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Insights into the mechanism of a G-quadruplex-unwinding DEAH-box helicase

机译:对解开G-四链体DEAH-box解旋酶的机制的见解

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The unwinding of nucleic acid secondary structures within cells is crucial to maintain genomic integrity and prevent abortive transcription and translation initiation. DHX36, also known as RHAU or G4R1, is a DEAH-box ATP-dependent helicase highly specific for DNA and RNA G-quadruplexes (G4s). A fundamental mechanistic understanding of the interaction between helicases and their G4 substrates is important to elucidate G4 biology and pave the way toward G4-targeted therapies. Here we analyze how the thermodynamic stability of G4 substrates affects binding and unwinding by DHX36. We modulated the stability of the G4 substrates by varying the sequence and the number of G-tetrads and by using small, G4stabilizing molecules. We found an inverse correlation between the thermodynamic stability of the G4 substrates and rates of unwinding by DHX36. In stark contrast, the ATPase activity of the helicase was largely independent of substrate stability pointing toward a decoupling mechanism akin to what has been observed for many double-stranded DEAD-box RNA helicases. Our study provides the first evidence that DHX36 uses a local, non-processive mechanism to unwind G4 substrates, reminiscent of that of eukaryotic initiation factor 4A (eIF4A) on double-stranded substrates.
机译:细胞内核酸二级结构的展开对于维持基因组完整性并防止流产的转录和翻译启动至关重要。 DHX36,也称为RHAU或G4R1,是一种对DNA和RNA G四联体(G4s)具有高度特异性的DEAH-box ATP依赖性解旋酶。对解旋酶及其G4底物之间相互作用的基本机理的理解对于阐明G4生物学和为靶向G4的疗法铺平道路非常重要。在这里,我们分析了G4底物的热力学稳定性如何影响DHX36的结合和展开。我们通过改变G-四联体的序列和数量以及使用小的G4稳定分子来调节G4底物的稳定性。我们发现G4底物的热力学稳定性与DHX36展开速度之间呈反比关系。与之形成鲜明对比的是,解旋酶的ATPase活性在很大程度上与底物稳定性无关,指向类似于许多双链DEAD-box RNA解旋酶观察到的解耦机制。我们的研究提供了第一个证据,表明DHX36使用局部非加工性机制解开G4底物,让人联想到双链底物上的真核生物起始因子4A(eIF4A)。

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