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一种从包含阳离子功能的RNA文库中筛选出的新型、依赖修饰的ATP结合适体。

A novel, modification-dependent ATP-binding aptamer selected from an RNA library incorporating a cationic functionality.

作者信息

Vaish Narendra K, Larralde Rosa, Fraley Andrew W, Szostak Jack W, McLaughlin Larry W

机构信息

Department of Chemistry, Boston College, 140 Commonwealth Avenue, Chestnut Hill, Massachusetts 02467, USA.

出版信息

Biochemistry. 2003 Jul 29;42(29):8842-51. doi: 10.1021/bi027354i.

Abstract

An analogue of uridine triphosphate containing a cationic functional group was incorporated into a degenerate RNA library by enzymatic polymerization. In vitro selection experiments using this library yielded a novel receptor that binds ATP under physiological pH and salt conditions in a manner completely dependent on the presence of the cationic functionality. The consensus sequence and a secondary structure model for the ATP binding site were obtained by the analysis of functional sequences selected from a partially randomized pool based on the minimal parental sequence. Mutational studies of this receptor indicated that several of the modified uridines are critical for ATP binding. Analysis of the binding of ATP analogues revealed that the modified RNA receptor makes numerous contacts with ATP, including interactions with the triphosphate group. In contrast, the aptamer repeatedly isolated from natural RNA libraries does not interact with the triphosphate group of ATP. The incorporation of a cationic amine into nucleic acids clearly allows novel interactions to occur during the molecular recognition of ligands, which carries interesting implications for the RNA world hypothesis. In addition, new materials generated from such functionalized nucleic acids could be useful tools in research and diagnostics.

摘要

一种含有阳离子官能团的三磷酸尿苷类似物通过酶促聚合被掺入到一个简并RNA文库中。使用该文库进行的体外筛选实验产生了一种新型受体,该受体在生理pH和盐条件下以完全依赖阳离子官能团存在的方式结合ATP。通过对基于最小亲本序列从部分随机库中选择的功能序列进行分析,获得了ATP结合位点的共有序列和二级结构模型。对该受体的突变研究表明,几个修饰的尿苷对ATP结合至关重要。对ATP类似物结合的分析表明,修饰的RNA受体与ATP有大量接触,包括与三磷酸基团的相互作用。相比之下,从天然RNA文库中反复分离出的适配体不与ATP的三磷酸基团相互作用。将阳离子胺掺入核酸显然允许在配体的分子识别过程中发生新的相互作用,这对RNA世界假说具有有趣的启示。此外,由这种功能化核酸产生的新材料可能是研究和诊断中的有用工具。

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