IFN‐γ is an Absolute Requirement for Spontaneous Acceptance of Liver Allografts

Abstract

Experimental liver allografts undergo spontaneous acceptance despite undergoing rejection during the first few weeks post transplant. We explored the role of interferon‐γ (IFN‐γ) in the spontaneous acceptance of mouse liver allografts. Strain of mouse (CBA) liver allografts transplanted into normal BALB/c mice developed histologic changes typical of rejection that spontaneously regressed, permitting long‐term survival of these allografts similar to that of syngeneic grafts. In contrast, CBA liver allografts in IFN‐γ‐deficient hosts manifested not only infiltration but also hemorrhage and necrosis, with no survival beyond 14 days. Despite differences in survival, local expression of cytotoxic T‐cell genes in the transplant was not increased in IFN‐γ‐deficient hosts, but livers in interferon‐γ‐deficient mice (GKO) hosts displayed much less induction of major histocompatibility complex (MHC) class I and II expression. To determine whether the difference in survival was secondary to the direct effects of IFN‐γ on the liver, we transplanted livers from IFN‐γ‐receptor‐deficient mice into normal hosts. Liver allografts lacking IFN‐γ receptors also developed hemorrhage and necrosis with minimal induction of MHC expression. Thus IFN‐γ mediates a direct effect on rejecting liver allografts that reduces hemorrhage and necrosis, induces MHC expression, and is absolutely required for spontaneous acceptance.