De Novo Donor-Specific HLA Antibody Formation in Two Patients With Crigler-Najjar Syndrome Type I Following Human Hepatocyte Transplantation With Partial Hepatectomy Preconditioning

Jorns, Carl; Nowak, Greg; Németh, Antal; Zemack, Helen; Mörk, L-M; Johansson, H; Gramignoli, Roberto; Watanabe, Masaaki; Karadagi, Ahmad; Alheim, Mats; Hauzenberger, Dan; Dijk, Remco van; Bosma, Piter J.; Ebbesen, Finn; Szakos, Attila; Fischler, Björn; Strom, Stephen C.; Ellis, Ewa; Bg, Ericzon

doi:10.1111/ajt.13487

Cited by 60 publications

(59 citation statements)

References 23 publications

(32 reference statements)

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“…Clinical experience to date with hepatocyte or islet transplant to the liver demonstrate the failure to achieve long-term cellular allograft survival despite the use of conventional immunosuppression. Thus, in contrast to the immunotolerant theory of the liver microenvironment which would predict the need for minimal immunosuppression, the current studies highlight the need to develop more effective immunotherapeutic strategies to target both unique CD8-mediated immune responses primed in the liver and conventional alloimmune rejection pathways 13,17,18,71 .…”

Section: Discussionmentioning

confidence: 95%

Unique CD8+ T Cell–Mediated Immune Responses Primed in the Liver

et al. 2016

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Background The liver immune environment is tightly regulated to balance immune activation with immune tolerance. Understanding the dominant immune pathways initiated in the liver is important since the liver is a site for cell transplantation, such as for islet and hepatocyte transplantation. The purpose of this study is to examine the consequences of alloimmune stimulation when allogeneic cells are transplanted to the liver in comparison to a different immune locale, such as the kidney. Methods We investigated cellular and humoral immune responses when allogeneic hepatocytes are transplanted directly to the recipient liver by intraportal injection. A heterotopic kidney engraftment site was used for comparison to immune activation in the liver microenvironment. Results Transplantation of allogeneic hepatocytes delivered directly to the liver, via recipient portal circulation, stimulated long-term, high magnitude CD8+ T cell-mediated allocytotoxicity. CD8+ T cells initiated significant in vivo allocytotoxicity as well as rapid rejection of hepatocytes transplanted to the liver even in the absence of secondary lymph nodes or CD4+ T cells. In contrast, in the absence of recipient peripheral lymphoid tissue and CD4+ T cells, CD8-mediated in vivo allocytotoxicity was abrogated and rejection was delayed when hepatocellular allografts were transplanted to the kidney subcapsular site. Conclusions These results highlight the CD8-dominant proinflammatory immune responses unique to the liver microenvironment. Allogeneic cells transplanted directly to the liver do not enjoy immune privilege but rather require immunosuppression to prevent rejection by a robust and persistent CD8‐dependent allocytotoxicity primed in the liver.

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Section: Discussionmentioning

confidence: 95%

Unique CD8+ T Cell–Mediated Immune Responses Primed in the Liver

et al. 2016

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“…Given the importance of AMR in causing acute graft dysfunction 11 and the negative correlation of DSA with long-term allograft survival for both cell and organ transplants 7-9,35-38 , it is of great interest to devise optimal maintenance immunosuppression to suppress the emergence of DSA posttransplant. The clinical literature includes publications which report that no current immunosuppressive regimens effectively prevent the development of DSA 10,11 , while others infer relative efficacy of CNi by reporting that conversion of kidney transplant recipients from CNi to mTORi-based therapy is associated with a negative impact on DSA production and graft survival 19,39-41 .…”

Section: Discussionmentioning

confidence: 99%

“…CNi-based immunotherapies are used following clinical cell transplantation including hepatocyte transplantation but have been associated with limited success for sustained hepatocellular allograft survival 9,58-60 While early studies have not sufficiently explored alloantibody responses following clinical hepatocyte transplant, recently Jorns et al reported the development of de novo donor-specific HLA antibody in 2 patients who underwent hepatocyte transplantation. The onset of humoral alloimmunity and graft loss occurred in the context of lowering and eventual discontinuation of immunosuppression in 1 patient and despite the use of maintenance immunosuppression with CNi and low dose steroids in the second case 9 . The current experimental studies which demonstrate the lack of efficacy of CNi for suppression of alloantibody production provide insight into clinical studies which demonstrate detection of DSA in CNi-treated recipients.…”

Section: Discussionmentioning

confidence: 99%

“…De novo DSA are particularly detrimental to cellular transplants, which have relatively smaller parenchymal cell mass and increased exposure to circulating antibodies 5 . Development of humoral alloimmunity after islet 6-8 and hepatocyte transplant 9 is associated with deterioration of graft function and is a barrier to long-term graft survival. Current therapies available for treatment of AMR include removal of deleterious alloantibodies, targeting IgG + cells, cellular depletion, or a combination of these strategies 10,11 .…”

