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From the Cover: NS3 helicase actively separates RNA strands and senses sequence barriers ahead of the opening fork

机译:从封面:NS3解旋酶可主动分离RNA链并在分叉前感知序列障碍

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摘要

RNA helicases regulate virtually all RNA-dependent cellular processes. Although much is known about helicase structures, very little is known about how they deal with barriers in RNA and the factors that affect their processivity. The hepatitis C virus encodes NS3, an RNA helicase that is essential for viral RNA replication. We have used optical tweezers to determine at the single-molecule level how the local stability of the RNA substrate affects the enzyme rate of strand separation, whether separation occurs by an active or a passive mechanism, and whether processivity is affected. We show that sequence barriers in RNA modulate NS3 activity. NS3 processivity depends on barriers ahead of the opening fork. Our results rule out a model where NS3 passively waits for the thermal fraying of double-stranded RNA. Instead, we find that NS3 destabilizes the duplex before separating the strands. Failure to do so before a strong barrier leads to helicase dissociation and limits the processivity of the enzyme.
机译:RNA解旋酶实际上调节所有依赖RNA的细胞过程。尽管对解旋酶结构了解很多,但对它们如何处理RNA屏障以及影响其合成能力的因素知之甚少。丙型肝炎病毒编码NS3,这是一种RNA解旋酶,对于病毒RNA复制至关重要。我们已经使用光镊来确定单分子水平上RNA底物的局部稳定性如何影响链分离的酶速率,分离是通过主动还是被动机制进行,以及是否影响了合成能力。我们表明RNA中的序列障碍调节NS3活性。 NS3的合成能力取决于分叉前的障碍。我们的结果排除了NS3被动等待双链RNA热磨损的模型。相反,我们发现NS3在分离链之前会破坏双链体的稳定性。在强屏障之前未这样做会导致解旋酶解离并限制了酶的合成能力。

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