AI Article Synopsis
- CD4 T cells in the liver contribute to inflammation after ischemia/reperfusion (I/R) injury, and their activation mechanisms remain unclear.
- Using paricalcitol to generate tolerogenic dendritic cells (DCs), researchers found that these cells could reduce CD4 T-cell recruitment and tissue damage in postischemic livers.
- Blocking the interaction between CD4 T cells and DCs intensified inflammation and tissue injury, highlighting the critical role of hepatic DCs in modulating T-cell responses during I/R injury.
Article Abstract
CD4 T cells recruited to the liver play a key role in the pathogenesis of ischemia/reperfusion (I/R) injury. The mechanism of their activation during alloantigen-independent I/R is not completely understood. We hypothesized that liver-resident dendritic cells (DCs) interact with CD4 T cells in the postischemic liver and that modulation of DCs or T-cell-DC interactions attenuates liver inflammation. In mice, warm hepatic I/R (90/120-240 min) was induced. Tolerogenic DCs were generated by pretreatment of animals with the vitamin D analog paricalcitol. A mAb-CD44 was used for blockade of CD4 T-cell-DC interactions. As shown by 2-photon microscopy as well as confocal microscopy, CD4 T cells were closely colocalized with DCs in the postischemic liver. Pretreatment with paricalcitol attenuated I/R-induced maturation of DCs (flow cytometry), CD4 T-cell recruitment into the liver (intravital microscopy), and hepatocellular/microvascular damage (intravital microscopy, alanine aminotransferase/aspartate aminotransferase, histology). However, interruption of T-cell-DC interaction increased proinflammatory DC maturation and even enhanced tissue damage. Simultaneous treatment with an anti-CD44mAb completely abolished the beneficial effect of paricalcitol on T-cell migration and tissue injury. Our study demonstrates for the first time that hepatic DCs interact with CD4 T cells in the postischemic liver ; modulation of DCs and/or generation of tolerogenic DCs attenuates intrahepatic CD4 T-cell recruitment and reduces I/R injury; and interruption of CD44-dependent CD4 T-cell-DC interactions enhances tissue injury by preventing the modulatory effect of hepatic DCs on T cells, especially type 1 T helper effector cells. Thus, hepatic DCs are strongly involved in the promotion of CD4 T-cell-dependent postischemic liver inflammation.-Funken, D., Ishikawa-Ankerhold, H., Uhl, B., Lerchenberger, M., Rentsch, M., Mayr, D., Massberg, S., Werner, J., Khandoga, A. targeting of dendritic cells sets tolerogenic environment and ameliorates CD4 T-cell response in the postischemic liver.
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