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工程化核糖开关的机制见解:赋予核糖开关活性的开关元件。

Mechanistic insights into an engineered riboswitch: a switching element which confers riboswitch activity.

机构信息

RNA Biochemistry, Johann Wolfgang Goethe-University Frankfurt, Max-von-Laue-Str. 9, D-60438 Frankfurt/M, Germany.

出版信息

Nucleic Acids Res. 2011 Apr;39(8):3363-72. doi: 10.1093/nar/gkq946. Epub 2010 Dec 11.

Abstract

While many different RNA aptamers have been identified that bind to a plethora of small molecules only very few are capable of acting as engineered riboswitches. Even for aptamers binding the same ligand large differences in their regulatory potential were observed. We address here the molecular basis for these differences by using a set of unrelated neomycin-binding aptamers. UV melting analyses showed that regulating aptamers are thermally stabilized to a significantly higher degree upon ligand binding than inactive ones. Regulating aptamers show high ligand-binding affinity in the low nanomolar range which is necessary but not sufficient for regulation. NMR data showed that a destabilized, open ground state accompanied by extensive structural changes upon ligand binding is important for regulation. In contrast, inactive aptamers are already pre-formed in the absence of the ligand. By a combination of genetic, biochemical and structural analyses, we identified a switching element responsible for destabilizing the ligand free state without compromising the bound form. Our results explain for the first time the molecular mechanism of an engineered riboswitch.

摘要

虽然已经鉴定出许多与大量小分子结合的不同 RNA 适体,但只有极少数能够作为工程化的核酶发挥作用。即使对于结合相同配体的适体,它们的调节潜力也存在很大差异。我们通过一组不相关的新霉素结合适体来解决这些差异的分子基础。UV 融解分析表明,与无活性的适体相比,调节适体在配体结合时的热稳定性显著提高。调节适体表现出高的配体结合亲和力,在低纳摩尔范围内,这是必需的,但不足以进行调节。NMR 数据表明,在配体结合时,不稳定的、开放的起始状态伴随着广泛的结构变化对于调节是重要的。相比之下,无活性的适体在没有配体的情况下已经预先形成。通过遗传、生化和结构分析的结合,我们确定了一个开关元件,负责在不损害结合形式的情况下使无配体自由状态失稳。我们的结果首次解释了工程核酶的分子机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/412f/3082870/77cad71a63fc/gkq946f1.jpg

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