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A matrix metalloproteinase inhibitor prevents processing of tumor necrosis factor alpha (TNF alpha) and abrogates endotoxin-induced lethality

被引:74
作者
Solorzano, CC
Ksontini, R
Pruitt, JH
Auffenberg, T
Tannahill, C
Galardy, RE
Schultz, GP
MacKay, SLD
Copeland, EM
Moldawer, LL
机构
[1] UNIV FLORIDA,COLL MED,DEPT SURG,GAINESVILLE,FL 32610
[2] UNIV FLORIDA,COLL MED,DEPT OBSTET & GYNECOL,GAINESVILLE,FL 32610
来源
SHOCK | 1997年 / 7卷 / 06期
关键词
D O I
10.1097/00024382-199706000-00007
中图分类号
R4 [临床医学];
学科分类号
1002 ; 100602 ;
摘要
Excessive tumor necrosis factor alpha (TNF alpha) production in response to Gram-negative bacteremia or endotoxemia can often lead to hypotension, shock, and increased mortality. Current approaches used to block the deleterious effects of exaggerated TNF alpha production rely on monoclonal antibodies or immunoadhesins that bind TNF alpha and thus prevent the interaction with its cellular receptors. This report examines whether a previously described inhibitor of matrix metalloproteinases, GM-6001, can inhibit TNF alpha processing and release and attenuate endotoxin-induced mortality. In human peripheral blood mononuclear cells stimulated in vitro with I mu g/mL endotoxin, GM-6001 at concentrations >5 mu g/mL blocked release of TNF alpha, but did not affect the release of either IL-1 beta or IL-6. GM-6001 also inhibited the release of soluble TNF receptor (p75) from peripheral blood mononuclear cells stimulated with endotoxin and/or TNF alpha. To confirm the role of secreted TNF alpha in endotoxic shock-induced mortality, C57BL/6 mice were challenged with either endotoxin alone (500 mu g/mouse) or endotoxin (100 ng/mouse) plus D-galactosamine (8 mg/mouse). GM-6001 pretreatment(100 mg/kg) significantly attenuated the 90-minute plasma TNF alpha response in both models and improved survival in mice treated with low-dose endotoxin plus D-galactosamine. However, plasma IL-1 beta and IL-6 concentrations al 90 min after endotoxin treatment were unaffected by GM-6001 following lethal endotoxin challenge, confirming the in vivo specificity of this matrix metalloproteinase inhibitor for TNF alpha processing. These findings demonstrate that a novel inhibitor of matrix metalloproteinases can prevent the release of TNF alpha both in vitro and in vivo, and can abrogate the harmful sequelae of endotoxemic shock.
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页码:427 / 431
页数:5
相关论文
共 29 条
[21]   MICE LACKING THE TUMOR-NECROSIS-FACTOR RECEPTOR-1 ARE RESISTANT TO TNF-MEDIATED TOXICITY BUT HIGHLY SUSCEPTIBLE TO INFECTION BY LISTERIA-MONOCYTOGENES [J].
ROTHE, J ;
LESSLAUER, W ;
LOTSCHER, H ;
LANG, Y ;
KOEBEL, P ;
KONTGEN, F ;
ALTHAGE, A ;
ZINKERNAGEL, R ;
STEINMETZ, M ;
BLUETHMANN, H .
NATURE, 1993, 364 (6440) :798-802
[22]  
SCHULTZ GS, 1992, INVEST OPHTH VIS SCI, V33, P3325
[23]  
Solorzano CC, 1997, J IMMUNOL, V158, P414
[24]   A genomic polymorphism within the tumor necrosis factor locus influences plasma tumor necrosis factor-alpha concentrations and outcome of patients with severe sepsis [J].
Stuber, F ;
Petersen, M ;
Bokelmann, F ;
Schade, U .
CRITICAL CARE MEDICINE, 1996, 24 (03) :381-384
[25]  
TARTAGLIA LA, 1993, J IMMUNOL, V151, P4637
[26]   TUMOR-NECROSIS-FACTOR SOLUBLE RECEPTORS CIRCULATE DURING EXPERIMENTAL AND CLINICAL INFLAMMATION AND CAN PROTECT AGAINST EXCESSIVE TUMOR-NECROSIS-FACTOR-ALPHA INVITRO AND INVIVO [J].
VANZEE, KJ ;
KOHNO, T ;
FISCHER, E ;
ROCK, CS ;
MOLDAWER, LL ;
LOWRY, SF .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (11) :4845-4849
[27]   A HUMAN TUMOR-NECROSIS-FACTOR (TNF) ALPHA-MUTANT THAT BINDS EXCLUSIVELY TO THE P55 TNF RECEPTOR PRODUCES TOXICITY IN THE BABOON [J].
VANZEE, KJ ;
STACKPOLE, SA ;
MONTEGUT, WJ ;
ROGY, MA ;
CALVANO, SE ;
HSU, KC ;
CHAO, M ;
MESCHTER, CL ;
LOETSCHER, H ;
STUBER, D ;
ETTLIN, U ;
WIPF, B ;
LESSLAUER, W ;
LOWRY, SF ;
MOLDAWER, LL .
JOURNAL OF EXPERIMENTAL MEDICINE, 1994, 179 (04) :1185-1191
[28]  
VASSALLI P, 1992, ANNU REV IMMUNOL, V10, P411, DOI 10.1146/annurev.immunol.10.1.411
[29]  
WANG P, 1995, SHOCK S2, V3, P35
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