首页> 外文OA文献 >Oligonucleotide-directed self-assembly of proteins: semisynthetic DNA--streptavidin hybrid molecules as connectors for the generation of macroscopic arrays and the construction of supramolecular bioconjugates.
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Oligonucleotide-directed self-assembly of proteins: semisynthetic DNA--streptavidin hybrid molecules as connectors for the generation of macroscopic arrays and the construction of supramolecular bioconjugates.

机译:寡核苷酸定向的蛋白质自组装:半合成DNA-链霉亲和素杂合分子作为连接器,用于产生宏观阵列和构建超分子生物结合物。

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摘要

Modified biomolecules were used for the non-covalent assembly of novel bioconjugates. Hybrid molecules were synthesized from short single-stranded DNA and streptavidin by chemical methods using a heterobispecific crosslinker. The covalent attachment of an oligonucleotide moiety to streptavidin provides a specific recognition domain for a complementary nucleic acid sequence, in addition to the four native biotin-binding sites. These bispecific binding capabilities allow the hybrid molecules to serve as versatile connectors in a variety of applications. Bifunctional constructs have been prepared from two complementary hybrid molecules, each previously conjugated to biotinylated immunoglobulin G or alkaline phosphatase. The use of nucleic acid sequences as a template for the formation of an array of proteins is further demonstrated on two size scales. A macroscopic DNA array on a microtiter plate has been transformed into a comparable protein chip. A nano-scale array was made by hybridizing DNA-tagged proteins to specific positions along a RNA or DNA sequence. The generation of supramolecular bioconjugates was shown by quantitative measurements and gel-retardation assays.
机译:修饰的生物分子用于新型生物缀合物的非共价组装。使用异双特异性交联剂通过化学方法由短的单链DNA和链霉亲和素合成杂合分子。寡核苷酸部分与链霉亲和素的共价连接,除了四个天然生物素结合位点以外,还为互补核酸序列提供了特异性识别域。这些双特异性结合功能使杂化分子可以在多种应用中用作通用连接器。已经从两个互补的杂合分子制备了双功能构建体,每个分子先前已与生物素化的免疫球蛋白G或碱性磷酸酶缀合。在两个大小尺度上进一步证明了将核酸序列用作形成蛋白质阵列的模板。微量滴定板上的宏观DNA阵列已被转化为可比较的蛋白质芯片。通过将标记有DNA的蛋白质与沿RNA或DNA序列的特定位置杂交,可以制成纳米级阵列。超分子生物共轭物的产生通过定量测量和凝胶延迟测定显示。

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