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DNA methylation in inflammatory bowel disease and beyond
Authors:Daren Low  Atsushi Mizoguchi  Emiko Mizoguchi  Gastrointestinal Unit
Affiliation:Daren Low;Atsushi Mizoguchi;Emiko Mizoguchi;Gastrointestinal Unit,Department of Medicine,Massachusetts General Hospital,Harvard Medical School;Molecular Pathology Unit,Department of Pathology,Massachusetts General Hospital,Harvard Medical School;Center for the Study of Inflammatory Bowel Disease,Massachusetts General Hospital,Harvard Medical School;
Abstract:Inflammatory bowel disease (IBD) is a consequence of the complex, dysregulated interplay between genetic predisposition, environmental factors, and microbial composition in the intestine. Despite a great advancement in identifying host-susceptibility genes using genome-wide association studies (GWAS), the majority of IBD cases are still underrepresented. The immediate challenge in post-GWAS era is to identify other causative genetic factors of IBD. DNA methylation has received increasing attention for its mechanistical role in IBD pathogenesis. This stable, yet dynamic DNA modification, can directly affect gene expression that have important implications in IBD development. The alterations in DNA methylation associated with IBD are likely to outset as early as embryogenesis all the way until old-age. In this review, we will discuss the recent advancement in understanding how DNA methylation alterations can contribute to the development of IBD.
Keywords:Intestinal inflammation   Crohn’s disease   Colitis   DNA methyltransferase   Epi-therapy
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