| Literature DB >> 24551271 |
Xiaoming Shi1, Mingjian Zhang2, Fang Liu1, Zhengxing Wang1, Luding Zhang1, Haifei Cheng3, Shu Zhang4, Teng Fei1, Meng Guo1, Jun Bian3, Quanxing Wang2, Guoshan Ding1.
Abstract
Previously, we demonstrated that Tim-1-Fc prevents acute cardiac graft rejection by inhibiting Th1 response. In the present report, we tackled the impact of Tim-1-Fc on Th17 cells in a model of cardiac chronic rejection. Administration of Tim-1-Fc did not result in a detectable impact on innate immunity and regulatory T cells, while it provided protection for Bm12-derive cardiac grafts against chronic rejection in B6 recipients, as manifested by the reduction of inflammatory infiltration along with less severity of vasculopathy. Studies in T-bet(-/-) recipients by implanting Bm12-derived cardiac grafts further revealed that Tim-1-Fc significantly protected cardiac grafts from chronic rejection along with attenuated production of IL-17 producing T cells. Depletion of CD4 and CD8 T cells or blockade of IL-17 in T-bet(-/-) recipients demonstrated that Tim-1-Fc selectively suppresses Th17 differentiation along with attenuated IL-17 secretion. Together, our data suggest that Tim-1-Fc protects cardiac grafts from chronic rejection by suppressing CD4 Th17 development and functionality. Therefore, Tim-1-Fc might be a potential immunosuppressive agent in the setting of cardiac transplantation.Entities:
Keywords: Th17; Tim-1; vasculopathy
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Year: 2014 PMID: 24551271 PMCID: PMC3925895
Source DB: PubMed Journal: Int J Clin Exp Pathol ISSN: 1936-2625