miR-137 is a tumor suppressor in endometrial cancer and is repressed by DNA hypermethylation

miR-137 is a tumor suppressor in endometrial cancer and is repressed by DNA hypermethylation

Endometrial cancer is the most common gynecological cancer in the United States. We wanted to identify epigenetic aberrations involving microRNAs (miRNAs), whose genes become hypermethylated in endometrial primary tumors. By integrating known miRNA sequences from the miRNA database (miRBase) with DN...

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Veröffentlicht in:Laboratory investigation 2018-11, Vol.98 (11), p.1397-1407
Hauptverfasser: Zhang, Wei, Chen, Jo-Hsin, Shan, Tianjiao, Aguilera-Barrantes, Irene, Wang, Li-Shu, Huang, Tim Hui-Ming, Rader, Janet S., Sheng, Xiugui, Huang, Yi-Wen
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Sprache:eng
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Adenocarcinoma - genetics
Adenocarcinoma - metabolism
Animals
Cancer
Cell Line, Tumor
Cell proliferation
CpG islands
Deoxyribonucleic acid
DNA
DNA Methylation
DNA sequencing
Endometrial cancer
Endometrial Neoplasms - genetics
Endometrial Neoplasms - metabolism
Endometrium
Enhancer of Zeste Homolog 2 Protein - metabolism
Epigenetics
Female
Gene Silencing
Histone Demethylases - metabolism
Hormone replacement therapy
Humans
Laboratory Medicine
Medicine
Medicine & Public Health
Mice, Nude
MicroRNAs - genetics
MicroRNAs - metabolism
miRNA
Nucleotide sequence
Pathology
Tumor suppressor genes
Tumors
Xenografts
Xenotransplantation
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Zusammenfassung:Endometrial cancer is the most common gynecological cancer in the United States. We wanted to identify epigenetic aberrations involving microRNAs (miRNAs), whose genes become hypermethylated in endometrial primary tumors. By integrating known miRNA sequences from the miRNA database (miRBase) with DNA methylation data from methyl-CpG-capture sequencing, we identified 111 differentially methylated regions (DMRs) associated with CpG islands (CGIs) and miRNAs. Among them, 22 DMRs related to 29 miRNAs and within 8 kb of CGIs were hypermethylated in endometrial tumors but not in normal endometrium. miR-137 was further validated in additional endometrial primary tumors. Hypermethylation of miR-137 was found in both endometrioid and serous endometrial cancer (P < 0.01), and it led to the loss of miR-137 expression. Treating hypermethylated endometrial cancer cells with epigenetic inhibitors reactivated miR-137. Moreover, genetic overexpression of miR-137 suppressed cancer cell proliferation and colony formation in vitro. When transfected cancer cells were implanted into nude mice, the cells that overexpressed miR-137 grew more slowly and formed smaller tumors (P < 0.05) than vector transfectants. Histologically, xenograft tumors from cancer cells expressing miR-137 were less proliferative (P < 0.05), partly due to inhibition of EZH2 and LSD1 expression (P < 0.01) in both the transfected cancer cells and tumors. Reporter assays indicated that miR-137 targets EZH2 and LSD1. These results suggest that miR-137 is a tumor suppressor that is repressed in endometrial cancer because the promoter of its gene becomes hypermethylated. The authors aimed to identify epigenetic aberrations involving microRNAs (miRNAs) whose genes become hypermethylated in endometrial primary tumors. They found that that miR-137 is hypermethylated and loses expression in human endometrial tumors. Increasing miR-137 expression suppresses endometrial cancer cell growth in vitro and xenograft tumor growth in nude mice, partly because miR-137 targets EZH2, which participates in histone methylation, and LSD1, a histone demethylation enzyme.
ISSN:0023-6837
1530-0307
DOI:10.1038/s41374-018-0092-x