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Time resolved Gene Expression Analysis during Tamoxifen adaption of MCF-7 cells identifies long non-coding RNAs with prognostic Impact

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Taylor & Francis Group2024-02-20 更新2026-04-16 收录
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https://tandf.figshare.com/articles/dataset/Time_resolved_Gene_Expression_Analysis_during_Tamoxifen_adaption_of_MCF-7_cells_identifies_long_non-coding_RNAs_with_prognostic_Impact/7717820/1
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Acquired tamoxifen resistance is a persistent problem for the treatment of estrogen receptor positive, premenopausal breast cancer patients and predictive biomarkers are still elusive. We here analyzed gene expression changes in a cellular model to identify early and late changes upon tamoxifen exposure and thereby novel prognostic biomarkers. Estrogen receptor positive MCF-7 cells were incubated with 4OH-tamoxifen (10 nM) and gene expression analyzed by array hybridization during 12 weeks. Array results were confirmed by nCounter- and qRT-PCR technique. Pathway enrichment analysis revealed that early responses concerned mainly amine synthesis and NRF2-related signaling and evolved into a stable gene expression pattern within 4 weeks characterized by changes in glucuronidation-, estrogen metabolism-, nuclear receptor- and interferon signaling pathways. As a large number of long non coding RNAs was subject to regulation, we investigated 5 of these (linc01213, linc00632 linc0992, LOC101929547 and XR_133213) in more detail. From these, only linc01213 was upregulated but all were less abundant in estrogen-receptor negative cell lines (MDA-MB 231, SKBR-3 and UACC3199). In a web-based survival analysis linc01213 and linc00632 turned out to have prognostic impact. Linc01213 was investigated further by plasmid-mediated over-expression as well as siRNA down-regulation in MCF-7 cells. Nevertheless, this had no effect on proliferation or expression of tamoxifen regulated genes, but migration was increased. In conclusion, the cellular model identified a set of lincRNAs with prognostic relevance for breast cancer. One of these, linc01213 although regulated by 4OH-tamoxifen, is not a central regulator of tamoxifen adaption, but interferes with the regulation of migration.
提供机构:
Porsch, Martin; Hoffmann, Katrin; Kalinski, Thomas; Haybaeck, Johannes; Bull, Fabian; Özdemir, Esra; Nass, Norbert; Graf, Sebastian; Ignatov, Atanas; Große, Ivo; Wisniewski, Martin
创建时间:
2019-02-14
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