首页> 外文OA文献 >G4 Resolvase 1 Binds Both DNA and RNA Tetramolecular Quadruplex with High Affinity and Is the Major Source of Tetramolecular Quadruplex G4-DNA and G4-RNA Resolving Activity in HeLa Cell Lysates*
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G4 Resolvase 1 Binds Both DNA and RNA Tetramolecular Quadruplex with High Affinity and Is the Major Source of Tetramolecular Quadruplex G4-DNA and G4-RNA Resolving Activity in HeLa Cell Lysates*

机译:G4 Resolvase 1结合DNA和RNA的四分子四链体具有很高的 亲和力是四分子四链体G4-DNA和 HeLa细胞中的G4-RNA分解活性 裂解物*

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摘要

Quadruplex structures that result from stacking of guanine quartets in nucleic acids possess such thermodynamic stability that their resolution in vivo is likely to require specific recognition by specialized enzymes. We previously identified the major tetramolecular quadruplex DNA resolving activity in HeLa cell lysates as the gene product of DHX36 (Vaughn, J. P., Creacy, S. D., Routh, E. D., Joyner-Butt, C., Jenkins, G. S., Pauli, S., Nagamine, Y., and Akman, S. A. (2005) J. Biol Chem. 280, 38117–38120), naming the enzyme G4 Resolvase 1 (G4R1). G4R1 is also known as RHAU, an RNA helicase associated with the AU-rich sequence of mRNAs. We now show that G4R1/RHAU binds to and resolves tetramolecular RNA quadruplex as well as tetramolecular DNA quadruplex structures. The apparent Kd values of G4R1/RHAU for tetramolecular RNA quadruplex and tetramolecular DNA quadruplex were exceptionally low: 39 ± 6 and 77 ± 6pm, respectively, as measured by gel mobility shift assay. In competition studies tetramolecular RNA quadruplex structures inhibited tetramolecular DNA quadruplex structure resolution by G4R1/RHAU more efficiently than tetramolecular DNA quadruplex structures inhibited tetramolecular RNA quadruplex structure resolution. Down-regulation of G4R1/RHAU in HeLa T-REx cells by doxycycline-inducible short hairpin RNA caused an 8-fold loss of RNA and DNA tetramolecular quadruplex resolution, consistent with G4R1/RHAU representing the major tetramolecular quadruplex helicase activity for both RNA and DNA structures in HeLa cells. This study demonstrates for the first time the RNA quadruplex resolving enzymatic activity associated with G4R1/RHAU and its exceptional binding affinity, suggesting a potential novel role for G4R1/RHAU in targeting in vivo RNA quadruplex structures.
机译:由鸟嘌呤四联体堆叠在核酸中产生的四链体结构具有如此的热力学稳定性,以至于它们在体内的分解可能需要特殊酶的特异性识别。我们先前在HeLa细胞裂解物中鉴定了主要的四分子四链体DNA解析活性作为DHX36的基因产物(Vaughn,JP,Creacy,SD,Routh,ED,Joyner-Butt,C.,Jenkins,GS,Pauli,S.,Nagamine ,Y。,和Akman,SA(2005)J. Biol Chem。280,38117-38120),将酶命名为G4 Resolvase 1(G4R1)。 G4R1也称为RHAU,一种与富含AU的mRNA序列相关的RNA解旋酶。我们现在显示G4R1 / RHAU结合并解析四分子RNA四链体以及四分子DNA四链体结构。四分子RNA四链体和四分子DNA四链体的G4R1 / RHAU的表观Kd值异常低:分别通过凝胶迁移率移动分析法测得,分别为39±6pm和77±6pm。在竞争研究中,四分子RNA四链体结构通过G4R1 / RHAU抑制四分子DNA四链体结构的分辨率比四分子DNA四链体结构抑制四分子RNA四链体结构的抑制更有效。强力霉素诱导的短发夹RNA对HeLa T-REx细胞中G4R1 / RHAU的下调导致RNA和DNA四分子四链体分辨率下降8倍,这与G4R1 / RHAU代表了主要的四分子四链体解旋酶活性有关HeLa细胞中的DNA结构。这项研究首次证明了解决与G4R1 / RHAU相关的酶促活性的RNA四链体及其异常的结合亲和力,暗示了G4R1 / RHAU在靶向体内RNA四链体结构中的潜在新作用。

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