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Publication : IL-10 regulates movement of intestinally derived CD4+ T cells to the liver.

First Author  Bliss SK Year  2007
Journal  J Immunol Volume  178
Issue  12 Pages  7974-83
PubMed ID  17548634 Mgi Jnum  J:148582
Mgi Id  MGI:3845730 Doi  10.4049/jimmunol.178.12.7974
Citation  Bliss SK, et al. (2007) IL-10 regulates movement of intestinally derived CD4+ T cells to the liver. J Immunol 178(12):7974-83
abstractText  Diseases that affect the intestine may have hepatic manifestations, but the mechanisms involved in establishing hepatic disease secondarily remain poorly understood. We previously reported that IL-10 knockout (KO) mice developed severe necrotizing hepatitis following oral infection with Trichinella spiralis. In this study, we used this model of intestinal inflammation to further examine the role of IL-10 in regulating hepatic injury. Hepatic damage was induced by migrating newborn larvae. By delivering the parasite directly into the portal vein, we demonstrated that an ongoing intestinal immune response was necessary for the development of hepatitis. Intestinally derived CD4+ cells increased in the livers of IL-10 KO mice, and Ab-mediated blockade of MAdCAM-1 inhibited the accumulation of CD4+alpha(4)beta(7)+ cells in the liver. Moreover, adoptive transfer of intestinally primed CD4+ T cells from IL-10 KO mice caused hepatitis in infected immunodeficient animals. Conversely, transfer of wild-type donor cells reduced the severity of hepatic inflammation in IL-10 KO recipients, demonstrating regulatory activity. Our results revealed that IL-10 prevented migration of intestinal T cells to the liver and inhibited the development of hepatitis.
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