Endometrial Cancer and Hypermethylation: Regulation of DNA and MicroRNA by Epigenetics

Abstract

Endometrial cancer is the seventh most common cancer in women worldwide. Therefore elucidation of the pathogenesis and development of effective treatment for endometrial cancer are important. However, several aspects of the mechanism of carcinogenesis in the endometrium remain unclear. Associations with genetic variation and mutations of cancer-related genes have been shown, but these do not provide a complete explanation. Therefore, in recent years, epigenetic mechanisms that do not involve changes in DNA sequences have been examined. Studies aimed at detection of aberrant DNA hypermethylation in cancer cells present in microscopic amountsin vivoand application of the results to cancer diagnosis have also started. Breakdown of the DNA mismatch repair mechanism is thought to play a large role in the development of endometrial cancer, with changes in the expression of thehMLH1gene being particularly important. Silencing of genes such asAPCandCHFR,Sprouty 2,RASSF1A,GPR54,CDH1, andRSK4by DNA hypermethylation, onset of Lynch syndrome due to hereditary epimutation ofhMLH1andhMSH2mismatch repair genes, and regulation of gene expression by microRNAs may also underlie the carcinogenic mechanisms of endometrial cancer. Further understanding of these issues may permit development of new therapies.