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Structural insight into the mechanism of stabilization of the 7SK small nuclear RNA by LARP7

机译:LARP7对7SK小核RNA稳定机制的结构见解

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The non-coding RNA 7SK is the scaffold for a small nuclear ribonucleoprotein (7SKsnRNP) which regulates the function of the positive transcription elongation factor P-TEFb in the control of RNA polymerase II elongation in metazoans. The La-related protein LARP7 is a component of the 7SKsnRNP required for stability and function of the RNA. To address the function of LARP7 we determined the crystal structure of its La module, which binds a stretch of uridines at the 3'-end of 7SK. The structure shows that the penultimate uridine is tethered by the two domains, the La-motif and the RNA-recognition motif (RRM1), and reveals that the RRM1 is significantly smaller and more exposed than in the La protein. Sequence analysis suggests that this impacts interaction with 7SK. Binding assays, footprinting and small-angle scattering experiments show that a second RRM domain located at the C-terminus binds the apical loop of the 3' hairpin of 7SK, while the N-terminal domains bind at its foot. Our results suggest that LARP7 uses both its N- and C-terminal domains to stabilize 7SK in a closed structure, which forms by joining conserved sequences at the 5'-end with the foot of the 3' hairpin and has thus functional implications.
机译:非编码RNA 7SK是小核糖核糖核蛋白(7SKsnRNP)的支架,它调节阳性转录延伸因子P-TEFb在后生动物中控制RNA聚合酶II延伸的功能。 La相关蛋白LARP7是7SKsnRNP的组成部分,是RNA稳定性和功能所必需的。为了解决LARP7的功能,我们确定了其La模块的晶体结构,该模块在7SK的3'末端结合了一段尿苷。该结构显示倒数第二个尿苷由La-基序和RNA识别基序(RRM1​​)这两个域束缚,并显示RRM1比La蛋白中的小得多,并且暴露得多。序列分析表明,这会影响与7SK的相互作用。结合测定,足迹和小角度散射实验表明,位于C末端的第二个RRM结构域与7SK 3'发夹的顶端环结合,而N末端结构域在其脚部结合。我们的结果表明,LARP7使用其N和C端结构域将7SK稳定在一个封闭的结构中,该结构通过将5'端的保守序列与3'发夹的脚连接起来而形成,因此具有功能意义。

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