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Oncogenic lncRNA transgene transcription modulates epigenetic memory at a naïve chromosomal locus

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Taylor & Francis Group2025-12-12 更新2026-04-16 收录
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https://tandf.figshare.com/articles/dataset/Oncogenic_lncRNA_transgene_transcription_modulates_epigenetic_memory_at_a_na_ve_chromosomal_locus/29756938/1
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Maintaining genome integrity is essential for the proper functioning and development of organisms. An intriguing aspect is that neocentromeres can form at non-centromeric sites. CENP-A, a key epigenetic marker of centromeres, is often mislocalized to ectopic sites in cancers when overexpressed. Its deposition on centromeres relies on transcription of centromeric non-coding RNAs. Subsequently, ectopic CENP-A is frequently found at transcriptionally active and chromosome breakpoint regions. We previously engineered a stable ectopic CENP-A site on a naïve chromosome by overexpressing PCAT2, a non-centromeric oncogenic lncRNA that recruits CENP-A to its transcribing locus. We tracked cells with this transgene to analyze the longevity of ectopic CENP-A. We discovered that this induced epigenetic memory was lost due to suppression by epigenetic silencing mechanisms, restoring CENP-A to previous levels. These findings suggest that cells have mechanisms to prevent neocentromere formation at ectopic sites by suppressing transcription unless selective pressure favors it
提供机构:
Dalal, Yamini; Sikder, Sweta; Arunkumar, Ganesan; Baek, Songjoon
创建时间:
2025-08-01
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