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Burdennyy, A. M.; Filippova, E. A.; Lukina, S. S.; Ivanova, N. A.; Pronina, I. V.; Loginov, V. I.; Kazubskaya, T. P.; Kushlinskii, N. E.; Braga, E. A.
Bulletin of experimental biology and medicine, 02/2024, Letnik: 176, Številka: 4Journal Article
There are three types of metastases in ovarian cancer: lymphogenous, hematogenous, and peritoneal. Dissemination of the tumor in the peritoneum is directly related with the development of ascites and a poor prognosis. The purpose of this study is to determine changes in the methylation level of a group of long non-coding RNA (lncRNA) genes at different stages of ovarian cancer progression. The methylation level of 7 lncRNA genes ( LINC00472 , LINC00886 , MAFG-DT , SNHG1 , SNHG6 , TP53TG1 , and TUG1 ) was studied by quantitative methyl-specific PCR in 93 samples of ovarian tumors and 75 paired samples of histologically normal tissue, as well as in 29 peritoneal macroscopic metastases. Using the nonparametric Mann—Whitney test, a significant ( p <0.001) increase in the level of methylation of the LINC00886 , SNHG1 , SNHG6 , and TUG1 genes in the tumor tissue was shown. For the LINC00472 , LINC00886 , and SNHG6 genes, a significant relationship was found with the clinical stage ( p ≤0.001), as well as with the appearance of metastases for the LINC00472 ( p <0.001) and SNHG6 ( p =0.005) genes. There was a significant increase in the level of methylation of MAFG-DT and TP53TG1 ( p <0.001) genes, as well as a decrease in LINC00886 ( p =0.003) in peritoneal metastases relative to the primary focus. Methylation of the LINC00472 and SNHG6 genes can be considered as a factor in initiating ovarian cancer metastasis, and methylation of the LINC00886 , MAFG-DT , and TP53TG1 genes as a colonization factor for metastases in the peritoneum. Thus, a relationship between methylation of a group of lncRNA genes at different stages of ovarian cancer dissemination was shown, which is important for understanding the mechanisms of these processes and for developing innovative approaches to ovarian cancer therapy.
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JCR | SNIP | JCR | SNIP | JCR | SNIP | JCR | SNIP |
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