The HMGB1/RAGE axis triggers neutrophil-mediated injury amplification following necrosis
Peter Huebener, … , John D. Loike, Robert F. Schwabe
Peter Huebener, … , John D. Loike, Robert F. Schwabe
Published December 22, 2014
Citation Information: J Clin Invest. 2015;125(2):539-550. https://doi.org/10.1172/JCI76887.
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Research Article Hepatology Immunology Inflammation

The HMGB1/RAGE axis triggers neutrophil-mediated injury amplification following necrosis

Abstract

In contrast to microbially triggered inflammation, mechanisms promoting sterile inflammation remain poorly understood. Damage-associated molecular patterns (DAMPs) are considered key inducers of sterile inflammation following cell death, but the relative contribution of specific DAMPs, including high–mobility group box 1 (HMGB1), is ill defined. Due to the postnatal lethality of Hmgb1-knockout mice, the role of HMGB1 in sterile inflammation and disease processes in vivo remains controversial. Here, using conditional ablation strategies, we have demonstrated that epithelial, but not bone marrow–derived, HMGB1 is required for sterile inflammation following injury. Epithelial HMGB1, through its receptor RAGE, triggered recruitment of neutrophils, but not macrophages, toward necrosis. In clinically relevant models of necrosis, HMGB1/RAGE-induced neutrophil recruitment mediated subsequent amplification of injury, depending on the presence of neutrophil elastase. Notably, hepatocyte-specific HMGB1 ablation resulted in 100% survival following lethal acetaminophen intoxication. In contrast to necrosis, HMGB1 ablation did not alter inflammation or mortality in response to TNF- or FAS-mediated apoptosis. In LPS-induced shock, in which HMGB1 was considered a key mediator, HMGB1 ablation did not ameliorate inflammation or lethality, despite efficient reduction of HMGB1 serum levels. Our study establishes HMGB1 as a bona fide and targetable DAMP that selectively triggers a neutrophil-mediated injury amplification loop in the setting of necrosis.

Authors

Peter Huebener, Jean-Philippe Pradere, Celine Hernandez, Geum-Youn Gwak, Jorge Matias Caviglia, Xueru Mu, John D. Loike, Robert F. Schwabe

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Figure 5

RAGE, but not TLR4, mediates neutrophil recruitment following necrosis.

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RAGE, but not TLR4, mediates neutrophil recruitment following ...
(A) Migration of WT, Tlr4–/–, and RAGE-deficient (RAGE encoded by Ager) neutrophils (Ager–/– neutrophils, n ≥2 separate isolations per experiment) toward WT liver lysates. GM-CSF served as a positive control. (BE) Analysis of hepatic neutrophil infiltration (B), inflammatory gene expression (C), H&E staining and necrosis quantification (D), and serum ALT concentrations (E) in WT (n = 9) and Tlr4–/– (n = 7) mice treated with acetaminophen (300 mg/kg). (FI) Analysis of hepatic neutrophil infiltration (F), inflammatory gene expression (G), H&E staining and necrosis quantification (H), and serum ALT concentrations (I) in WT (n = 10) and Ager–/– (n = 9) mice treated with acetaminophen (300 mg/kg). *P < 0.05 and **P < 0.01 by unpaired 2-tailed t test. Scale bars: 200 μm.