CD39 Is Critical for Inducing Tolerance in Murine Allogeneic Liver Transplantation.

Abstract

Background: ATP is abundant in the cell cytosol and important for cell metabolism. Once cells die or are injured, ATP is released into the extracellular space and activates immune cells as a DAMP (damage-associated molecule pattern). CD39 regulates immune activation by hydrolysis of extracellular (e)ATP. We have found that conventional mouse liver myeloid(m) DC express comparatively high levels of surface CD39 and that this contributes to protection of the liver from cold ischemia reperfusion injury after syngeneic liver transplantation (LTx). We hypothesized that CD39 might play an important role in “spontaneous” transplant tolerance after allogeneic mouse LTx. METHODS: 10-12 week-old male B6 WT or CD39 KO (B6 background) livers were transplanted orthotopically into normal 10-12 week-old male C3H mice. Graft rejection was assessed by host survival and histology and also by serum ALT on day 4 after LTx. Incidences of regulatory T cells (Treg) and IFN-γ+ CD8+ T cells in the graft were quantified by flow cytometry at day 4 post LTx. Anti-donor T cell proliferative responses were evaluated by CFSE-MLR. RESULTS: Whereas all the WT B6 liver transplanted C3H mice survived more than 100 days, animals that received CD39KO livers all died within 40 days (MST: WT: >100d vs CD39 KO 8d; p<0.01). Serum ALT at day 4 post LTx was significantly higher in mice given CD39KO livers than in those with WT livers (WT: 480±226 IU/l vs CD39KO 860±484IU/l; p<0.05). The frequency of Treg in liver graft non-parenchymal cells after LTx was significantly lower in CD39KO livers than in WT livers (WT: 3.4±0.5% vs CD39KO 2.6±0.2%; p<0.05). Moreover IFN-γ production by CD8+ liver T cells was significantly higher in CD39KO allografts than in WT allografts (WT: 38.8±1.7% vs CD39KO 46.6±2.0%; p<0.05). Splenic T cells from CD39KO liver transplant recipients exhibited greater proliferation against donor splenocytes than those from WT liver allografted mice (WT: 27.2±5.8% vs CD39KO 36.3±5.7%; p<0.05). CONCLUSION: CD39 deficiency in liver grafts induces stronger anti-donor T cell responses and breaks “spontaneous” tolerance after mouse liver Tx. CD39 may be an important molecule for promoting liver allograft tolerance.