[No authors listed]
Promoter methylationâassociated silencing of cancerâassociated microRNAs (miRNAs) is a common epigenetic mechanism during tumorigenesis in various types of human cancer. However, this has not been comprehensively examined in endometrial carcinoma (EC). In the present study, an miRNA microarray consisting of 1,347 common human miRNAs was used to select potential tumor suppressive miRNAs that were hyperâmethylated in EC. This led to the identification of miRâ638, miRâ210 and miRâ3665. The methylation status of miRâ638 was examined by bisulfite sequencing polymerase chain reaction and miRâ638 expression was measured by TaqMan miRNA assays. EC cell lines transfected with vectors overexpressing miRâ638, its target gene myocyte enhancer factor 2C (MEF2C) or both, were constructed. Dualâluciferase reporter assays, a xenograft mouse model and rescue experiments were designed to study miRâ638 and its target gene MEF2C. The results indicated that the promoter region of miRâ638 was highly methylated and the expression of miRâ638 was significantly downregulated in cancerous tissues from 42 patients with EC who underwent surgical resection. Additionally, a low expression of miRâ638 was significantly associated with advanced Federation of Gynecology and Obstetrics stage and was demonstrated to indicate shorter diseaseâfree survival. Functional studies indicated that the overexpression of miRâ638 in EC cell lines inhibited in vitro tumor progression and in vivo tumorigenicity. MEF2C was verified as a direct target of miRâ638 and was demonstrated to mediate the tumorâsuppressive function of miRâ638 in EC.
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