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StpA and Hha stimulate pausing by RNA polymerase by promoting DNA-DNA bridging of H-NS filaments

机译:STPA和HHA通过促进H-NS长丝的DNA-DNA桥接来刺激RNA聚合酶

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In enterobacteria, AT-rich horizontally acquired genes, including virulence genes, are silenced through the actions of at least three nucleoid-associated proteins (NAPs): H-NS, StpA and Hha. These proteins form gene-silencing nucleoprotein filaments through direct DNA binding by H-NS and StpA homodimers or heterodimers. Both linear and bridged filaments, in which NAPs bind one or two DNA segments, respectively, have been observed. Hha can interact with H-NS or StpA filaments, but itself lacks a DNA-binding domain. Filaments composed of H-NS alone can inhibit transcription initiation and, in the bridged conformation, slow elongating RNA polymerase (RNAP) by promoting backtracking at pause sites. How the other NAPs modulate these effects of H-NS is unknown, despite evidence that they help regulate subsets of silenced genes in vivo (e.g. in pathogenicity islands). Here we report that Hha and StpA greatly enhance H-NS-stimulated pausing by RNAP at 20 degrees C. StpA: H-NS or StpA-only filaments also stimulate pausing at 37 degrees C, a temperature at which Hha: H-NS or H-NS-only filaments have much less effect. In addition, we report that both Hha and StpA greatly stimulate DNA-DNA bridging by H-NS filaments. Together, these observations indicate that Hha and StpA can affect H-NS-mediated gene regulation by stimulating bridging of H-NS/DNA filaments.
机译:在细菌中,通过至少三种核性相关蛋白(小睡):H-NS,STPA和HHA的作用,富含富含毒力基因的水平获得的基因,包括毒力基因,包括毒力基因。这些蛋白质通过通过H-NS和STPA同源过二聚体或异二聚体直接DNA结合来形成基因沉默的核蛋白长丝。已经观察到分别点线和桥接细丝,其中分别没有结合一种或两个DNA段。 HHA可以与H-NS或STPA长丝相互作用,但本身缺乏DNA结合结构域。单独由H-NS组成的长丝可以通过促进暂停位点促进反向特性,促进转录起始,并且在桥接构象中,慢伸长RNA聚合酶(RNAP)。尽管有证据表明它们有助于调节体内沉默基因的亚群(例如,在致病性岛屿中),但其他疏水部门如何调节这些H-NS的效果。在这里,我们报告HHA和STPA在20摄氏度下,HHA和STPA大大提高了HHA和刺激的暂停,STPA:H-NS或STPA的长丝也刺激37℃,HHA:H-NS或HHA的温度H-NS-oply丝的效果少得多。此外,我们报告说,HHA和STPA都大大刺激了H-NS长丝的DNA-DNA桥接。这些观察结果表明,HHA和STPA可以通过刺激H-NS / DNA长丝的桥接来影响H-NS介导的基因调节。

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