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异染色质对LCR介导的基因转录频率和持续时间的影响。

Heterochromatin effects on the frequency and duration of LCR-mediated gene transcription.

作者信息

Milot E, Strouboulis J, Trimborn T, Wijgerde M, de Boer E, Langeveld A, Tan-Un K, Vergeer W, Yannoutsos N, Grosveld F, Fraser P

机构信息

Erasmus University, Department of Cell Biology, Rotterdam, The Netherlands.

出版信息

Cell. 1996 Oct 4;87(1):105-14. doi: 10.1016/s0092-8674(00)81327-6.

Abstract

Locus control regions (LCRs) are responsible for initiating and maintaining a stable tissue-specific open chromatin structure of a locus. In transgenic mice, LCRs confer high level expression on linked genes independent of position in the mouse genome. Here we show that an incomplete LCR loses this property when integrated into heterochromatic regions. Two disruption mechanisms were observed. One is classical position-effect variegation, resulting in continuous transcription in a clonal subpopulation of cells. The other is a novel mechanism resulting in intermittent gene transcription in all cells. We conclude that only a complete LCR fully overcomes heterochromatin silencing and that it controls the level of transcription by ensuring activity in all cells at all times rather than directly controlling the rate of transcription.

摘要

基因座控制区(LCRs)负责启动和维持一个基因座稳定的组织特异性开放染色质结构。在转基因小鼠中,LCRs使连锁基因在小鼠基因组中的表达不受位置影响而保持高水平。在此我们表明,一个不完整的LCR整合到异染色质区域时会丧失这一特性。观察到两种破坏机制。一种是经典的位置效应斑驳,导致在细胞的克隆亚群中持续转录。另一种是一种新机制,导致在所有细胞中间歇性基因转录。我们得出结论,只有完整的LCR才能完全克服异染色质沉默,并且它通过确保在所有时间所有细胞中的活性来控制转录水平,而不是直接控制转录速率。

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