Diet Restriction Inhibits Apoptosis and HMGB1 Oxidation and Promotes Inflammatory Cell Recruitment during Acetaminophen Hepatotoxicity

Antoine, Daniel J.; Williams, Dominic P.; Kipar, Anja; Laverty, Hugh; Park, B. Kevin

doi:10.2119/molmed.2010.00126

Cited by 95 publications

(127 citation statements)

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“…Acetaminophen overdose is a well-known cause of DILI (Lee, 2004). A number of animal and human studies have demonstrated that serum HMGB1 is a diagnosis and severity-assessment biomarker of acute liver injury induced by acetaminophen, as well as other drugs (Antoine et al, 2013; Antoine et al, 2012a; Antoine et al, 2010; Dragomir et al, 2011; Gong et al, 2010a; Yang et al, 2012g; Zhou et al, 2011c). HMGB1 release during acetaminophen-mediated liver injury impairs the innate immune response and accelerates the inflammatory response (Scaffidi et al, 2002; Wang et al, 2007a; Wang et al, 2013m).…”

Section: Hmgb1 and Diseasementioning

confidence: 99%

HMGB1 in health and disease

Kang

Chen

Zhang

et al. 2014

Molecular Aspects of Medicine

801

828

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Complex genetic and physiological variations as well as environmental factors that drive emergence of chromosomal instability, development of unscheduled cell death, skewed differentiation, and altered metabolism are central to the pathogenesis of human diseases and disorders. Understanding the molecular bases for these processes is important for the development of new diagnostic biomarkers, and for identifying new therapeutic targets. In 1973, a group of non-histone nuclear proteins with high electrophoretic mobility was discovered and termed High-Mobility Group (HMG) proteins. The HMG proteins include three superfamilies termed HMGB, HMGN, and HMGA. High-mobility group box 1 (HMGB1), the most abundant and well-studied HMG protein, senses and coordinates the cellular stress response and plays a critical role not only inside of the cell as a DNA chaperone, chromosome guardian, autophagy sustainer, and protector from apoptotic cell death, but also outside the cell as the prototypic damage associated molecular pattern molecule (DAMP). This DAMP, in conjunction with other factors, thus has cytokine, chemokine, and growth factor activity, orchestrating the inflammatory and immune response. All of these characteristics make HMGB1 a critical molecular target in multiple human diseases including infectious diseases, ischemia, immune disorders, neurodegenerative diseases, metabolic disorders, and cancer. Indeed, a number of emergent strategies have been used to inhibit HMGB1 expression, release, and activity in vitro and in vivo. These include antibodies, peptide inhbitiors, RNAi, anti-coagulants, endogenous hormones, various chemical compounds, HMGB1-receptor and signaling pathway inhibition, artificial DNAs, physical strategies including vagus nerve stimulation and other surgical approaches. Future work further investigating the details of HMGB1 localizationtion, structure, post-translational modification, and identifccation of additional partners will undoubtedly uncover additional secrets regarding HMGB1’s multiple functions.

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Section: Hmgb1 and Diseasementioning

confidence: 99%

HMGB1 in health and disease

Kang

Chen

Zhang

et al. 2014

Molecular Aspects of Medicine

801

828

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“…It is likely that this protein took the all-thiol form of HMGB1 as it had chemotactic qualities to recruit enterocytes, smooth muscle, and endothelial, and stem cells (32,51,74,81,99,121,131). During active inflammation the predominant form of HMGB1 is thought to be the disulfide bond C23 and C45 (disulfide-HMGB1); however, when inflammation begins to subside, HMGB1 is terminally oxidized at the cysteine residues rendering it biological inactive (oxidized-HMGB1) (6,121,135). Subsequently, an oxidizing environment following inflammation or injury may promote HMGB1 cytokine activity, instead of cellular repair by monocyte recruitment (121).…”

Section: Hmgb1 Releasementioning

confidence: 99%

The HMGB1-RAGE Inflammatory Pathway: Implications for Brain Injury-Induced Pulmonary Dysfunction

Weber

Allette

Wilkes

et al. 2015

Antioxidants & Redox Signaling

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“…Anti-HMGB1 monoclonal antibody [29] Anti-HMGB1 polyclonal antibody [28] Box A antagonist [28,30] Nuclear retention [24,27] Endotoxemia Inhibition of HMBG-1 release [31] CLP Anti-HMGB1 monoclonal antibody [34] Glucan phosphate (nuclear sequestering of HMGB1) [ Ischemia-reperfusion (kidney) Nuclear retention [37] Anti-HMGB1 polyclonal antibody [39] Ischemia-reperfusion (intestine) Anti-HMGB1 polyclonal antibody [41] Hepatoxicity Anti-HMGB1 polyclonal antibody [42] Pain Systemic injection of glycyrrhizin (binds to HMGB1) [43] Anti-HMGB1 polyclonal antibody [44,45] Islet transplantation Anti-HMGB1 monoclonal antibody [46] Atherosclerosis Anti-HMGB1 monoclonal antibody [47] Ischemia (brain) siRNA for HMGB1 [48] Anti-HMGB1 monoclonal antibody [49] Brain injury/damage to the blood-brain barrier Box A antagonist [50] Anti-HMGB1 monoclonal antibody [51] Intestinal tissue damage Anti-HMGB1 polyclonal antibody, nuclear retention [52] CLP, cecal ligation and puncture.…”

Section: Arthritismentioning

confidence: 99%