Data of transcriptional effects of the merbarone-mediated inhibition of TOP2

Fernando M Delgado-Chaves; Pedro Manuel Martínez-García; Andrés Herrero-Ruiz; Francisco Gómez-Vela; Federico Divina; Silvia Jimeno-González; Felipe Cortés-Ledesma

doi:10.1016/j.dib.2022.108499

Data of transcriptional effects of the merbarone-mediated inhibition of TOP2

Data Brief. 2022 Aug 1:44:108499. doi: 10.1016/j.dib.2022.108499. eCollection 2022 Oct.

Authors

Fernando M Delgado-Chaves¹, Pedro Manuel Martínez-García², Andrés Herrero-Ruiz^{2

3}, Francisco Gómez-Vela¹, Federico Divina¹, Silvia Jimeno-González², Felipe Cortés-Ledesma³

Affiliations

¹ Division of Computer Science, Pablo de Olavide University, Seville ES-41013, Spain.
² Andalusian Molecular Biology and Regenerative Medicine Center (CABIMER), University of Seville - CSIC - Pablo de Olavide University, Seville ES-41092 Spain.
³ Topology and DNA breaks Group, Spanish National Cancer Research Center (CNIO), Madrid ES-28029, Spain.

Abstract

Type II DNA topoisomerases relax topological stress by transiently gating DNA passage in a controlled cut-and-reseal mechanism that affects both DNA strands. Therefore, they are essential to overcome topological problems associated with DNA metabolism. Their aberrant activity results in the generation of DNA double-strand breaks, which can seriously compromise cell survival and genome integrity. Here, we profile the transcriptome of human-telomerase-immortalized retinal pigment epithelial 1 (RPE-1) cells when treated with merbarone, a drug that catalytically inhibits type II DNA topoisomerases. We performed RNA-Seq after 4 and 8 h of merbarone treatment and compared transcriptional profiles versus untreated samples. We report raw sequencing data together with lists of gene counts and differentially expressed genes.

Keywords: DNA supercoiling; Differential gene expression; Merbarone; RNA-Seq; Topoisomerase inhibition.