4.7 Article

Reduced nonprotein thiols inhibit activation and function of MMP-9: Implications for chemoprevention

Journal

FREE RADICAL BIOLOGY AND MEDICINE
Volume 41, Issue 8, Pages 1315-1324

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.freeradbiomed.2006.07.014

Keywords

glutathione; nonprotein thiols; MMPs; cell invasion; thiolation; chemoprevention; free radicals

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Clinical studies demonstrate a positive correlation between the extent of matrix metalloproteinase (MNIP) activation and malignant progression of precancerous lesions. Therefore, identification of effective, well-tolerated MMP inhibitors represents a rational chemopreventive strategy. A variety of agents, including proteinases and thiol-oxidizing compounds, activate MMPs by initiating release of the propeptide's cysteine sulfur blockage of the MMP active site. Despite the importance of the propeptide's cysteine thiol in preserving MNIP latency, limited studies have evaluated the effects of reduced thiols on MMP function. This study investigated the effects of two naturally occurring nonprotein thiols, i.e., glutathione (GSH) and N-acetylcysteine (NAC), on activation, function, and cellular-extracellular matrix interactions of the basement-membrane-degrading gelatinase, MMP-9. Our results reveal that NAC and GSH employ protein S-thiolation to inhibit organomercurial activation of pro-MMP-9. Gelatinase activity assays showed that GSH and NAC significantly inhibited MMP-9 but not MMP-2 function, implying isoform structural specificity. Immunoblot analyses, which suggested GSH interacts with MMP-9's active-site Zn, were corroborated by computational molecular modeling. Cell invasion assays revealed that NAC enhanced endostatin's ability to inhibit human cancer cell invasion. Collectively, these data demonstrate that nonprotein thiols suppress MMP-9 activation and function and introduce the prospect for their use in chemopreventive applications. (c) 2006 Elsevier Inc. All rights reserved.

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