| Literature DB >> 28443478 |
Fuminori Ito1, Yuki Yamada1, Aiko Shigemitsu1, Mika Akinishi1, Hiroko Kaniwa1, Ryuta Miyake1, Shoichiro Yamanaka1, Hiroshi Kobayashi1.
Abstract
Aberrant DNA methylation and histone modification are associated with an increased risk of reproductive disorders such as endometriosis. However, a cause-effect relationship between epigenetic mechanisms and endometriosis development has not been fully determined. This review provides current information based on oxidative stress in epigenetic modification in endometriosis. This article reviews the English-language literature on epigenetics, DNA methylation, histone modification, and oxidative stress associated with endometriosis in an effort to identify epigenetic modification that causes a predisposition to endometriosis. Oxidative stress, secondary to the influx of hemoglobin, heme, and iron during retrograde menstruation, is involved in the expression of CpG demethylases, ten-eleven translocation, and jumonji (JMJ). Ten-eleven translocation and JMJ recognize a wide range of endogenous DNA methyltransferases (DNMTs). The increased expression levels of DNMTs may be involved in the subsequent downregulation of the decidualization-related genes. This review supports the hypothesis that there are at least 2 distinct phases of epigenetic modification in endometriosis: the initial wave of iron-induced oxidative stress would be followed by the second big wave of epigenetic modulation of endometriosis susceptibility genes. We summarize the recent advances in our understanding of the underlying epigenetic mechanisms focusing on oxidative stress in endometriosis.Entities:
Keywords: DNA methylation; endometriosis; epigenetics; histone modification
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Year: 2017 PMID: 28443478 DOI: 10.1177/1933719117704909
Source DB: PubMed Journal: Reprod Sci ISSN: 1933-7191 Impact factor: 3.060