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- Title
Hypermethylation in Ovarian Cancer of Long Noncoding RNA Genes: HOTAIR, GAS5, LINC00472, LINC00886, TUG1.
- Authors
Burdennyy, A. M.; Lukina, S. S.; Uroshlev, L. A.; Filippova, E. A.; Pronina, I. V.; Fridman, M. V.; Zhordaniya, K. I.; Kazubskaya, T. P.; Kushlinskii, N. E.; Loginov, V. I.; Braga, E. A.
- Abstract
Recently, more and more data have been accumulating indicating the role of long noncoding RNAs (lncRNAs) in the regulation of biological processes in cells, as well as in the mechanisms of cancer development and progression. Aberrant methylation of promoter regions of both protein genes and lncRNA genes can disrupt their expression and functional activity. Using bioinformatics databases, six lncRNA genes (GAS5, HOTAIR, LINC00472, LINC00886, SNHG17, and TUG1) with CpG islands differentially expressed and presumably hypermethylated in tumors of patients with ovarian cancer (OC) were selected. Using a sample of 93 OC samples, real-time methylation specific PCR showed a statistically significant (p < 0.05) increase in the level of methylation in tumors. Moreover, for the genes LINC00472, LINC00886, SNHG17, and TUG1, hypermethylation in OC was detected for the first time. Five genes (except SNHG17) showed a further increase in methylation levels at a more advanced stage, and four genes (except SNHG17 and LINC00886) showed a significant association with metastasis. Using real-time RT-PCR, differential changes in the expression level of the GAS5, HOTAIR, SNHG17, and TUG1 genes and a significant correlation of methylation with expression for the GAS5 gene were shown. Thus, hypermethylation associated with the progression and/or development of OC was detected for six lncRNA genes, which is important for elucidating the epigenetic processes involved in the pathogenesis of OC and can be used as new biomarkers of OC.
- Subjects
GROWTH arrest-specific 5; LINCRNA; OVARIAN cancer; P16 gene; GENE expression; GENES; PROMOTERS (Genetics)
- Publication
Russian Journal of Genetics, 2024, Vol 60, Issue 5, p665
- ISSN
1022-7954
- Publication type
Article
- DOI
10.1134/S1022795424700029