Literature DB >> 19009023

Macrophage migration inhibitory factor promotes colorectal cancer.

Xing-Xiang He1, Ken Chen, Jun Yang, Xiao-Yu Li, Huo-Ye Gan, Cheng-Yong Liu, Thomas R Coleman, Yousef Al-Abed.   

Abstract

A growing body of evidence implicates macrophage migration inhibitory factor (MIF) in tumorigenesis and metastasis. In this study, we investigated whether MIF expression was associated with clinicopathologic features of colorectal carcinoma (CRC), especially in tumors with hepatic metastasis, and whether neutralization of endogenous MIF using anti-MIF therapeutics would inhibit tumor growth and/or decrease the frequency of colorectal hepatic metastases in a mouse colon carcinoma model. The concentration of serum MIF was positively correlated with an increased risk of hepatic metastasis in human patients with CRC (R = 1.25, 95% confidence internal = 1.02-1.52, P = 0.03). MIF was also dramatically upregulated in human colorectal tissue, with 20-40 times as many MIF-positive cells found in the mucosa of patients with CRC than in normal tissue (P < 0.001 ANOVA). Moreover, in those patients with metastatic colorectal cancer in the liver, MIF-positive cells were similarly increased in the diseased hepatic tissue. This increased MIF expression was restricted to diseased tissue and not found in areas of the liver with normal morphology. In subsequent in vitro experiments, we found that addition of recombinant MIF to colonic cell lines significantly increased their invasive properties and the expression of several genes (for example, matrix metalloproteinase 9 and vascular endothelial growth factor) known to be upregulated in cancerous tissue. Finally, we treated mice that had been given CT26 colon carcinoma cell transplants with anti-MIF therapeutics--either the MIF-specific inhibitor ISO-1 or neutralizing anti-MIF antibodies--and observed a significant reduction in tumor burden relative to vehicle-treated animals. Taken together, these data demonstrate that MIF expression was not only correlated with the presence of colorectal cancer but also may play a direct role in cancer development.

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Year:  2008        PMID: 19009023      PMCID: PMC2581606          DOI: 10.2119/molmed.2008.00107

Source DB:  PubMed          Journal:  Mol Med        ISSN: 1076-1551            Impact factor:   6.354


  53 in total

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3.  ISO-1 binding to the tautomerase active site of MIF inhibits its pro-inflammatory activity and increases survival in severe sepsis.

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Journal:  Gastroenterology       Date:  2005-11       Impact factor: 22.682

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  42 in total

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Journal:  Cytokine       Date:  2012-04-14       Impact factor: 3.861

2.  The MIF homologue D-dopachrome tautomerase promotes COX-2 expression through β-catenin-dependent and -independent mechanisms.

Authors:  Dan Xin; Beatriz E Rendon; Ming Zhao; Millicent Winner; Arlixer McGhee Coleman; Robert A Mitchell
Journal:  Mol Cancer Res       Date:  2010-11-11       Impact factor: 5.852

3.  MIF antagonist (CPSI-1306) protects against UVB-induced squamous cell carcinoma.

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4.  Association Between Genetic Polymorphism of the MIF Gene and Colorectal Cancer in Taiwan.

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5.  Macrophage migration inhibitory factor (MIF) enzymatic activity and lung cancer.

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Review 6.  MicroRNAs in colorectal cancer: role in metastasis and clinical perspectives.

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7.  Involvement of macrophage migration inhibitory factor in cancer and novel therapeutic targets.

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Review 8.  Inflammation and cancer: macrophage migration inhibitory factor (MIF)--the potential missing link.

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9.  An integrated signal transduction network of macrophage migration inhibitory factor.

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10.  Microarray-based cancer prediction using soft computing approach.

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