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Nutrient isothiocyanates covalently modify and inhibit the inflammatory cytokine macrophage migration inhibitory factor (MIF)

Janet V Cross, Joshua M Rady, Frank W Foss, Charles E Lyons, Timothy L Macdonald, and Dennis J Templeton

Biochem J 423(3):315-321 (2009) PMID 19723024 PMCID PMC2858637

Dietary ITCs (isothiocyanates) prevent cancer and show other bioactivities in vivo. As electrophiles, ITCs may covalently modify cellular proteins. Using a novel proteomics screen, we identified MIF (macrophage migration inhibitory factor) as the principal target of nutrient ITCs in intact cells. ITCs covalently modify the N-terminal proline residue of MIF and extinguish its catalytic tautomerase activity. MIF deficiency does not prevent induction of Phase 2 gene expression, a hallmark of many cancer chemopreventives, including ITCs. Due to the emerging role of MIF in the control of malignant cell growth and its clear involvement in inflammation, inhibition of MIF by nutrient ITCs suggests therapeutic strategies for inflammatory diseases and cancer.

DOI: 10.1042/BJ20091170
Version: za2963e q8za2 q8zb8 q8zc0 q8zdc q8ze2 q8zfd q8zga
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