Section: Introductionmentioning

confidence: 99%

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mTOR Inhibition Suppresses Posttransplant Alloantibody Production Through Direct Inhibition of Alloprimed B Cells and Sparing of CD8+ Antibody-Suppressing T cells

et al. 2016

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Background De novo alloantibodies (DSA) contribute to antibody-mediated rejection and poor long-term graft survival. Since the development of DSA is associated with early graft loss of cell transplants and reduced long-term survival of solid organ transplants, we hypothesized that conventional immunosuppressives, calcineurin inhibitors (CNi) and mammalian target of rapamycin inhibitors (mTORi), may not be as effective for suppression of humoral alloimmunity as for cell-mediated immunity. Methods Wild-type or CD8-depleted mice were transplanted with allogeneic hepatocytes. Recipients were treated with mTORi and/or CNi and serially monitored for alloantibody and graft survival. The direct effect of mTORi and CNi on alloprimed B cell function was investigated in Rag1-/- mice adoptively transferred with alloprimed IgG1+ B cells. The efficacy of mTORi and/or CNi to suppress CD8-mediated cytotoxicity of IgG1+ B cells was evaluated in in vitro and in vivo cytotoxicity assays. Results mTORi, but not CNi, reduced alloantibody production in transplant recipients, directly suppressed alloantibody production by alloprimed IgG1+ B cells and delayed graft rejection in both low and high alloantibody-producers. Combination treatment with mTORi and CNi resulted in loss of the inhibitory effect observed for mTORi monotherapy in part due to CNi-suppression of CD8+ T cells which downregulate alloantibody production (CD8+ TAb-supp cells). Conclusions Our data supports that mTORi is a potent inhibitor of humoral immunity through suppression of alloprimed B cells and preservation of CD8+ TAb-supp cells. In contrast, alloantibody is readily detected in CNi-treated recipients because CNi does not suppress alloprimed B cells and interferes with downregulatory CD8+ TAb-supp cells.

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“…The development and contribution of donor-specific antibodies (DSA) in HT is still very much unknown. The presence of de novo DSA following HT has been temporarily associated with graft loss (9, 25) and in one reported case was associated with the peak measurement of the immune reactivity index score that has been shown to enable the prediction rejection (25). Ultimately, a more robust understanding of the immunological responses induced by HT is needed to help guide therapeutic regimens that will enable extended cell graft survival and broader application of HT to patients who will benefit from this promising therapy.…”

Section: Improving Transplanted Hepatocyte Survival and Monitoringmentioning

confidence: 96%

Clinical Hepatocyte Transplantation: What Is Next?

et al. 2017

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Purpose of review Significant recent scientific developments have occurred in the field of liver repopulation and regeneration. While techniques to facilitate liver repopulation with donor hepatocytes and different cell sources have been studied extensively in the laboratory, in recent years clinical hepatocyte transplantation (HT) and liver repopulation trials have demonstrated new disease indications and also immunological challenges that will require the incorporation of a fresh look and new experimental approaches. Recent findings Growth advantage and regenerative stimulus are necessary to allow donor hepatocytes to proliferate. Current research efforts focus on mechanisms of donor hepatocyte expansion in response to liver injury/preconditioning. Moreover, latest clinical evidence shows that important obstacles to HT include optimizing engraftment and limited duration of effectiveness, with hepatocytes being lost to immunological rejection. We will discuss alternatives for cellular rejection monitoring, as well as new modalities to follow cellular graft function and near-to-clinical cell sources. Summary HT partially corrects genetic disorders for a limited period of time and has been associated with reversal of ALF. The main identified obstacles that remain to make HT a curative approach include improving engraftment rates, and methods for monitoring cellular graft function and rejection. This review aims to discuss current state-of-the-art in clinical HT and provide insights into innovative approaches taken to overcome these obstacles.

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De Novo Donor-Specific HLA Antibody Formation in Two Patients With Crigler-Najjar Syndrome Type I Following Human Hepatocyte Transplantation With Partial Hepatectomy Preconditioning

Cited by 60 publications

References 23 publications

Unique CD8+ T Cell–Mediated Immune Responses Primed in the Liver

Unique CD8+ T Cell–Mediated Immune Responses Primed in the Liver

mTOR Inhibition Suppresses Posttransplant Alloantibody Production Through Direct Inhibition of Alloprimed B Cells and Sparing of CD8+ Antibody-Suppressing T cells

Clinical Hepatocyte Transplantation: What Is Next?

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