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Sequential growth of long DNA strands with user-defined patterns for nanostructures and scaffolds

机译:具有用户定义的纳米结构和支架模式的长DNA链的顺序生长

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摘要

DNA strands of well-defined sequence are valuable in synthetic biology and nanostructure assembly. Drawing inspiration from solid-phase synthesis, here we describe a DNA assembly method that uses time, or order of addition, as a parameter to define structural complexity. DNA building blocks are sequentially added with in-situ ligation, then enzymatic enrichment and isolation. This yields a monodisperse, single-stranded long product (for example, 1,000 bases) with user-defined length and sequence pattern. The building blocks can be repeated with different order of addition, giving different DNA patterns. We organize DNA nanostructures and quantum dots using these backbones. Generally, only a small portion of a DNA structure needs to be addressable, while the rest is purely structural. Scaffolds with specifically placed unique sites in a repeating motif greatly minimize the number of components used, while maintaining addressability. This combination of symmetry and site-specific asymmetry within a DNA strand is easily accomplished with our method.
机译:序列明确的DNA链在合成生物学和纳米结构组装中很有价值。从固相合成中汲取灵感,在此我们描述一种DNA组装方法,该方法使用时间或添加顺序作为定义结构复杂性的参数。依次添加DNA结构单元并进行原位连接,然后进行酶促富集和分离。这将产生具有用户定义的长度和序列模式的单分散,单链长产物(例如1,000个碱基)。可以按不同的添加顺序重复构建基块,从而提供不同的DNA模式。我们使用这些主链来组织DNA纳米结构和量子点。通常,只有一小部分DNA结构需要寻址,而其余部分仅是结构性的。在重复基序中具有独特放置的独特位点的支架极大地减少了使用的组件数量,同时保持了可寻址性。 DNA链内对称性和位点特异性不对称性的结合很容易通过我们的方法完成。

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