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Building expanded structures from tetrahedral DNA branching elements, RNA and TMV protein

机译:构建扩大从DNA四面体结构分支元素,RNA和烟草花叶病毒的蛋白质

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摘要

By combining both chemical and enzymatic ligation with procedures guiding the self-assembly of nanotubular tobacco mosaic virus (TMV)-like particles (TLPs), novel nucleoprotein structures based on DNA-terminated branching elements, RNA scaffolds and TMV coat protein (CP) are made accessible. Tetrahedral tetrakis(hydroxybiphenyl)adamantane cores with four 5-phosphorylated dinucleotide arms were coupled to DNA linkers by chemical ligation. The resulting three-dimensional (3D) branching elements were enzymatically ligated to the 3 termini of RNA scaffolds either prior to or after the RNAs' incorporation into TLPs. Thus, architectures with interconnected nanotube domains in two different length classes were generated, each containing 70 CP subunits per 10 nm length. Short TMV origin-of-assembly-containing RNA scaffolds ligated to the DNA allowed the growth of protein-coated 34 nm tubes on the terminal RNA strands in situ. Alternatively, 290 nm pre-fabricated tubes with accessible RNA 3 termini, attained by DNA blocking elements hybridized to the RNAs, were ligated with the branched cores. Both approaches resulted in four-armed nanoobjects, demonstrating a so far unique combination of organic synthesis of branching elements, enzymatic modifications, nucleic acid-based scaffolding and RNA-guided and DNA-controlled assembly of tubular RNA-encapsidating protein domains, yielding a novel class of 3D nucleoprotein architectures with polyvalent protein elements. In the long term, the production route might give rise to supramolecular systems with complex functionalities, installed via the orthogonal coupling of effector molecules to TLP domains.
机译:结合化学和酶结扎自组装的过程指导nanotubular烟草花叶病毒(TMV)的地方粒子(tlp),小说核蛋白质结构基于DNA-terminated分支元素,RNA支架和烟草花叶病毒外壳蛋白(CP)可访问。tetrakis——hydroxybiphenyl adamantane cores产的四个5-phosphorylated二核苷酸的手臂耦合到DNA连接基团通过化学结扎。生成的三维(3 d)的分支元素具有结扎3目的地的RNA脚手架之前或之后rna的并入张力腿平台。架构与互连纳米管域名长度在两个不同的类生成,每个包含每10 70 CP子单元纳米长度。origin-of-assembly-containing RNA支架结扎DNA允许的增长在终端RNA protein-coated 34纳米管股原位。预制的管道与访问RNA 3DNA末端,达到阻断元素杂化的rna,结扎了支核心。四名武装nanoobjects,展示一个到目前为止有机合成的独特组合分支元素,酶的修改,核酸脚手架和RNA-guided和DNA-controlled组装的管状RNA-encapsidating蛋白质域,产生一个小说类的3 d核蛋白质的架构蛋白质与多价元素。术语,可能引起生产路线超分子系统与复杂功能,通过正交安装耦合效应分子TLP域。

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