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W2171738609 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." @default.
W2171738609 created "2016-06-24" @default.
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W2171738609 date "2019-03-04" @default.
W2171738609 modified "2023-10-17" @default.
W2171738609 title "The HMGB1/RAGE axis triggers neutrophil-mediated injury amplification following necrosis" @default.
W2171738609 cites W1615683666 @default.
W2171738609 cites W1672954108 @default.
W2171738609 cites W1718807171 @default.
W2171738609 cites W1965588383 @default.
W2171738609 cites W1966977448 @default.
W2171738609 cites W1973412402 @default.
W2171738609 cites W1975202537 @default.
W2171738609 cites W1978083259 @default.
W2171738609 cites W1981010107 @default.
W2171738609 cites W1985042500 @default.
W2171738609 cites W1987751311 @default.
W2171738609 cites W1992082488 @default.
W2171738609 cites W1992944558 @default.
W2171738609 cites W1993877349 @default.
W2171738609 cites W1995337037 @default.
W2171738609 cites W1998212202 @default.
W2171738609 cites W1999246265 @default.
W2171738609 cites W2002817805 @default.
W2171738609 cites W2003499107 @default.
W2171738609 cites W2004266769 @default.
W2171738609 cites W2005647807 @default.
W2171738609 cites W2014678245 @default.
W2171738609 cites W2018653121 @default.
W2171738609 cites W2025501637 @default.
W2171738609 cites W2029068688 @default.
W2171738609 cites W2034594119 @default.
W2171738609 cites W2038434279 @default.
W2171738609 cites W2038970416 @default.
W2171738609 cites W2042851093 @default.
W2171738609 cites W2048922948 @default.
W2171738609 cites W2052308581 @default.
W2171738609 cites W2055132644 @default.
W2171738609 cites W2060724258 @default.
W2171738609 cites W2065429310 @default.
W2171738609 cites W2072805330 @default.
W2171738609 cites W2074291164 @default.
W2171738609 cites W2080586887 @default.
W2171738609 cites W2085153086 @default.
W2171738609 cites W2093826422 @default.
W2171738609 cites W2093982770 @default.
W2171738609 cites W2114445825 @default.
W2171738609 cites W2117584263 @default.
W2171738609 cites W2117807235 @default.
W2171738609 cites W2119961443 @default.
W2171738609 cites W2132812582 @default.
W2171738609 cites W2135131688 @default.
W2171738609 cites W2141438911 @default.
W2171738609 cites W2144152742 @default.
W2171738609 cites W2144578574 @default.
W2171738609 cites W2145736817 @default.
W2171738609 cites W2147426561 @default.
W2171738609 cites W2147627101 @default.
W2171738609 cites W2151277012 @default.
W2171738609 cites W2160369507 @default.
W2171738609 cites W2164714222 @default.
W2171738609 cites W2164906049 @default.
W2171738609 cites W2164990391 @default.
W2171738609 cites W2169930621 @default.
W2171738609 cites W2325491525 @default.
W2171738609 cites W2371948111 @default.
W2171738609 cites W2417433128 @default.
W2171738609 cites W46766210 @default.
W2171738609 cites W67488918 @default.
W2171738609 doi "https://doi.org/10.1172/jci126975" @default.
W2171738609 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6436859" @default.
W2171738609 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30829652" @default.
W2171738609 hasPublicationYear "2019" @default.
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