| Literature DB >> 27447360 |
Jung Hwa Park1, Jong-Hwa Jang2, Eun Jung Choi1, Young Seob Kim1, Eun Ji Lee1, In Duk Jung1, Hee Dong Han1, T-C Wu3,4,5,6, Chien-Fu Hung3,6, Tae Heung Kang1, Yeong-Min Park1.
Abstract
The identification of HMGB1 as a late-mediator in sepsis has highlighted HMGB1 as a promising therapeutic target for sepsis treatment. Recent studies have revealed that annexin A5, a 35 kDa Ca2+-dependent phospholipid binding protein, exerts anti-inflammatory effect by inhibiting LPS binding to TLR4/MD2 complex. Annexin A5 administration has been shown to protect against endotoxin lethality even when the treatment was given after the early cytokine response, which prompted our group to suspect that annexin A5 may inhibit the binding of HMGB1, as well as endotoxin to TLR4. Here we suggest annexin A5 as a new inhibitor of HMGB1-mediated pro-inflammatory cytokine production and coagulation in sepsis. We first confirmed the inhibitory role of annexin A5 in LPS-induced production of pro-inflammatory cytokines both in vitro and in vivo. We observed that annexin A5 protects against tissue damage and organ dysfunction during endotoxemia in vivo. We then assessed the inhibiting role of annexin A5 in HMGB1/TLR4 interaction, and showed that annexin A5 treatment reduces HMGB1-mediated cytokines IL6 and TNFα both in vitro and in vivo. Finally, we confirmed that anticoagulant property of annexin A5 persists in various septic conditions including elevated HMGB1. Overall, we suggest annexin A5 as an alternative therapeutic approach for controlling HMGB1-mediated pro-inflammation and coagulation in patients with sepsis.Entities:
Keywords: HMGB1 Protein; Toll-like receptor 4; anticoagulants; lipopolysaccharides; severe sepsis
Year: 2016 PMID: 27447360 PMCID: PMC5072405 DOI: 10.2119/molmed.2016.00026
Source DB: PubMed Journal: Mol Med ISSN: 1076-1551 Impact factor: 6.354