NOVEL HMGB1-INHIBITING THERAPEUTIC AGENTS FOR EXPERIMENTAL SEPSIS

被引：124

作者：

Wang, Haichao ^{[1
,2
]}

Ward, Mary F. ^{[2
]}

Sama, Andrew E. ^{[2
]}

机构：

[1] N Shore LIJ Hlth Syst, Feinstein Inst Med Res, Manhasset, NY 11030 USA

[2] NYU, Sch Med, N Shore Univ Hosp, Dept Emergency Med, Manhasset, NY USA

来源：

SHOCK | 2009年 / 32卷 / 04期

基金：

美国国家卫生研究院;

关键词：

Innate immune cells; phagocytes; inflammation; cytokines; sepsis; antibodies; HMGB1; tanshinones; MOBILITY GROUP BOX-1; NECROSIS-FACTOR-ALPHA; GRAM-NEGATIVE BACTEREMIA; CHROMATIN PROTEIN HMGB1; GLYCATION END-PRODUCTS; ACUTE LUNG INJURY; HIGH-MOBILITY-GROUP-BOX-1; PROTEIN; LETHAL SEPSIS; SEPTIC SHOCK; MONOCLONAL-ANTIBODY;

D O I：

10.1097/SHK.0b013e3181a551bd

中图分类号：

R4 [临床医学];

学科分类号：

1002 ; 100602 ;

摘要：

Sepsis refers to a systemic inflammatory response syndrome resulting from a microbial infection. The inflammatory response is partly mediated by innate immune cells (such as macrophages, monocytes, and neutrophils), which not only ingest and eliminate invading pathogens but also initiate an inflammatory response by producing early (e.g., TNF and IFN-gamma and late (e.g., high-mobility group box [HMGB1]) proinflammatory cytokines. Here, we briefly review emerging evidence that support extracellular HMGB1 as a late mediator of experimental sepsis and discuss therapeutic potential of several HMGB1-inhibiting agents (including neutralizing antibodies and steroid-like tanshinones) in experimental sepsis.

引用

页码：348 / 357

页数：10

共 143 条

[21] A new model of sciatic inflammatory neuritis (SIN): induction of unilateral and bilateral mechanical allodynia following acute unilateral peri-sciatic immune activation in rats [J].

Chacur, M ;

Milligan, ED ;

Gazda, LS ;

Armstrong, C ;

Wang, HC ;

Tracey, KJ ;

Maier, SF ;

Watkins, LR .

PAIN, 2001, 94 (03) :231-244

[22] Suppression of HMGB1 release by stearoyl lysophosphatidylcholine: an additional mechanism for its therapeutic effects in experimental sepsis [J].

Chen, GQ ;

Li, JH ;

Qiang, XL ;

Czura, CJ ;

Ochani, M ;

Ochani, K ;

Ulloa, L ;

Yang, H ;

Tracey, KJ ;

Wang, P ;

Sama, AE ;

Wang, HC .

JOURNAL OF LIPID RESEARCH, 2005, 46 (04) :623-627

[23] Dengue virus infection induces passive release of high mobility group box 1 protein by epithelial cells [J].

Chen, Lien-Cheng ;

Yeh, Trai-Ming ;

Wu, Huey-Nan ;

Lin, Yi-Ying ;

Shyu, Huey-Wen .

JOURNAL OF INFECTION, 2008, 56 (02) :143-150

[24] Cardiovascular effects of Danshen [J].

Cheng, Tsung O. .

INTERNATIONAL JOURNAL OF CARDIOLOGY, 2007, 121 (01) :9-22

[25] Ghrelin protects against experimental sepsis by inhibiting high-mobility group box 1 release and by killing bacteria [J].

Chorny, Alejo ;

Anderson, Per ;

Gonzalez-Rey, Elena ;

Delgado, Mario .

JOURNAL OF IMMUNOLOGY, 2008, 180 (12) :8369-8377

[26] Neuropeptides rescue mice from lethal sepsis by down-regulating secretion of the late-acting inflammatory mediator high mobility group box 1 [J].

Chorny, Alejo ;

Delgado, Mario .

AMERICAN JOURNAL OF PATHOLOGY, 2008, 172 (05) :1297-1302

[27] The mechanism of cell death during West Nile virus infection is dependent on initial infectious dose [J].

Chu, JJH ;

Ng, ML .

JOURNAL OF GENERAL VIROLOGY, 2003, 84 :3305-3314

[28] Adjunctive therapy in sepsis: a critical analysis of the clinical trial programme [J].

Cohen, J .

BRITISH MEDICAL BULLETIN, 1999, 55 (01) :212-225

[29]

DAVIS CE, 1969, J IMMUNOL, V102, P563

[30] The nuclear protein HMGB1, a new kind of chemokine? [J].

Degryse, B ;

de Virgilio, M .

FEBS LETTERS, 2003, 553 (1-2) :11-17

← 1 2 3 4 5 6 7 8 9 10 →