[No authors listed]
In a previous study, it was demonstrated that Tâcell immune response cDNA 7 (TIRC7) levels reflect the efficacy of treatment of patients with acute graftâversusâhost disease (GVHD). However, the pathogenesis of TIRC7 in acute GVHD remains poorly understood. Lymphocytes from patients with acute GVHD were selected as targeT cells, and the effects of TIRC7 on cytotoxic T lymphocyte antigenâ4 (CTLAâ4), T cell activation and cytokine secretion were observed by electroporation. A mouse model of acute GVHD was established; antiâTIRC7 and antiâCTLAâ4 monoclonal antibodies were intraperitoneally injected into recipient mice. Then, the effects of TIRC7 and CTLAâ4 on T cell activation and acute GVHD were monitored. After TIRC7 expression was downregulated, CTLAâ4 levels were decreased and phosphorylation was reduced; conversely, the activation capacity of T lymphocytes was elevated, and the secretion of interferonâγ and other cytokines was increased. The mice in the TIRC7 + CTLAâ4 coâadministration group exhibited the lowest acute GVHD scores, with the longest average survival time and shortest recovery time of hematopoietic reconstitution. In conclusion, the results indicated that TIRC7 may positively regulate the function of CTLAâ4 and inhibit T cell activation, thus suppressing the development and progression of acute GVHD.
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