Conventional DCs reduce liver ischemia/reperfusion injury in mice via IL-10 secretion
Zubin M. Bamboat, … , George Plitas, Ronald P. DeMatteo
Zubin M. Bamboat, … , George Plitas, Ronald P. DeMatteo
Published January 19, 2010
Citation Information: J Clin Invest. 2010;120(2):559-569. https://doi.org/10.1172/JCI40008.
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Research Article Immunology

Conventional DCs reduce liver ischemia/reperfusion injury in mice via IL-10 secretion

Abstract

TLRs are recognized as promoters of tissue damage, even in the absence of pathogens. TLR binding to damage-associated molecular patterns (DAMPs) released by injured host cells unleashes an inflammatory cascade that amplifies tissue destruction. However, whether TLRs possess the reciprocal ability to curtail the extent of sterile inflammation is uncertain. Here, we investigated this possibility in mice by studying the role of conventional DCs (cDCs) in liver ischemia/reperfusion (I/R) injury, a model of sterile inflammation. Targeted depletion of mouse cDCs increased liver injury after I/R, as assessed by serum alanine aminotransferase and histologic analysis. In vitro, we identified hepatocyte DNA as an endogenous ligand to TLR9 that promoted cDCs to secrete IL-10. In vivo, cDC production of IL-10 required TLR9 and reduced liver injury. In addition, we found that inflammatory monocytes recruited to the liver via chemokine receptor 2 were downstream targets of cDC IL-10. IL-10 from cDCs reduced production of TNF, IL-6, and ROS by inflammatory monocytes. Our results implicate inflammatory monocytes as mediators of liver I/R injury and reveal that cDCs respond to DAMPS during sterile inflammation, providing the host with protection from progressive tissue damage.

Authors

Zubin M. Bamboat, Lee M. Ocuin, Vinod P. Balachandran, Hebroon Obaid, George Plitas, Ronald P. DeMatteo

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Figure 1

Liver I/R induces cDC death.

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Liver I/R induces cDC death. CD11c-DTR mice, which were pretreated with ...
CD11c-DTR mice, which were pretreated with DT or PBS 18 hours earlier, underwent a sham laparotomy (Sham) or 1 hour of ischemia, followed by 12 hours of reperfusion (I/R). Ischemic liver cDCs were assessed by flow cytometry and are shown as (A) the percentage of hepatic leukocytes within each gated region or (B) the absolute number of cDCs within the ischemic liver. Ischemic liver cDCs from PBS-treated CD11c-DTR mice were analyzed for (C) the percentage of apoptosis (AnnexinV+PI) and necrosis (Annexin V+PI+) by flow cytometry or (D) CD40, CD80, and CD86 expression 12 hours after the sham procedure or I/R. Isotype controls are shown as shaded histograms. The bar graph represents cDC maturation data pooled from 3 independent experiments. Data represent mean ± SEM (BD). Data in all panels are representative of at least 3 independent experiments; n = 5 mice per group. *P < 0.05; **P < 0.01.