Literature DB >> 17206675

Comparative analysis of colonic gene expression of three experimental colitis models mimicking inflammatory bowel disease.

Anje A te Velde1, Floor de Kort, Ellen Sterrenburg, Inge Pronk, Fiebo J W ten Kate, Daniel W Hommes, Sander J H van Deventer.   

Abstract

BACKGROUND: Mouse models of inflammatory bowel diseases (IBD) are used to unravel the pathophysiology of IBD and to study new treatment modalities, but their relationship to Crohn's disease (CD) or ulcerative colitis (UC) is speculative.
METHODS: Using Agilent mouse TOX oligonucleotide microarrays, we analyzed colonic gene expression profiles in three widely used models of experimental colitis. In 2 of the models (TNBS and DSS-induced colitis), exogenous agents induce the colitis. In the third model the colitis is induced after transfer of a T-cell population (CD4(+)CD45RB(high) T cells) that lacks regulatory cells into an immunodeficient host.
RESULTS: Compared with control mice, in DSS, TNBS, and the CD45RB transfer colitis mice, 387, 21, and 582 genes were more than 2-fold upregulated in the intestinal mucosa. Analyses of exclusively shared gene expression profiles between the different models revealed that DSS/transfer colitis share 69 concordantly upregulated genes, DSS/TNBS 6, and TNBS/transfer colitis 1. Seven genes were upregulated in all three models. The CD45RB transfer model expression profile included the most genes that are known to be upregulated in IBD. Of 32 genes that are known to change transcriptional activity in IBD (TNF, IFN-gamma, Ltbeta, IL-6, IL-16, IL-18R1, IL-22, CCR2, 7, CCL2, 3, 4, 5, 7, 11, 17, 20, CXCR3, CXCL1, 5, 10, Mmp3, 7,9, 14, Timp1, Reg3gamma, and Pap, S-100a8, S-100a9, Abcb1, and Ptgs2), 2/32 are upregulated in TNBS, 15/32 are upregulated or downregulated in DSS and 30/32 are upregulated or downregulated in the CD45RB transfer colitis.
CONCLUSION: The pattern of gene expression in the CD45RB transfer model most closely reflects altered gene expression in IBD.

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Year:  2007        PMID: 17206675     DOI: 10.1002/ibd.20079

Source DB:  PubMed          Journal:  Inflamm Bowel Dis        ISSN: 1078-0998            Impact factor:   5.325


  67 in total

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Review 4.  Pharmacological intervention studies using mouse models of the inflammatory bowel diseases: translating preclinical data into new drug therapies.

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Journal:  Inflamm Bowel Dis       Date:  2011-02-10       Impact factor: 5.325

5.  The myeloid differentiation factor 88 (MyD88) is required for CD4+ T cell effector function in a murine model of inflammatory bowel disease.

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6.  Molecular Characterization of the Onset and Progression of Colitis in Inoculated Interleukin-10 Gene-Deficient Mice: A Role for PPARalpha.

Authors:  Bianca Knoch; Matthew P G Barnett; Janine Cooney; Warren C McNabb; Diane Barraclough; William Laing; Shuotun Zhu; Zaneta A Park; Paul Maclean; Scott O Knowles; Nicole C Roy
Journal:  PPAR Res       Date:  2010-06-30       Impact factor: 4.964

7.  Maize global transcriptomics reveals pervasive leaf diurnal rhythms but rhythms in developing ears are largely limited to the core oscillator.

Authors:  Kevin R Hayes; Mary Beatty; Xin Meng; Carl R Simmons; Jeffrey E Habben; Olga N Danilevskaya
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8.  Changes in colon gene expression associated with increased colon inflammation in interleukin-10 gene-deficient mice inoculated with Enterococcus species.

Authors:  Matthew P G Barnett; Warren C McNabb; Adrian L Cookson; Shuotun Zhu; Marcus Davy; Bianca Knoch; Katia Nones; Alison J Hodgkinson; Nicole C Roy
Journal:  BMC Immunol       Date:  2010-07-15       Impact factor: 3.615

9.  Multifactorial patterns of gene expression in colonic epithelial cells predict disease phenotypes in experimental colitis.

Authors:  Aubrey L Frantz; Maria E C Bruno; Eric W Rogier; Halide Tuna; Donald A Cohen; Subbarao Bondada; R Lakshman Chelvarajan; J Anthony Brandon; C Darrell Jennings; Charlotte S Kaetzel
Journal:  Inflamm Bowel Dis       Date:  2012-02-22       Impact factor: 5.325

10.  A role for CD47 in the development of experimental colitis mediated by SIRPalpha+CD103- dendritic cells.

Authors:  Genevieve Fortin; Marianne Raymond; Vu Quang Van; Manuel Rubio; Patrick Gautier; Marika Sarfati; Denis Franchimont
Journal:  J Exp Med       Date:  2009-08-24       Impact factor: 14.307

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