Redox modulation of HMGB1-related signaling

Janko C, Filipovic M, Munoz Becerra L, Schorn C, Schett G, Ivanovic-Burmazovic I, Herrmann M (2014)

Publication Type: Journal article, Review article

Publication year: 2014

Journal

Antioxidants & Redox Signaling Mary Ann Liebert

Original Authors: Janko C., Filipovic M., Munoz L.E., Schorn C., Schett G., Ivanovic-Burmazovic I., Herrmann M.

Publisher: Mary Ann Liebert

Book Volume: 20

Pages Range: 1075-1085

Journal Issue: 7

DOI: 10.1089/ars.2013.5179

Abstract

Significance: In the cells' nuclei, high-mobility group box protein 1 (HMGB1) is a nonhistone chromatin-binding protein involved in the regulation of transcription. Extracellularly, HMGB1 acts as a danger molecule with properties of a proinflammatory cytokine. It can be actively secreted from myeloid cells or passively leak from any type of injured, necrotic cell. Increased serum levels of active HMGB1 are often found in pathogenic inflammatory conditions and correlate with worse prognoses in cancer, sepsis, and autoimmunity. By damaging cells, superoxide and peroxynitrite promote leakage of HMGB1. Recent Advances: The activity of HMGB1 strongly depends on its redox state: Inflammatory-active HMGB1 requires an intramolecular disulfide bond (Cys23 and Cys45) and a reduced Cys106. Oxidation of the latter blocks its stimulatory activity and promotes immune tolerance. Critical Issues: Reactive oxygen and nitrogen species create an oxidative environment and can be detoxified by superoxide dismutase (SOD), catalase, and peroxidases. Modifications of the oxidative environment influence HMGB1 activity. Future Directions: In this review, we hypothesize that manipulations of an oxidative environment by SOD mimics or by hydrogen sulfide are prone to decrease tissue damage. Both the concomitant decreased HMGB1 release and its redox chemical modifications ameliorate inflammation and tissue damage. Antioxid. Redox Signal. 20, 1075-1085. © Mary Ann Liebert, Inc.

Authors with CRIS profile

Christina Janko Lehrstuhl für Genetik Milos Filipovic Lehrstuhl für Bioanorganische Chemie Christine Schorn Lehrstuhl für Genetik Georg Schett Lehrstuhl für Innere Medizin III Ivana Ivanovic-Burmazovic Lehrstuhl für Bioanorganische Chemie Martin Herrmann Department of Medicine 3 – Rheumatology and Immunology

How to cite

APA:

Janko, C., Filipovic, M., Munoz Becerra, L., Schorn, C., Schett, G., Ivanovic-Burmazovic, I., & Herrmann, M. (2014). Redox modulation of HMGB1-related signaling. Antioxidants & Redox Signaling, 20(7), 1075-1085. https://dx.doi.org/10.1089/ars.2013.5179

MLA:

Janko, Christina, et al. "Redox modulation of HMGB1-related signaling." Antioxidants & Redox Signaling 20.7 (2014): 1075-1085.

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