| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2112564 | Cancer Letters | 2014 | 10 Pages |
•miR-370 is down-regulated in endometrioid ovarian cancer cells.•miR-370 suppresses endometrioid ovarian cancer cell viability.•miR-370 enhances endometrioid ovarian cancer cell chemosensitivity to cDDP.•Endoglin is directly regulated by miR-370 in endometrioid ovarian cancer cells.•miR-370 acts as a tumor suppressor in endometrioid ovarian cancer.
MicroRNAs (miRNAs) are a class of non-coding RNAs that post-transcriptionally inhibit gene expression. In this study, we discovered that microRNA-370 (miR-370) was down-regulated in endometrioid ovarian cancer cells. In IGROV1 and TOV112D endometrioid ovarian cancer cells, miR-370 suppressed cellular viability and colony formation. miR-370 also enhanced endometrioid ovarian cancer cell chemosensitivity to cDDP. Endoglin (ENG) was directly and negatively regulated by miR-370. In addition, hypermethylation was a potential mechanism of miR-370 epigenetic silencing. We conclude that miR-370 acts as a tumor suppressor in endometrioid ovarian cancer via ENG regulation.
