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体内上游DNA对动态超螺旋的功能反应。

The functional response of upstream DNA to dynamic supercoiling in vivo.

作者信息

Kouzine Fedor, Sanford Suzanne, Elisha-Feil Zichrini, Levens David

机构信息

Laboratory of Pathology, National Cancer Institute, 10 Center Drive, Building 10, Room 2N106, Bethesda, Maryland 20892-1500, USA.

出版信息

Nat Struct Mol Biol. 2008 Feb;15(2):146-54. doi: 10.1038/nsmb.1372. Epub 2008 Jan 13.

Abstract

Because RNA polymerase is a powerful motor, transmission of transcription-generated forces might directly alter DNA structure, chromatin or gene activity in mammalian cells. Here we show that transcription-generated supercoils streaming dynamically from active promoters have considerable consequences for DNA structure and function in cells. Using a tamoxifen-activatable Cre recombinase to excise a test segment of chromatin positioned between divergently transcribed metallothionein-IIa promoters, we found the degree of dynamic supercoiling to increase as transcription intensified, and it was very sensitive to the specific arrangement of promoters and cis elements. Using psoralen as an in vivo probe confirmed that, during transcription, sufficient supercoiling is produced to enable transitions to conformations other than B-DNA in elements such as the human MYC far upstream element (FUSE), which in turn recruit structure-sensitive regulatory proteins, such as FUSE Binding Protein (FBP) and FBP-Interacting Repressor (FIR). These results indicate that mechanical stresses, constrained by architectural features of DNA and chromatin, may broadly contribute to gene regulation.

摘要

由于RNA聚合酶是一种强大的分子马达,转录产生的力的传递可能会直接改变哺乳动物细胞中的DNA结构、染色质或基因活性。在此,我们表明,从活跃启动子动态流出的转录产生的超螺旋对细胞中的DNA结构和功能具有相当大的影响。使用他莫昔芬可激活的Cre重组酶切除位于反向转录的金属硫蛋白-IIa启动子之间的染色质测试片段,我们发现随着转录增强,动态超螺旋程度增加,并且它对启动子和顺式元件的特定排列非常敏感。使用补骨脂素作为体内探针证实,在转录过程中,会产生足够的超螺旋,以使诸如人类MYC远上游元件(FUSE)等元件转变为除B-DNA之外的构象,进而招募结构敏感的调节蛋白,如FUSE结合蛋白(FBP)和FBP相互作用阻遏物(FIR)。这些结果表明,受DNA和染色质结构特征限制的机械应力可能广泛参与基因调控。

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