Effect of MDR1 gene promoter methylation in patients with ulcerative colitis
Altered MDR1 expression and/or function contribute to the pathogenesis of inflammatory bowel disease (IBD). DNA methylation was shown as an important mechanism in gene silencing. We investigated DNA methylation of the MDR1 gene in ulcerative colitis (UC) and its relation to MDR1 C3435T genotypes. Ei...
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Veröffentlicht in: | International journal of molecular medicine 2009-04, Vol.23 (4), p.521-527 |
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Zusammenfassung: | Altered MDR1 expression and/or function contribute to the pathogenesis
of inflammatory bowel disease (IBD). DNA methylation was shown as an important
mechanism in gene silencing. We investigated DNA methylation of the MDR1 gene
in ulcerative colitis (UC) and its relation to MDR1 C3435T genotypes. Eighty-three
UC patients were enrolled. Methylation of MDR1 promoter was determined by methylation
specific polymerase (MSP) for rectal inflammatory mucosa from all patients and
normal terminal ileum from 17 patients. Promoter methylation of MDR1 gene was
also quantified by digital densitographic analysis following MSP. MDR1 methylation
was detected in 51 (61.4%) out of 83 patients in rectal inflammatory mucosa. Mean
methylation level of MDR1 gene in rectal inflammatory mucosa was significantly
higher than in normal terminal ileum (p=0.021). MDR1 methylation occurred more
frequently in total colitis, and total + left side colitis, compared to rectal
colitis (p=0.001, 0.013, respectively). Higher methylation levels were also associated
with chronic continuous type (p=0.034) and earlier onset of disease (p=0.038).
The 3435 CC+CT genotype of MDR1 was associated with more than 6-fold increased
risk of MDR1 methylation, especially in UC patients with 9 years and shorter duration.
Both frequency and level of MDR1 methylation were higher in UC onset at younger
or in middle age with the same genotype. MDR1 methylation frequently occurred
in inflammatory rectal mucosa from UC patients and was influenced by MDR1 C3435T
polymorphism, especially in patients with shorter duration and younger onset. |
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ISSN: | 1107-3756 |
DOI: | 10.3892/ijmm_00000160 |