Mechanisms of Alloimmunization and Subsequent Bone Marrow Transplantation Rejection Induced by Platelet Transfusion in a Murine Model

Patel, Seema R.; Smith, Nicole H.; Kapp, Linda M.; Zimring, James C.

doi:10.1111/j.1600-6143.2011.03959.x

Cited by 13 publications

(21 citation statements)

References 28 publications

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“…Our studies build upon previous work by others demonstrating that costimulatory signal deliver by helper T cells, predominantly transmitted via the indirect pathway of allorecognition, are required for induction of high titer, isotype switched, IgG, alloantibody reactive to donor antigens (7,8,10,(30)(31)(32)(33)(34)(35)(36). Using an allosensitization model in which the prior administration of a single fully MHC disparate splenocyte dose provides sufficient high-titer alloantibody to reject allogeneic BM grafts even 1 year postpriming, we newly demonstrate that only a combination of a highly depletionary anti-CD20 mAb plus LTbR-Ig that reduces GC formation sufficiently eliminates alloantibody to permit donor BM rescue of lethally irradiated, T-and NK-depleted recipients ( Figure 5D).…”

Section: Discussionsupporting

confidence: 67%

“…We and others have shown in preclinical murine models that allosensitization presents a formidable barrier to bone marrow (BM) engraftment (6)(7)(8)(9)(10)(11). Preformed alloreactive antibody, rather than primed donor reactive T cells, prevents engraftment of allogeneic full MHCdisparate BM in presensitized recipients: a single intravenous infusion of allogeneic splenocytes to mimic a blood transfusion resulted in high, sustained serum antibody titers sufficient to cause the elimination of a moderate dose of allogeneic BM in irradiated recipients by 3 h post-BMT (6).…”

Section: Introductionmentioning

confidence: 99%

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Strategies to Inhibit Alloantibody Production in Alloprimed Murine Recipients of Hematopoietic Stem Cell Grafts

Blazar¹,

Flynn²,

Lee

et al. 2015

American Journal of Transplantation

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Alloantibody, not primed T cells, is the major barrier to bone marrow (BM) engraftment in allosensitized mice. We have shown that a single intravenous injection of donor splenocytes, to mimic a blood transfusion, results in high, sustained levels of serum alloantibody sufficient to eliminate donor BM within 3 h, resulting in uniform mortality in lethally irradiated allogeneic recipients. Current studies focused preventing and treating allopriming. Blockade of B cell survival signals with mTACI-Ig pre-and postpriming was ineffective, as was the B cell but not plasma cell depleting anti-CD20 mAb. Germinal center formation inhibition by lymphotoxin-beta receptor-Ig (LbR-Ig) diminished allosensitization, although conditional Prmd1 (Blimp-1) deletion in CD19þ cells was highly effective. By combining anti-CD20 mAb to reduce B cells and LTbR-Ig to diminish the frequency of B cells that could form germinal centers pre-and postpriming, allosensitization was precluded, permitting long-term survival in T-and NK-depleted, irradiated allogeneic recipients, whereas combined therapy postpriming alone was ineffective. As evidence of the critical role of B cells, the proteosomal inhibitor, bortezomib, given unencapsulated or encapsulated, proved ineffective in influencing allosensitization. These data extend our understanding of allopriming and provide a potential therapy for patients at risk for allosensitization and BM graft rejection.Abbreviations: APRIL, a proliferation-inducing ligand; BLIMP-1, B-lymphocyte induced maturation protein-1; BLyS, B-lymphocyte stimulator; BM, bone marrow; BMT, bone marrow transplantation; BTZ, bortezomib; Fl, flox; Ig, immunoglobulin; LTbR-Ig, lymphotoxinbeta receptor-immunoglobulin; MFI, mean fluorescent intensity; (m)TACI, (mouse) transmembrane activator and calcium-modulator and cyclophilin ligand receptor interactor; PB, peripheral blood; PBL, peripheral blood lymphocyte; PC, plasma cell; Prmd1, PR domain containing 1, with ZNF domain; Tfh, T follicular helper cell

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Section: Discussionsupporting

confidence: 67%

Section: Introductionmentioning

confidence: 99%

Strategies to Inhibit Alloantibody Production in Alloprimed Murine Recipients of Hematopoietic Stem Cell Grafts

