Novel markers of gene methylation and expression in breast cancer

Autor:	T. V. Kekeeva, Vladimir V Strelnikov, Ekaterina B. Kuznetsova, Marina V. Nemtsova, Larin Ss, D. V. Zaletayev, V. V. Zemlyakova, O. V. Babenko
Rok vydání:	2007
Předmět:	Bisulfite sequencing Biophysics Methylation Biology medicine.disease Molecular biology Breast cancer Differentially methylated regions CpG site Structural Biology DNA methylation medicine Cancer research Illumina Methylation Assay Epigenetics
Zdroj:	Molecular Biology. 41:562-570
ISSN:	1608-3245 0026-8933
Popis:	An optimized methylation-sensitive restriction fingerprinting technique was used to search for differentially methylated CpG islands in the tumor genome and detected seven genes subject to abnormal epigenetic regulation in breast cancer: SEMA6B, BIN1, VCPIP1, LAMC3, KCNH2, CACNG4, and PSMF1. For each gene, the rate of promoter methylation and changes in expression were estimated in tumor and morphologically intact paired specimens of breast tissue (N = 100). Significant methylation rates of 38, 18, and 8% were found for SEMA6B, BIN1, and LAMC3, respectively. The genes were not methylated in morphologically intact breast tissue. The expression of SEMA6B, BIN1, VCPIP1, LAMC3, KCNH2, CACNG4, and PSMF1 was decreased in 44–94% of tumor specimens by the real-time RT-PCR assay. The most profound changes in SEMA6B and LAMC3 suggest that these genes can be included in biomarker panels for breast cancer diagnosis. Fine methylation mapping of the most frequently methylated CpG islands (SEMA6B, BIN1, and LAMC3) provides a fundamental basis for developing efficient methylation tests for these genes.
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=doi_________::bfd41827eb3b7e9b3cb01b4b60583bb6 https://doi.org/10.1134/s0026893307040061 Zobrazit plný text záznamu Full text from SpringerLink