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Maximizing RNA folding rates: a balancing act.

机译:最大化RNA折叠率:一种平衡行为。

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Large ribozymes typically require very long times to refold into their active conformation in vitro, because the RNA is easily trapped in metastable misfolded structures. Theoretical models show that the probability of misfolding is reduced when local and long-range interactions in the RNA are balanced. Using the folding kinetics of the Tetrahymena ribozyme as an example, we propose that folding rates are maximized when the free energies of forming independent domains are similar to each other. A prediction is that the folding pathway of the ribozyme can be reversed by inverting the relative stability of the tertiary domains. This result suggests strategies for optimizing ribozyme sequences for therapeutics and structural studies.
机译:大的核酶通常需要很长时间才能在体外重折叠成其活性构象,因为RNA容易被困在亚稳错折叠的结构中。理论模型表明,当RNA中的局部和远程相互作用平衡时,错误折叠的可能性会降低。以四膜虫核酶的折叠动力学为例,我们提出当形成独立结构域的自由能彼此相似时,折叠速率最大。可以预测,通过反转第三域的相对稳定性,可以逆转核酶的折叠途径。该结果提出了优化用于治疗和结构研究的核酶序列的策略。

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