Blazar¹,

Flynn²,

Lee

et al. 2015

American Journal of Transplantation

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“…Rejection can be defined as graft damage arising from response to the transplanted organ by the recipient immune system and may take several forms resulting in different clinical patterns (12)(13)(14). The two major presentations after liver transplantation are acute and chronic rejection, with hyperacute rejection rarely encountered (15,16).…”

Section: Mechanisms Of Rejectionmentioning

confidence: 99%

“…Medawar was the first to assert that rejection was an immunological response, with the inflammatory reaction due to lymphocyte infiltration (1,9). Graft rejection may be governed in part by the type and extent of histocompatibility differences between donor and recipient with humoral mechanisms of likely greater importance in the rejection of renal than liver grafts (1,12,19). The two principal events of the human immune response are the recognition of epitopes on peptide antigens by T-cell receptors (TCR) and recognition of different epitopes on processed antigens by B-cell receptors.…”

Section: Mechanisms Of Rejectionmentioning

confidence: 99%

Nephro and neurotoxicity of calcineurin inhibitors and mechanisms of rejections: A review on tacrolimus and cyclosporin in organ transplantation

Tolou-Ghamari¹

2012

jnp

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Implication for health policy/practice/research/medical education:Previous studies from the 12-th century B.C. up to modern times have focused on quality and quantity of life in transplant recipients. This review focuses on the history of transplant and immunosuppressive drug therapy.Please cite this paper as: Tolou-Ghamari Z. Nephro and neurotoxicity, mechanisms of rejection: A review on Tacrolimus and Cyclosporin in organ transplantation.

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“…Depletion of recipient CD4 + T cells after transfusions but prior to transplantation has been reported to prevent transfusion induced BMT rejection across mHA barriers [57]. On the contrary, CD4 + T cell depletion after rejection of an initial BMT but prior to rejection of a re-transplantation had no effect upon rejection of the second BMT [57].…”

Section: Introductionmentioning

confidence: 99%

Transfusion-Induced Bone Marrow Transplant Rejection Due to Minor Histocompatibility Antigens

Patel

Zimring

2013

Transfusion Medicine Reviews

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Traditionally, alloimmunization to transfused blood products has focused exclusively upon recipient antibodies recognizing donor alloantigens present on the cell surface. Accordingly, the immunological sequelae of alloimmunization have been antibody mediated effects (i.e. hemolytic transfusion reactions, platelet refractoriness, anti-HLA and anti-HNA effects, etc.). However, in addition to the above sequelae, there is also a correlation between the number of antecedent transfusions in humans and the rate of bone marrow transplant (BMT) rejection - under reduced intensity conditioning with HLA matched or HLA identical marrow. BMT of this nature is the only existing cure for a series of non-malignant hematological diseases (e.g. sickle cell disease, thalassemias, etc.); however, rejection remains a clinical problem. It has been hypothesized that transfusion induces subsequent BMT rejection through immunization. Studies in animal models have observed the same effect and have demonstrated that transfusion induced BMT rejection can occur in response to alloimmunization. However, unlike traditional antibody responses, sensitization in this case results in cellular immune effects, involving populations such as T cell or NK cells. In this case, rejection occurs in the absence of alloantibodies, and would not be detected by existing immune-hematological methods. We review human and animal studies in light of the hypothesis that, for distinct clinical populations, enhanced rejection of BMT may be an unappreciated adverse consequence of transfusion which current blood bank methodologies are unable to detect.

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Mechanisms of Alloimmunization and Subsequent Bone Marrow Transplantation Rejection Induced by Platelet Transfusion in a Murine Model

Cited by 13 publications

References 28 publications

Strategies to Inhibit Alloantibody Production in Alloprimed Murine Recipients of Hematopoietic Stem Cell Grafts

Strategies to Inhibit Alloantibody Production in Alloprimed Murine Recipients of Hematopoietic Stem Cell Grafts

Nephro and neurotoxicity of calcineurin inhibitors and mechanisms of rejections: A review on tacrolimus and cyclosporin in organ transplantation

Transfusion-Induced Bone Marrow Transplant Rejection Due to Minor Histocompatibility Antigens

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