Rationale: Immune cells play an important role during the generation and resolution of thrombosis. T cells are powerful regulators of immune and nonimmune cell function, however, their role in sterile inflammation in venous thrombosis has not been systematically examined.
Objective: This study investigated the recruitment, activation, and inflammatory activity of T cells in deep vein thrombosis and its consequences for venous thrombus resolution.
Methods And Results: CD4 and CD8 T cells infiltrate the thrombus and vein wall rapidly on deep vein thrombosis induction and remain in the tissue throughout the thrombus resolution. In the vein wall, recruited T cells largely consist of effector-memory T (T) cells. Using T-cell receptor transgenic reporter mice, we demonstrate that deep vein thrombosis-recruited T receive an immediate antigen-independent activation and produce IFN-γ (interferon) in situ. Mapping inflammatory conditions in the thrombotic vein, we identify a set of deep vein thrombosis upregulated cytokines and chemokines that synergize to induce antigen-independent IFN-γ production in CD4 and CD8 T cells. Reducing the number of T cells through a depletion recovery procedure, we show that intravenous T activation determines neutrophil and monocyte recruitment and delays thrombus neovascularization and resolution. Examining T-cell recruitment in human venous stasis, we show that superficial varicose veins preferentially contain activated memory T cells.
Conclusions: T orchestrate the inflammatory response in venous thrombosis affecting thrombus resolution.
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| http://dx.doi.org/10.1161/CIRCRESAHA.116.309301 | DOI Listing |
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