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基于磷酸盐配位的具有芳香盒的三螺旋体对胆碱的选择性结合。

Selective binding of choline by a phosphate-coordination-based triple helicate featuring an aromatic box.

作者信息

Jia Chuandong, Zuo Wei, Yang Dong, Chen Yanming, Cao Liping, Custelcean Radu, Hostaš Jiří, Hobza Pavel, Glaser Robert, Wang Yao-Yu, Yang Xiao-Juan, Wu Biao

机构信息

Key Laboratory of Synthetic and Natural Functional Molecule Chemistry of the Ministry of Education, College of Chemistry and Materials Science, Northwest University, 710069, Xi'an, China.

Chemical Sciences Division, Oak Ridge National Laboratory, Oak Ridge, TN, 37831-6119, USA.

出版信息

Nat Commun. 2017 Oct 16;8(1):938. doi: 10.1038/s41467-017-00915-8.

Abstract

In nature, proteins have evolved sophisticated cavities tailored for capturing target guests selectively among competitors of similar size, shape, and charge. The fundamental principles guiding the molecular recognition, such as self-assembly and complementarity, have inspired the development of biomimetic receptors. In the current work, we report a self-assembled triple anion helicate (host 2) featuring a cavity resembling that of the choline-binding protein ChoX, as revealed by crystal and density functional theory (DFT)-optimized structures, which binds choline in a unique dual-site-binding mode. This similarity in structure leads to a similarly high selectivity of host 2 for choline over its derivatives, as demonstrated by the NMR and fluorescence competition experiments. Furthermore, host 2 is able to act as a fluorescence displacement sensor for discriminating choline, acetylcholine, L-carnitine, and glycine betaine effectively.The choline-binding protein ChoX exhibits a synergistic dual-site binding mode that allows it to discriminate choline over structural analogues. Here, the authors design a biomimetic triple anion helicate receptor whose selectivity for choline arises from a similar binding mechanism.

摘要

在自然界中,蛋白质已经进化出复杂的空腔,能够在大小、形状和电荷相似的竞争者中选择性地捕获目标客体。指导分子识别的基本原理,如自组装和互补性,启发了仿生受体的发展。在当前的工作中,我们报道了一种自组装的三重阴离子螺旋体(主体2),其具有与胆碱结合蛋白ChoX相似的空腔,晶体结构和密度泛函理论(DFT)优化结构表明了这一点,该螺旋体以独特的双位点结合模式结合胆碱。结构上的这种相似性导致主体2对胆碱的选择性高于其衍生物,核磁共振(NMR)和荧光竞争实验证明了这一点。此外,主体2能够作为荧光位移传感器,有效地区分胆碱、乙酰胆碱、左旋肉碱和甘氨酸甜菜碱。胆碱结合蛋白ChoX表现出协同双位点结合模式,使其能够区分胆碱和结构类似物。在这里,作者设计了一种仿生三重阴离子螺旋体受体,其对胆碱的选择性源于类似的结合机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f011/5643546/ae674de4fb74/41467_2017_915_Fig1_HTML.jpg

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