The Role of HMGB1 in the Pathogenesis of Inflammatory and Autoimmune Diseases

Magna, Melinda; Pisetsky, David S.

doi:10.2119/molmed.2013.00164

Cited by 287 publications

(214 citation statements)

References 72 publications

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“…HMGB1 is a well-known endogenous ligand of TLR4 that has the ability to trigger an inflammatory response [23][24][25]. HMGB1-TLR4 interaction results in downstream activation of NFκB, and subsequent inflammation via generation of PIC and reactive oxygen species [67].…”

Section: Discussionmentioning

confidence: 99%

“…The release of HMGB1 marks the initiation of host defense or inflammatory tissue repair mechanisms [21]. Receptor blocking studies have shown that HMGB1 is a strong endogenous ligand of TLR4 receptor [22][23][24][25]. TLR4 is a receptor found on the cell surface that mediates the proinflammatory effects [26,27] of its ligands through the NFkB signaling pathway.…”

Section: Introductionmentioning

confidence: 99%

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Angiotensin II-induced hypertensive renal inflammation is mediated through HMGB1-TLR4 signaling in rat tubulo-epithelial cells

Nair

Ebenezer

Saini

et al. 2015

Experimental Cell Research

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Angiotensin II-induced hypertensive renal inflammation is mediated through HMGB1-TLR4 signaling in rat tubulo-epithelial cells

Nair

Ebenezer

Saini

et al. 2015

Experimental Cell Research

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“…In mammalian cells, the nucleus contains approximately 1 HMGB protein for every 10 nucleosomes (90). In addition to roles in DNA-dependent events, HMGB proteins sense cellular stress and function as extracellular cytokines, contributing to inflammatory and immune responses (91).…”

Section: High Mobility Group Proteinsmentioning

confidence: 99%

Yeast HMO1: Linker Histone Reinvented

Panday

Grove

2017

Microbiol Mol Biol Rev

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SUMMARY Eukaryotic genomes are packaged in chromatin. The higher-order organization of nucleosome core particles is controlled by the association of the intervening linker DNA with either the linker histone H1 or high mobility group box (HMGB) proteins. While H1 is thought to stabilize the nucleosome by preventing DNA unwrapping, the DNA bending imposed by HMGB may propagate to the nucleosome to destabilize chromatin. For metazoan H1, chromatin compaction requires its lysine-rich C-terminal domain, a domain that is buried between globular domains in the previously characterized yeast Saccharomyces cerevisiae linker histone Hho1p. Here, we discuss the functions of S. cerevisiae HMO1, an HMGB family protein unique in containing a terminal lysine-rich domain and in stabilizing genomic DNA. On ribosomal DNA (rDNA) and genes encoding ribosomal proteins, HMO1 appears to exert its role primarily by stabilizing nucleosome-free regions or “fragile” nucleosomes. During replication, HMO1 likewise appears to ensure low nucleosome density at DNA junctions associated with the DNA damage response or the need for topoisomerases to resolve catenanes. Notably, HMO1 shares with the mammalian linker histone H1 the ability to stabilize chromatin, as evidenced by the absence of HMO1 creating a more dynamic chromatin environment that is more sensitive to nuclease digestion and in which chromatin-remodeling events associated with DNA double-strand break repair occur faster; such chromatin stabilization requires the lysine-rich extension of HMO1. Thus, HMO1 appears to have evolved a unique linker histone-like function involving the ability to stabilize both conventional nucleosome arrays as well as DNA regions characterized by low nucleosome density or the presence of noncanonical nucleosomes.

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“…In this study, we detected the nuclear expression of HMGB1 in some of astrocytes, microglia and a few neurons in adult mouse spinal cord, which supplies more information to characterize the expression of HMGB1 in CNS and helps in discovering the potential CNS specific functions of HMGB1. Extracellular HMGB1, which is released passively by death cells or actively by stimulated cells such as macrophages, has been reported to play a key role in autoimmune diseases (Magna and Pisetsky, 2014), allograft rejection (Xia et al, 2014), ischemic stroke (Hayakawa et al, 2012), traumatic brain injury (Laird et al, 2014), and neurodegenerative diseases (Fang et al, 2012) as an inflammatory mediator. MS/EAE is a CNS specific autoimmune disease, which happens in adult human being or is induced in adult animal.…”

Section: Discussionmentioning

confidence: 99%