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Using droplet-based microfluidics to improve the catalytic properties of RNA under multiple-turnover conditions

机译:使用基于液滴的微流控技术改善多周转条件下RNA的催化性能

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In vitro evolution methodologies are powerful approaches to identify RNA with new functionalities. While Systematic Evolution of Ligands by Exponential enrichment (SELEX) is an efficient approach to generate new RNA aptamers, it is less suited for the isolation of efficient ribozymes as it does not select directly for the catalysis. In vitro compartmentalization (IVC) in aqueous droplets in emulsions allows catalytic RNAs to be selected under multiple-turnover conditions but suffers severe limitations that can be overcome using the droplet-based microfluidics workflow described in this paper. Using microfluidics, millions of genes in a library can be individually compartmentalized in highly monodisperse aqueous droplets and serial operations performed on them. This allows the different steps of the evolution process (gene amplification, transcription, and phenotypic assay) to be uncoupled, making the method highly flexible, applicable to the selection and evolution of a variety of RNAs, and easily adaptable for evolution of DNA or proteins. To demonstrate the method, we performed cycles of random mutagenesis and selection to evolve the X-motif, a ribozyme which, like many ribozymes selected using SELEX, has limited multiple-turnover activity. This led to the selection of variants, likely to be the optimal ribozymes that can be generated using point mutagenesis alone, with a turnover number under multiple-turnover conditions, k(cat)(ss), similar to 28-fold higher than the original X-motif, primarily due to an increase in the rate of product release, the rate-limiting step in the multiple-turnover reaction.
机译:体外进化方法学是鉴定具有新功能的RNA的有力方法。虽然通过指数富集进行配体的系统进化(SELEX)是生成新RNA适体的有效方法,但由于它不能直接选择进行催化,因此不太适合分离有效的核酶。乳液中的水滴中的体外区室化(IVC)允许在多周转条件下选择催化性RNA,但存在严重的局限性,可以使用本文所述的基于液滴的微流技术克服这一局限。使用微流体技术,可以将文库中的数百万个基因分别分隔在高度单分散的水滴中,并对其进行串行操作。这使得进化过程的不同步骤(基因扩增,转录和表型分析)可以解偶联,从而使该方法具有高度的灵活性,适用于多种RNA的选择和进化,并且易于适应DNA或蛋白质的进化。为了证明该方法,我们进行了随机诱变和选择的循环,以进化出X-基序(一种核酶,与使用SELEX选择的许多核酶一样,其多次转换活动受到限制)。这导致选择变体,可能是仅使用点诱变就可以产生的最佳核酶,其在多周转条件下的周转数k(cat)(ss),比原来高28倍。 X-基序,主要是由于产物释放速率的增加,这是多周转反应中的限速步骤。

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