4.8 Article

Quantitative analysis of associations between DNA hypermethylation, hypomethylation, and DNMT RNA levels in ovarian tumors

Journal

ONCOGENE
Volume 25, Issue 18, Pages 2636-2645

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/sj.onc.1209145

Keywords

DNA hypomethylation; DNA hypermethylation; DNA methyltransferases; ovarian tumors

Funding

  1. NCI NIH HHS [R01 CA081506, P01CA46589, P01 CA70972, CA81506, R01 CA096958, CA96958, P01 CA070972] Funding Source: Medline

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How hypermethylation and hypomethylation of different parts of the genome in cancer are related to each other and to DNA methyltransferase ( DNMT) gene expression is ill defined. We used ovarian epithelial tumors of different malignant potential to look for associations between 5'-gene region or promoter hypermethylation, satellite, or global DNA hypomethylation, and RNA levels for ten DNMT isoforms. In the quantitative MethyLight assay, six of the 55 examined gene loci ( LTB4R, MTHFR, CDH13, PGR, CDH1, and IGSF4) were significantly hypermethylated relative to the degree of malignancy ( after adjustment for multiple comparisons; P < 0.001). Importantly, hypermethylation of these genes was associated with degree of malignancy independently of the association of satellite or global DNA hypomethylation with degree of malignancy. Cancer-related increases in methylation of only two studied genes, LTB4R and MTHFR, which were appreciably methylated even in control tissues, were associated with DNMT1 RNA levels. Cancer-linked satellite DNA hypomethylation was independent of RNA levels for all DNMT3B isoforms, despite the ICF syndrome-linked DNMT3B deficiency causing juxtacentromeric satellite DNA hypomethylation. Our results suggest that there is not a simple association of gene hypermethylation in cancer with altered DNMT RNA levels, and that this hypermethylation is neither the result nor the cause of satellite and global DNA hypomethylation.

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