Please use this identifier to cite or link to this item: http://hdl.handle.net/2445/126414
Title: Genome-wide tracking of unmethylated DNA Alu repeats in normal and cancer cells
Author: Rodríguez Lumbiarres, Jairo
Vives, Laura
Jordà Ramos, Mireia
Morales, Cristina
Muñoz, Mar
Vendrell i Soler, Elisenda
Peinado Morales, Miguel Á. (Miguel Ángel)
Keywords: Càncer
Genòmica
Cancer
Genomics
Issue Date: Feb-2008
Publisher: Oxford University Press
Abstract: Methylation of the cytosine is the most frequent epigenetic modification of DNA in mammalian cells. In humans, most of the methylated cytosines are found in CpG-rich sequences within tandem and interspersed repeats that make up to 45 of the human genome, being Alu repeats the most common family. Demethylation of Alu elements occurs in aging and cancer processes and has been associated with gene reactivation and genomic instability. By targeting the unmethylated SmaI site within the Alu sequence as a surrogate marker, we have quantified and identified unmethylated Alu elements on the genomic scale. Normal colon epithelial cells contain in average 25486 +/- 10157 unmethylated Alus per haploid genome, while in tumor cells this figure is 41 995 +/- 17187 (P 0.004). There is an inverse relationship in Alu families with respect to their age and methylation status: the youngest elements exhibit the highest prevalence of the SmaI site (AluY: 42; AluS: 18, AluJ: 5) but the lower rates of unmethylation (AluY: 1.65%; AluS: 3.1%, AluJ: 12%). Data are consistent with a stronger silencing pressure on the youngest repetitive elements, which are closer to genes. Further insights into the functional implications of atypical unmethylation states in Alu elements will surely contribute to decipher genomic organization and gene regulation in complex organisms.
Note: Reproducció del document publicat a: https://doi.org/10.1093/nar/gkm1105
It is part of: Nucleic Acids Research, 2008, vol. 36, num. 3, p. 770-784
URI: http://hdl.handle.net/2445/126414
Related resource: https://doi.org/10.1093/nar/gkm1105
Appears in Collections:Articles publicats en revistes (Institut d'lnvestigació Biomèdica de Bellvitge (IDIBELL))

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