Immunobiology of liver xenotransplantation

Ekser, Burçin; Burlak, Christopher; Waldman, Joshua; Lutz, Andrew J.; Paris, Leela L.; Veroux, Massimiliano; Robson, Simon C.; Rees, Michael; Ayares, David; Gridelli, Bruno; Tector, A. Joseph; Cooper, David K. C.

doi:10.1586/eci.12.56

Cited by 20 publications

(32 citation statements)

References 97 publications

(158 reference statements)

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“…More difficult is the situation with pig liver transplantation [55]. In pig to non-human primate studies, the transplantation of livers from pigs transgenic for hCD55 or from GTKO animals, which in addition expressed hCD46, was associated with a survival time of 7 to 9 days [55][56][57] including coagulation, have proved to be satisfactory, the immediate development of thrombocytopenia was extremely limiting.…”

Section: Physiological Compatibilitymentioning

confidence: 99%

“…In pig to non-human primate studies, the transplantation of livers from pigs transgenic for hCD55 or from GTKO animals, which in addition expressed hCD46, was associated with a survival time of 7 to 9 days [55][56][57] including coagulation, have proved to be satisfactory, the immediate development of thrombocytopenia was extremely limiting. The thrombocytopenia resulted in hemorrhages in various organs and tissues, as well as in the transplanted liver [56].…”

Section: Physiological Compatibilitymentioning

confidence: 99%

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Recent Progress in Xenotransplantation, with Emphasis on Virological Safety

Denner

2016

Ann Transplant

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Section: Physiological Compatibilitymentioning

confidence: 99%

Section: Physiological Compatibilitymentioning

confidence: 99%

Recent Progress in Xenotransplantation, with Emphasis on Virological Safety

Denner

2016

Ann Transplant

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“…However, for the purposes of this review, subsequent attention will be concentrated on the adaptive response and, particularly, on what biologic and pharmacologic agents are likely to play an important role in its control. Pig liver (81) and lung (82) transplantation into NHPs result in rapid graft loss through complex mechanisms that are unrelated to the adaptive response, and in pig islet transplantation the problem of the instant blood-mediated inflammatory reaction has to be overcome (3). These topics deserve in depth consideration in another context, but in this review attention will be directed to immunosuppressive regimens that have been utilized in pig heart and kidney xenotransplantation models.…”

Section: Specific Suppression Of the Adaptive Immune Responsementioning

confidence: 99%

New Concepts of Immune Modulation in Xenotransplantation

et al. 2013

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The shortage of human organs for transplantation has focused research on the possibility of transplanting pig organs into humans. Many factors contribute to the failure of a pig organ graft in a primate. A rapid innate immune response (natural anti-pig antibody, complement activation, and an innate cellular response, e.g., neutrophils, monocytes, macrophages, NK cells) is followed by an adaptive immune response, although T cell infiltration of the graft has rarely been reported. Other factors (e.g., coagulation dysregulation, inflammation) appear to play a significantly greater role than in allotransplantation. The immune responses to a pig xenograft cannot therefore be controlled simply by suppression of T cell activity. Before xenotransplantation can be introduced successfully into the clinic, the problems of the innate, coagulopathic, and inflammatory responses will have to be overcome, most likely by the transplantation of organs from genetically-engineered pigs. Many of the genetic manipulations aimed at protecting against these responses also reduce the adaptive response. The T cell and elicited antibody responses can be prevented by the biologic and/or pharmacologic agents currently available, in particular, by costimulation blockade-based regimens. The exogenous immunosuppressive regimen may be significantly reduced by the presence of a graft from a pig transgenic for a mutant (human) class II transactivator gene, resulting in downregulation of SLA class II expression, or from a pig with ‘local’ vascular endothelial cell expression of an immunosuppressive gene, e.g., CTLA4-Ig. The immunomodulatory efficacy of regulatory T cells or mesenchymal stromal cells has been demonstrated in vitro, but not yet in vivo.

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“…At necropsy some days later, some livers showed macroscopic changes consistent with cholestasis, except for some patchy dark areas which microscopically showed hemorrhagic necrosis, platelet-fibrin thrombi, monocyte/macrophage margination, and vascular endothelial cell hypertrophy (Figure 2C). 12,28,36–38 No cell infiltration was seen. Confocal microscopy has confirmed tissue factor expression on platelets, and platelet and platelet/leukocyte aggregates in liver sinusoids.…”

Section: Introductionmentioning

confidence: 96%

Pig Liver Xenotransplantation

et al. 2016

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Experience with clinical liver xenotransplantation has largely involved the transplantation of livers from nonhuman primates. Experience with pig livers has been scarce. This brief review will be restricted to assessing the potential therapeutic impact of pig liver xenotransplantation in acute liver failure and the remaining barriers that currently do not justify clinical trials. A relatively new surgical technique of heterotopic pig liver xenotransplantation is described that might play a role in bridging a patient with acute liver failure until either the native liver recovers or a suitable liver allograft is obtained. Other topics discussed include the possible mechanisms for the development of the thrombocytopenis that rapidly occurs after pig liver xenotransplantation in a primate, the impact of pig complement on graft injury, the potential infectious risks, and potential physiologic incompatibilities between pig and human. There is cautious optimism that all of these problems can be overcome by judicious genetic manipulation of the pig. If liver graft survival could be achieved in the absence of thrombocytopenia or rejection for a period of even a few days, there may be a role for pig liver transplantation as a bridge to allotransplantation in carefully selected patients.

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Immunobiology of liver xenotransplantation

Cited by 20 publications

References 97 publications

Recent Progress in Xenotransplantation, with Emphasis on Virological Safety

Recent Progress in Xenotransplantation, with Emphasis on Virological Safety

New Concepts of Immune Modulation in Xenotransplantation

Pig Liver Xenotransplantation

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