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The influence of a metastable structure in plasmid primer RNA on antisense RNA binding kinetics.

机译:质粒引物RNA中的亚稳结构对反义RNA结合动力学的影响。

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摘要

Replication of the ColE1 group plasmids is kinetically regulated by the interaction between plasmid-encoded primer RNA II and antisense RNA I. The binding is dependent on alternative RNA II conformations, formed during the transcription, and effectively inhibits the primer function within some time interval. In this paper, the folding pathways for the wild type and copy number mutants of ColE1 RNA II are studied using simulations by a genetic algorithm. The simulated pathways reveal a transient formation of a metastable structure, which is stabilized by copy number mutations. The folding kinetics of the proposed conformational transitions is calculated using a model of a multistep refolding process with elementary steps of double-helical stem formation or disruption. The approximation shows that the lifetime of the metastable structure is relatively long and is considerably increased in the mutants, resulting in a delay of the formation of the stable RNA II structure, which is the most sensitive to the inhibition by the antisense RNA I. Thus the effect of copy number mutations can be interpreted as a compression of the time window of effective inhibition due to an increased time spent by the RNA II in the metastable state. The implications of metastable foldings in RNA functioning are discussed.
机译:ColE1组质粒的复制受到质粒编码引物RNA II和反义RNA I之间相互作用的动力学调控。结合依赖于转录过程中形成的其他RNA II构象,并在一定时间间隔内有效抑制了引物功能。在本文中,使用遗传算法通过模拟研究了ColE1 RNA II的野生型和拷贝数突变体的折叠途径。模拟的途径揭示了亚稳态结构的瞬时形成,其通过拷贝数突变得以稳定。拟议的构象转变的折叠动力学是使用具有双螺旋茎形成或破坏的基本步骤的多步重折叠过程的模型来计算的。近似表明,亚稳结构的寿命相对较长,并且在突变体中显着增加,从而导致稳定的RNA II结构的形成延迟,该结构对反义RNA I的抑制作用最为敏感。拷贝数突变的影响可以解释为有效抑制时间窗口的压缩,这是由于处于亚稳状态的RNA II花费的时间增加了。讨论了亚稳态折叠对RNA功能的影响。

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