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In vitro selections with RNAs of variable length converge on a robust catalytic core

机译:在鲁棒催化芯上具有可变长度的RNA的体外选择

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摘要

In vitro selection is a powerful tool that can be used to understand basic principles of molecular evolution. We used in vitro selection to understand how changes in length and the accumulation of point mutations enable the evolution of functional RNAs. Using RNA populations of various lengths, we performed a series of in vitro experiments to select for ribozymes with RNA ligase activity. We identified a core ribozyme structure that was robust to changes in RNA length, high levels of mutagenesis, and increased selection pressure. Elaboration on this core structure resulted in improved activity which we show is consistent with a larger trend among functional RNAs in which increasing motif size can lead to an exponential improvement in fitness. We conclude that elaboration on conserved core structures is a preferred mechanism in RNA evolution. This conclusion, drawn from selections of RNAs from random sequences, is consistent with proposed evolutionary histories of specific biological RNAs. More generally, our results indicate that modern RNA structures can be used to infer ancestral structures. Our observations also suggest a mechanism by which structural outcomes of early RNA evolution would be largely reproducible even though RNA fitness landscapes consist of disconnected clusters of functional sequences.
机译:体外选择是一种强大的工具,可用于了解分子演化的基本原则。我们使用体外选择来了解点突变的长度和积累的变化能够实现功能性RNA的演变。使用各种长度的RNA群体,我们进行了一系列体外实验,以选择具有RNA连接酶活性的核酶。我们鉴定了一种核苷核酶结构,其变化RNA长度,诱变水平高,以及增加的选择压力。在这种核心结构上的阐述导致我们展示的改善的活动与功能RNA的更大趋势一致,其中越来越多的图案尺寸可能导致适合度的指数改善。我们得出结论,保守核心结构的阐述是RNA进化中的优选机制。从来自随机序列的RNA的选择中得出的结论是与特定生物RNA的提出的进化历史一致的。更一般地,我们的结果表明,现代RNA结构可用于推断祖先结构。我们的观察结果还提出了一种机制,即使RNA适合景观包括断开的功能序列簇,即使具有断开连接的功能序列的簇,早期RNA演化的结构结果将主要是可重复的。

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