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组蛋白与猿猴病毒40增强子区域在体外的序列特异性相互作用。

Sequence-specific interaction of histones with the simian virus 40 enhancer region in vitro.

作者信息

Clarke M F, FitzGerald P C, Brubaker J M, Simpson R T

出版信息

J Biol Chem. 1985 Oct 15;260(23):12394-7.

PMID:2995375
Abstract

DNA fragments containing either one or both of the 72-base pair (bp) elements which constitute the SV40 enhancer and the three adjacent 21-bp repeats were associated with histone octomers from chicken erythrocytes in vitro. Both fragments formed complexes with electrophoretic mobilities of nucleosomes containing the appropriate length of DNA. Analysis of DNase I cutting of uniquely end-labeled complexes suggests that the fragment containing a single 72-bp element forms a positioned core particle. Control experiments show that positioning is not due to the 21-bp repeats or to end effects. The fragment with a tandem repeat of the 72-bp element also does not associate randomly with histones. The data are consistent with formation of a core particle on one or the other of the repeated enhancer sequences. We discuss possible functional consequences of such nucleosome positioning.

摘要

含有构成SV40增强子的72碱基对(bp)元件中的一个或两个以及三个相邻的21 bp重复序列的DNA片段,在体外与鸡红细胞中的组蛋白八聚体相关联。两个片段都形成了具有适当长度DNA的核小体电泳迁移率的复合物。对唯一末端标记复合物的DNase I切割分析表明,含有单个72 bp元件的片段形成了定位的核心颗粒。对照实验表明,定位不是由于21 bp重复序列或末端效应。具有72 bp元件串联重复的片段也不会与组蛋白随机结合。数据与在重复的增强子序列中的一个或另一个上形成核心颗粒一致。我们讨论了这种核小体定位可能的功能后果。

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