi mice expressing an alloreactive BCR, we recently reported that allograft tolerance was associated with the sustained deletion of the alloreactive B cells at the mature, but not the immature, stage. We have now investigated the basis for the long-term control of alloreactive B cell responses in a non-BCR-transgenic model of C57BL/6 cardiac transplantation into BALB/c recipients treated with anti-CD154 and transfusion of donor-specific spleen cells. We demonstrate that the long-term production of alloreactive Abs by alloreactive B cells is actively regulated in tolerant BALB/c mice through the dominant suppression of T cell help. Deletion of CD25+ cells resulted in a loss of tolerance and an acquisition of the ability to acutely reject allografts. In contrast, the restoration of alloantibody responses required both the deletion of CD25+ cells and the reconstitution of alloreactive B cells. Collectively, these data suggest that alloreactive B cell responses in this model of tolerance are controlled by dominant suppression of T cell help as well as the deletion of alloreactive B cells in the periphery.

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Intact Active Bone Transplantation Synergizes with Anti-CD40 Ligand Therapy to Induce B Cell Tolerance

Cited by 18 publications

References 43 publications

Free Bone Graft Attenuates Acute Rejection and in Combination with Cyclosporin A Leads to Indefinite Cardiac Allograft Survival

Free Bone Graft Attenuates Acute Rejection and in Combination with Cyclosporin A Leads to Indefinite Cardiac Allograft Survival

Peripheral deletion of mature alloreactive B cells induced by costimulation blockade

Long-Term Control of Alloreactive B Cell Responses by the Suppression of T Cell Help

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